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US20230277500A1 - Compositions comprising aticaprant - Google Patents

Compositions comprising aticaprant Download PDF

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Publication number
US20230277500A1
US20230277500A1 US18/179,093 US202318179093A US2023277500A1 US 20230277500 A1 US20230277500 A1 US 20230277500A1 US 202318179093 A US202318179093 A US 202318179093A US 2023277500 A1 US2023277500 A1 US 2023277500A1
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United States
Prior art keywords
aticaprant
weight
pharmaceutical composition
patient
treatment
Prior art date
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Abandoned
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US18/179,093
Inventor
Nicolaas Martha Felix Goyvaerts
Mark Schmidt
Vanina Popova
Adam Savitz
Rama Melkote
Wayne C. Drevets
Srihari Gopal
Darrel Pemberton
Chakradhar Lagishetty
Iva Kezic
Mahesh N. Samtani
Tom Huybrechts
Geert Van Der Avoort
Matthieu Ravelingien
Laura Martinez Marcos
Tatiana MARCOZZI
Katarina Jokicevic
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Janssen Pharmaceuticals Inc
Original Assignee
Janssen Pharmaceutica NV
Janssen Pharmaceuticals Inc
Janssen Research and Development LLC
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Application filed by Janssen Pharmaceutica NV, Janssen Pharmaceuticals Inc, Janssen Research and Development LLC filed Critical Janssen Pharmaceutica NV
Priority to US18/179,093 priority Critical patent/US20230277500A1/en
Publication of US20230277500A1 publication Critical patent/US20230277500A1/en
Assigned to Janssen Pharmaceuticals, Inc. reassignment Janssen Pharmaceuticals, Inc. ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: JANSSEN PHARMACEUTICA NV
Assigned to JANSSEN RESEARCH & DEVELOPMENT, LLC reassignment JANSSEN RESEARCH & DEVELOPMENT, LLC ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: SAVITZ, Adam, GOPAL, SRIHARI, SAMTANI, MAHESH N., MELKOTE, RAMA, DREVETS, WAYNE, LAGISHETTY, CHARKRADHAR
Assigned to JANSSEN PHARMACEUTICA NV reassignment JANSSEN PHARMACEUTICA NV ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: POPOVA, VANINA, MARCOZZI, Tatiana, SCHMIDT, MARK, RAVELINGIEN, Matthieu, GOYVAERTS, NICOLAAS MARTHA FELIX, JOKICEVIC, Katarina, MARCOS, Laura Martinez, PEMBERTON, DARREL, VAN DER AVOORT, Geert, Huybrechts, Tom, KEZIC, IVA
Assigned to Janssen Pharmaceuticals, Inc. reassignment Janssen Pharmaceuticals, Inc. ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: JANSSEN RESEARCH & DEVELOPMENT, LLC
Priority to US18/618,520 priority patent/US12201610B2/en
Priority to US19/023,669 priority patent/US20250228819A1/en
Abandoned legal-status Critical Current

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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/40Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having five-membered rings with one nitrogen as the only ring hetero atom, e.g. sulpiride, succinimide, tolmetin, buflomedil
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K45/00Medicinal preparations containing active ingredients not provided for in groups A61K31/00 - A61K41/00
    • A61K45/06Mixtures of active ingredients without chemical characterisation, e.g. antiphlogistics and cardiaca
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2009Inorganic compounds
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2013Organic compounds, e.g. phospholipids, fats
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2013Organic compounds, e.g. phospholipids, fats
    • A61K9/2018Sugars, or sugar alcohols, e.g. lactose, mannitol; Derivatives thereof, e.g. polysorbates
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2022Organic macromolecular compounds
    • A61K9/205Polysaccharides, e.g. alginate, gums; Cyclodextrin
    • A61K9/2054Cellulose; Cellulose derivatives, e.g. hydroxypropyl methylcellulose
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/28Dragees; Coated pills or tablets, e.g. with film or compression coating
    • A61K9/2806Coating materials
    • A61K9/2833Organic macromolecular compounds
    • A61K9/2853Organic macromolecular compounds obtained otherwise than by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyethylene glycol, polyethylene oxide, poloxamers, poly(lactide-co-glycolide)
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/4816Wall or shell material
    • A61K9/4825Proteins, e.g. gelatin
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/4841Filling excipients; Inactive ingredients
    • A61K9/4858Organic compounds
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/4841Filling excipients; Inactive ingredients
    • A61K9/4866Organic macromolecular compounds
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/24Antidepressants

Definitions

  • compositions including oral compositions, comprising aticaprant and methods of using the same.
  • Kappa opioid receptors and their native ligand dynorphin are localized in areas of the brain that effect reward and stress and may play a key role in mood, stress, and addictive disorders.
  • Chronic stress, substance abuse, and acute withdrawal lead to increased dynorphin expression, activating KORs and subsequent downstream signaling pathways to inhibit mesolimbic dopamine surge, contributing to negative affective states.
  • the behavioral pharmacology of KOR antagonism has been tested in animal models of anhedonia, depression, and anxiety and found to have meaningful effects that may translate to therapeutic benefit in humans.
  • KOR antagonists may be effective for the treatment of patients with mood disorders, perhaps by modulating the negative affective state associated with stress response.
  • Anhedonia is one of the core symptoms of depression. At least mild symptoms of anhedonia are present in about 90% of patients suffering from major depressive disorder (MDD). Only about 50% of patients with MDD show a meaningful response (>50% improvement to a first line antidepressant treatment), leaving many patients with substantial persistent impairment. Therapeutic strategies such as switching antidepressants and using adjuvant drug treatments can improve response, however almost 40% of patients remain symptomatic and fail to achieve full remission.
  • MDD major depressive disorder
  • the disclosure provides pharmaceutical compositions comprising about 2 mg to about 20 mg aticaprant and a filler, wherein the composition comprises between about 0.1% to about 90% aticaprant by weight.
  • the disclosure provides oral tablets comprising about 5 mg aticaprant, wherein the oral tablet comprises a core tablet of about 100 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 30 mg microcrystalline cellulose, about 30 mg lactose monohydrate, about 2.5 mg croscarmellose sodium, and about 0.5 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 28.5 mg silicified microcrystalline cellulose, about 2.5 mg croscarmellose sodium, about 0.5 mg silica, colloidal anhydrous, and about 0.5 mg magnesium stearate.
  • the disclosure provides oral tablets comprising about 10 mg aticaprant, wherein the oral tablet comprises a core tablet of about 200 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 60 mg microcrystalline cellulose, about 60 mg lactose monohydrate, about 5 mg croscarmellose sodium, and about 1 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 57 mg silicified microcrystalline cellulose, about 5 mg croscarmellose sodium, about 1 mg silica, colloidal anhydrous, and about 1 mg magnesium stearate.
  • the disclosure provides pharmaceutical compositions comprising between about 2 mg and 20 mg aticaprant, wherein the composition has a pharmacokinetic (PK) profile comprising one or more of the following parameters after administration of the composition to a human after at least a 10-hour fast (dose-normalized to 10 mg): (a) a mean C max between about 20 and 45 ng/mL; (b) a mean AUC infinity between about 250 and 450 h*ng/mL; (c) a mean AUC last between about 250 and 450 h*ng/mL; and (d) a median t max between about 1 to 4 hours.
  • PK pharmacokinetic
  • the disclosure provides methods for treating major depressive disorder (MDD) in a human patient, the method comprising administering to the patient a pharmaceutical composition comprising between about 2 mg and 20 mg aticaprant, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with aticaprant, and wherein the administration of the pharmaceutical composition to the patient achieves a pharmacokinetic (PK) profile comprising one or more of the following PK parameters (dose-normalized to 10 mg) after administration of the composition to a human after at least a 10-hour fast: (a) a mean C max between about 30 and 40 ng/mL; (b) a mean AUC infinity between about 300 and 430 h*ng/mL; (c) a mean AUC last between about 280 and 430 h*ng/mL; and (d) a median t max between about 1 to 4 hours.
  • PK pharmacokinetic
  • the disclosure provides solid pharmaceutical compositions comprising between about 2 mg and 20 mg aticaprant, wherein the composition has a dissolution profile comprising a Q value of between about 60% and 90% at 45 minutes, under the following dissolution operating conditions: Apparatus: Paddle (USP Type 2, Ph. Eur., JP); Dissolution medium: 0.01 M hydrochloric acid; Volume: 900 mL; Temperature: 37+/ ⁇ 0.5° C.; Rotation Speed: 50 rpm; and Analytical Finish: UHPLC with UV detection at 247 nm.
  • Apparatus Paddle (USP Type 2, Ph. Eur., JP); Dissolution medium: 0.01 M hydrochloric acid; Volume: 900 mL; Temperature: 37+/ ⁇ 0.5° C.; Rotation Speed: 50 rpm; and Analytical Finish: UHPLC with UV detection at 247 nm.
  • the disclosure provides methods of treating major depressive disorder (MDD) in a human patient comprising administering to the patient the pharmaceutical composition, oral tablet, or solid pharmaceutical composition described herein.
  • MDD major depressive disorder
  • FIG. 1 is the x-ray powder diffraction (XRPD) pattern of polymorph Form III of aticaprant (transmission mode).
  • FIG. 2 is the differential scanning calorimetry (DSC) thermogram of polymorph Form III of aticaprant.
  • FIG. 3 is the mDSC thermogram of polymorph Form III of aticaprant.
  • FIG. 4 is the trial design of Example 1.
  • FIG. 5 is a line graph showing the MADRS (Montgomery- ⁇ sberg Depression Rating Scale) total score: least squares mean changes from baseline ( ⁇ SE) during the treatment period for the enriched intent-to-treat (eITT) analysis set.
  • MADRS Monitoring- ⁇ sberg Depression Rating Scale
  • FIG. 6 is a plot showing MADRS total score changes at treatment week 6 for enriched and full population: MMRM results—estimated LS means and comparison versus placebo.
  • FIG. 7 is a line graph showing SHAPS (Snaith-Hamilton Pleasure Scale) total score: least squares mean changes from baseline ( ⁇ SE) during the treatment period for the eITT analysis set.
  • SHAPS Snaith-Hamilton Pleasure Scale
  • FIG. 8 is a plot showing SHAPS total score changes at treatment week 6 for enriched and full population: MMRM (Mixed-effects Model for Repeated Measures) Results—estimated LSMeans and comparison versus placebo
  • FIG. 9 is a line graph showing MADRS total score: mean values ( ⁇ SE) over time for the eITT analysis set.
  • FIG. 10 -A is a line graph showing MADRS total score: mean values ( ⁇ SE) over time for the full intent-to-treat (fITT) analysis set.
  • FIG. 10 -B is an excerpt from FIG. 10 -A for treatment weeks 0-6.
  • FIG. 11 is a line graph showing MADRS total score: percentage of subjects with remission of depressive symptoms (total score ⁇ 10) during the treatment period for the eITT analysis set.
  • FIG. 12 is a line graph showing MADRS total score: percentage of subjects with remission of depressive symptoms (total score ⁇ 10) during the treatment period for the fITT analysis set.
  • FIG. 13 is a line graph showing MADRS total score: percentage of responders ( ⁇ 30% improvement from baseline) during the treatment period for the eITT analysis set.
  • FIG. 14 is a line graph showing MADRS total score: percentage of responders ( ⁇ 30% improvement from baseline) during the treatment period for the fITT analysis set.
  • FIG. 15 is a line graph showing MADRS total score: percentage of responders ( ⁇ 50% improvement from baseline) during the treatment period for the eITT analysis set.
  • FIG. 16 is a line graph showing MADRS total score: percentage of responders ( ⁇ 50% improvement from baseline) during the treatment period for the fITT analysis set.
  • FIG. 17 is a line graph showing SHAPS total score: mean values ( ⁇ SE) over time for the eITT analysis set.
  • FIG. 18 is a line graph showing SHAPS total score: mean values ( ⁇ SE) over time for the fITT analysis set.
  • FIG. 19 illustrates the MADRS change from baseline by anhedonia severity.
  • FIG. 20 -A is a line graph showing MADRS change from baseline for patients with high anhedonia, i.e., SHAPS ⁇ 38.
  • FIG. 20 -B is a line graph showing MADRS change from baseline for patients with low anhedonia, i.e., SHAPS ⁇ 38.
  • FIG. 21 is bar graph showing the comparison of MADRS in patients having low and high anhedonia.
  • FIG. 22 is a line graph showing the ASEX total score mean change from baseline.
  • FIG. 23 is a bar graph showing ASEX item level change total score mean change from baseline.
  • FIG. 24 is the flow chart for the process for preparing tablets containing aticaprant.
  • a refers to microfine, i.e., milled aticaprant.
  • FIG. 25 is the schematic overview of part 1 of the study.
  • FIG. 26 is the schematic overview of part 2 of the study.
  • a) Day 1 of a treatment period is the first day of the washout period.
  • Treatment E 2 ⁇ 5 mg oral capsule administered in the morning, after at least 10-hour overnight fasting.
  • Treatment F 1 ⁇ 10 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting.
  • Treatment G 1 ⁇ 5 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting.
  • Treatment H 1 ⁇ 10 mg Formulation Concept 2 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
  • FIGS. 27 and 28 show the relative bioavailability results for aticaprant PK profiles relative to BA.
  • FIGS. 29 and 30 show the relative bioavailability results for aticaprant PK profile, dose-proportionality.
  • FIGS. 31 - 33 show the relative bioavailability results for aticaprant PK profile, food effect.
  • FIG. 34 is the study scheme for Example 7. All patients will continue their oral antidepressant SSRI/SNRI during the entire study. Approximately an additional 34 elderly participants will be randomized.
  • FIG. 35 is the study scheme for Example 8. All patients will continue their oral antidepressant SSRI/SNRI during the entire study. Approximately an additional 68 elderly participants will be randomized.
  • FIG. 36 is a bar graph showing the SHAPS items: LS means for change from baseline at week 6 by baseline SHAPS total score for the fITT analysis set.
  • the bars alternatively refer to placebo or aticaprant.
  • the first bar refers to aticaprant
  • the second bar refers to placebo
  • the third bar refers to aticaprant, etc.
  • FIG. 37 is a plot showing MADRS total score: difference of LSMeans (60% at Weeks 6 by different subgroups for the fITT analysis set. In this plot, ⁇ 17 indicates mild severity; 18-24 indicates mild to moderate severity, and 25-30 indicates moderate to severe.
  • compositions comprising pure crystalline Form of III aticaprant that are anhydrous and stable in the solid form.
  • crystalline refers to a solid form of a chemical moiety that contains a highly ordered intermolecular structure.
  • polymorph refers to a crystalline form of a molecule having one specific crystal structure.
  • a crystalline compound may have one crystal form or may have two or more crystal forms, i.e., polymorphs.
  • polymorphs of a chemical compound may distinguished from each other by compared physicochemical properties such as solubility, dissolution rate, stability, bioavailability, among others.
  • Polymorphs also may have different spectra selected from, without limitation, x-ray powder diffraction (XRPD), single crystal x-ray diffraction, thermogravimetric analysis (TGA), infrared spectroscopy, Raman spectroscopy, solid state nuclear magnetic resonance (NMR), differential scanning calorimetry (DSC), polarized light microscopy (PLM), hot stage microscopy, or dynamic solvent sorption.
  • XRPD x-ray powder diffraction
  • TGA thermogravimetric analysis
  • infrared spectroscopy Raman spectroscopy
  • NMR solid state nuclear magnetic resonance
  • DSC differential scanning calorimetry
  • PLM polarized light microscopy
  • hot stage microscopy or dynamic solvent sorption.
  • crystalline refers to solid state form of a chemical moiety wherein the atoms, molecules, or ions are assembled in a highly ordered structure that extends in all directions.
  • crystalline includes all crystalline forms of Compound I, including salts thereof. Characterization of crystalline forms may be performed by those skilled in the art including, without limitation, XRPD or DSC. Typically, the XRPD pattern contains sharp intensity peaks. This contrasts to the XRPD pattern of an amorphous form that often contains a broad, peak, without no identifying peaks.
  • a crystalline form may be completely crystalline or partially crystalline. In some aspects, a crystalline sample may be 100% w/w crystalline. A crystalline sample may also contain solids that are amorphous.
  • a crystalline form may contain solids such that the sample is at least about 99% w/w crystalline, at least about 95% w/w amorphous, at least about 90% w/w crystalline, at least about 85% w/w crystalline, at least about 80% w/w crystalline, or the like.
  • anhydrous or “anhydrate” as used herein refers to a crystalline as described herein that substantially lacks water.
  • an anhydrous form contains less than about 1% w/w of water.
  • an anhydrous form contains less than about 0.9%, about 0.8%, about 0.7%, about 0.6%, about 0.5%, about 0.4%, about 0.3%, about 0.2%, about 0.1% w/w of water.
  • temperatures noted herein vary by about 0.1°, about 0.5°, about 1°, about 2°, about 3°, about 4°, or about 5°.
  • 2 ⁇ values obtained from the XRPD patterns also may vary. Such variations may depend on instrument type, instrument parameters, laboratory techniques, sample (including particle size, impurities, etc.), and/or laboratory conditions. Unless otherwise defined, the XRPD patterns and/or the 2 ⁇ peak values may vary. In certain aspects, the 2 ⁇ peak values vary (higher or lower) by about 0.05°, about 0.1°, about 0.15°, or about 0.2°. In other aspects, one or more of the 2 ⁇ peak values are higher by about 0.05°, about 0.1°, about 0.15°, or about 0.2°. In further aspects, one or more of the 2 ⁇ peak values are lower by about 0.05°, about 0.1°, about 0.15°, or about 0.2°.
  • the term “corresponds to” may be used in reference to certain spectra.
  • “corresponds to” includes a spectrum that is identical or substantially similar to another spectrum.
  • One skilled in the art would be able to compare such spectra and determine if a spectrum corresponds to another.
  • the term “corresponds to” is used herein to compare XRPD patterns, DSC thermograms, among others.
  • one XRPD pattern corresponds to another XRPD pattern when their 2 ⁇ values are within the margin of error as described above.
  • one XRPD pattern corresponds to another XRPD pattern when the peaks have the same 2 ⁇ peak value, but one or more peaks have a different height (intensity).
  • one XRPD pattern corresponds to another XRPD pattern when the peaks have the same 2 ⁇ peak value, but one or more peaks have a different peak area.
  • one XRPD pattern corresponds to another XRPD pattern when the peaks have the same 2 ⁇ peak value, but one or more peak is obscured. Such obscured peaks may be due to impurities, excipients, or the like. Such obscured peaks typically do not prevent characterization of the crystalline form.
  • aticaprant refers to 3-fluoro-4-4-2-(3,5-dimethylphenyl)pyrrolidin-1-yl-methylphenoxybenzamide, i.e., the following compound:
  • aticaprant refers to the (S)-enantiomer of aticaprant, i.e., the following compound:
  • the aticaprant used in the methods described herein is substantially free of the (R)-enantiomer, i.e., (R)-aticaprant or (R)-3-fluoro-4-4-2-(3,5-dimethylphenyl)pyrrolidin-1-yl-methylphenoxybenzamide having the following structure:
  • the aticaprant contains less than about 10% by weight, based on the weight of aticaprant, of the (R)-enantiomer of aticaprant. In further embodiments, aticaprant contains less than about 10, about 9, about 8, about 7, about 6, about 5, about 4, about 3, about 2, about 1, about 0.5, about 0.1, about 0.005, or about 0.001% by weight, based on the weight of aticaprant, of the (R)-enantiomer of aticaprant. In yet other embodiments, the aticaprant contains about 0.001 to about 10% by weight, based on the weight of aticaprant, of the (R)-enantiomer of aticaprant.
  • the aticaprant contains about 0.001 to about 10%, about 0.001 to about 5%, about 0.001 to about 1%, about 0.001 to about 0.5%, about 0.001 to about 0.1%, about 0.1 to about 5%, about 0.1 to about 1%, about 0.1 to about 5%, or about 0.5 to about 5% by weight, based on the weight of aticaprant.
  • compositions of aticaprant are also contemplated by the present invention, which may be readily selected by those skilled in the art.
  • a “pharmaceutically acceptable salt” refers a salt of aticaprant that is non-toxic, biologically tolerable, or otherwise biologically suitable for administration to the subject. See, generally, G. S. Paulekuhn, “Trends in Active Pharmaceutical Ingredient Salt Selection based on Analysis of the Orange Book Database”, J. Med. Chem., 2007, 50:6665-72, S. M. Berge, “Pharmaceutical Salts”, J. Pharm.
  • salts examples include those that are pharmacologically effective and suitable for administration to patients without undue toxicity, irritation, or allergic response.
  • Examples of pharmaceutically acceptable salts include sulfates, pyrosulfates, bisulfates, sulfites, bisulfites, phosphates, monohydrogen-phosphates, dihydrogenphosphates, metaphosphates, pyrophosphates, bromides (such as hydrobromides), iodides (such as hydroiodides), acetates, propionates, decanoates, caprylates, acrylates, formates, isobutyrates, caproates, heptanoates, propiolates, oxalates, malonates, succinates, suberates, sebacates, fumarates, maleates, butyne-1,4-dioates, hexyne-1,6-dioates, benzoates, chlorobenzoates, methylbenzoates, dinitrobenzoates, hydroxybenzoates, methoxybenzoates, phthalates, sulfonates, xylenesulf
  • the aticaprant is crystalline Form III of aticaprant.
  • Crystalline Form III of aticaprant may be characterized by a number of techniques including, without limitation, x-ray diffraction and differential scanning calorimetry.
  • crystalline Form III of aticaprant is characterized by x-ray diffraction.
  • crystalline Form III of aticaprant is characterized by four or more x-ray diffraction pattern peaks at 2 ⁇ ( ⁇ 0.2) of 4.1°, 9.0°, 17.6°, 18.0°, or 21.4°.
  • crystalline Form III of aticaprant is characterized by four or more x-ray diffraction pattern peaks at 2 ⁇ ( ⁇ 0.2) of 4.1°, 9.0°, 17.6°, 18.0°, or 21.4° and one or more additional peaks at 16.4°, 20.1°, 20.3°, 24.1°, and 25.7°.
  • crystalline Form III of aticaprant is characterized by four or more x-ray diffraction pattern peaks at 2 ⁇ ( ⁇ 0.2) of 4.1°, 9.0°, 17.6°, 18.0°, or 21.4° and one or more additional peaks at 15.1°, 16.4°, 20.0°, 20.1°, 20.3°, 24.1°, 25.0°, 25.7°, 26.2°, and 28.8°.
  • crystalline Form III of aticaprant is characterized by four or more x-ray diffraction pattern peaks at 2 ⁇ ( ⁇ 0.2) of 4.1°, 9.0°, 17.6°, 18.0°, or 21.4° and one or more additional peaks at 8.2°, 9.7°, 12.0°, 13.5°, 15.1°, 16.4°, 19.4°, 28.4°, 20.0°, 20.1°, 20.3°, 24.1°, 25.0°, 25.7°, 26.2°, 28.8°, and 30.0°.
  • crystalline Form III of aticaprant is characterized by four or more x-ray diffraction pattern peaks at 2 ⁇ ( ⁇ 0.2) of 3.1°, 19.0°, 24.0°, 24.3°, or 26.2 and one or more additional peaks of Table 1.
  • crystalline Form III of aticaprant is characterized the x-ray diffraction pattern peaks in Table 2.
  • crystalline Form III of aticaprant is characterized the x-ray diffraction pattern peaks in Table 3.
  • crystalline Form III of aticaprant is characterized by an x-ray powder diffraction pattern that corresponds to FIG. 1 .
  • Crystalline Form III of aticaprant may also be characterized by differential scanning calorimetry.
  • the differential scanning calorimetry thermogram comprises a peak temperature (T m ) at about 121° C.
  • crystalline Form III of aticaprant is characterized by a differential scanning calorimetry thermogram that corresponds to FIG. 2 .
  • composition comprising aticaprant and one or more pharmaceutically acceptable excipient.
  • composition is intended to encompass a product comprising the specified ingredients in the specified amounts, as well as any product which results, directly or indirectly, from combinations of the specified ingredients in the specified amounts.
  • the preferred pharmaceutical composition contains crystalline Form III of aticaprant as the active ingredient intimately admixed with a pharmaceutical carrier according to conventional pharmaceutical compounding techniques, which carrier may take a wide variety of forms depending on the form of preparation desired for administration.
  • Suitable pharmaceutically acceptable carriers are well known in the art. Descriptions of some of these pharmaceutically acceptable carriers may be found in The Handbook of Pharmaceutical Excipients, published by the American Pharmaceutical Association and the Pharmaceutical Society of Great Britain.
  • the amount of aticaprant present in the compositions is about 2 mg to about 60 mg. In some embodiments, the composition contains about 2 mg to about 20 mg of aticaprant. In some embodiments, the composition contains about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 11, about 12, about 13, about 14, about 15, about 16, about 17, about 18, about 19, or about 20 mg of aticaprant. In other embodiments, the composition contains about 5 to about 20 mg, about 10 to about 20 mg, about 15 to about 20 mg, about 1 to about 15 mg, about 2 to about 15 mg, about 5 to about 15 mg, about 10 to about 15 mg, about 1 to about 10 mg, about 2 to about 10 mg, or about 5 to about 10 mg of aticaprant.
  • the effective amount of aticaprant is about 5 to about 15 mg. In further embodiments, the amount of aticaprant is about 5 or 10 mg. In other embodiments, the amount of aticaprant is about 5 mg. In still further embodiments, the amount of aticaprant is about 10 mg.
  • the composition contains about 0.1% to about 90% by weight of aticaprant. In some embodiments, the composition contains about 0.1, about 0.5, about 1, 5, about 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, about 50, about 55, about 60, about 65, about 70, about 75, about 80, about 85, about 90% by weight, based on the weight of the composition, of aticaprant.
  • the composition contains about 0.1 to about 80, about 0.1 to about 70, about 0.1 to about 60, about 0.1 to about 50, about 0.1 to about 40, about 0.1 to about 30, about 0.1 to about 20, about 0.1 to about 10, about 0.1 to about 5, about 0.1 to about 1, about 0.1 to about 0.5, about 1 to about 90, about 1 to about 80, about 1 to about 70, about 1 to about 60, about 1 to about 50, about 1 to about 40, about 1 to about 30, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 5 to about 90, about 5 to about 80, about 5 to about 70, about 5 to about 60, about 5 to about 50, about 5 to about 40, about 5 to about 30, about 5 to about 20, about 5 to about 10, about 10 to about 90, about 10 to about 80, about 10 to about 70, about 10 to about 60, about 10 to about 60, about 10 to about 50, about 10 to about 40, about 10 to about 30, about 10 to about 20, about 20 to about 90, about 20 to about 80, about 20 to about 20 to about
  • the composition contains about 5% by weight of aticaprant. In yet other embodiments, the composition contains about 6% by weight of aticaprant. In still further embodiments, the composition contains about 7% by weight of aticaprant. In other embodiments, the composition contains about 8% by weight of aticaprant. In further embodiments, the composition contains about 9% by weight of aticaprant. In still other embodiments, the composition contains about 10% by weight of aticaprant.
  • the amount of aticaprant for administration according to the methods described herein may be determined by one skill in the art and, unless otherwise noted, are set forth on an aticaprant free base basis. That is, the amounts indicate that amount of the aticaprant molecule administered, exclusive of, for example, solvent (such as in solvates) or counterions (such as in pharmaceutically acceptable salts).
  • the pharmaceutical compositions have a particular pharmacokinetic (PK) profile at a specific dose.
  • the pharmaceutical compositions have a PK profile that is dose-proportional.
  • the pharmaceutical compositions have a PK profile comprising parameters, e.g., exposure parameters such as C max or AUC, that are dose-proportional.
  • the pharmaceutical compositions have a PK profile or PK parameter that is dose-proportional between about 1 mg to 60 mg aticaprant, between about 2 mg to 60 mg aticaprant, between about 2 mg to 40 mg aticaprant, between about 2 mg to 20 mg aticaprant, between about 2 mg to 15 mg aticaprant, between about 2 mg to 10 mg aticaprant, and between about 5 mg to 10 mg aticaprant.
  • compositions comprising aticaprant that are bioequivalent to any one of the pharmaceutical compositions described herein.
  • the pharmaceutical composition comprises between about 2 mg and about 60 mg, between about 2 mg and about 20 mg aticaprant, between about 5 mg and about 10 mg aticaprant, or about 5 mg or about 10 mg aticaprant, wherein the composition is bioequivalent to a pharmaceutical composition comprising aticaprant which when administered to a human after at least a 10-hour fast yields a PK profile that includes one or more of: a mean Cmax of between about 30 and 35 ng/mL, a mean AUCinfinity of between about 300 and 320 ng/mL, and a median t max of about 1.5 hour (dose-normalized to 10 mg).
  • Bioequivalence may be demonstrated by any method known to one skilled in the art, for example, as described in Example 9 herein, or as described in Chow, Bioavailability and Bioequivalence in Drug Development, Wiley interdisciplinary reviews, Computational statistics, 6, 4 (2014): 304-312. doi:10.1002/wics.1310.
  • the pharmaceutical composition comprises between about 2 mg and about 20 mg aticaprant, about 5 mg aticaprant, or about 10 mg aticaprant, wherein when the pharmaceutical composition is compared to a reference composition, the 90% confidence interval of the ratio of geometric means of one or more PK parameters of the pharmaceutical composition and reference composition is within the bioequivalence limits of 80% and 125%.
  • the reference composition is a composition comprising aticaprant which when administered to a human after at least a 10-hour fast yields a PK profile that includes one or more of: a mean Cmax of between about 30 and 35 ng/mL, a mean AUCinfinity of between about 300 and 320 ng/mL, and a median t max of about 1.5 hour (dose-normalized to 10 mg).
  • the reference composition has a PK profile of any one of Treatment A, Treatment B, Treatment C, or Treatment D described in Table 69.
  • the PK profile is based on administration of the composition, containing about 2 mg to about 60 mg aticaprant, to a human after at least a 10-hour fast. In some other embodiments, the PK profile is based on administration of the composition, containing about 2 mg to about 60 mg aticaprant, to a human about 30 minutes after the start of a high-fat meal following at least a 10-hour fast. As another example, the PK profile is based on administration of the composition, containing about 2 mg to about 20 mg aticaprant, to a human after at least a 10-hour fast.
  • the PK profile is based on administration of a composition containing about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 11, about 12, about 13, about 14, about 15, about 16, about 17, about 18, about 19, or about 20 mg of aticaprant to a human.
  • the PK profile is based on administration of a composition containing about 2 to about 19, about 2 to about 18, about 2 to about 16, about 2 to about 14, about 2 to about 12, about 2 to about 10, about 2 to about 8, about 2 to about 6, about 2 to about 4, about 4 to about 20, about 4 to about 18, about 4 to about 16, about 4 to about 14, about 4 to about 12, about 4 to about 10, about 4 to about 8, about 4 to about 6, about 6 to about 20, about 6 to about 18, about 6 to about 16, about 6 to about 14, about 6 to about 12, about 6 to about 10, about 6 to about 8, about 8 to about 20, about 8 to about 18, about 8 to about 16, about 8 to about 14, about 8 to about 12, about 8 to about 10, about 10 to about 20, about 10 to about 18, about 10 to about 16, about 10 to about 14, about 10 to about 12, about 12 to about 20, about 12 to about 18, about 12 to about 16, about 16, about 12 to about 14, about 14 to about 20, about 14 to about 18, about 18, about 14 to about 16, about 16 to about 20, about 16 to about 18, or about 18 to about 20 mg of aticaprant to a
  • the PK profile is determined after an at least 10-hour food fast.
  • the food fast is at least about 1, about 2, about 4, about 5, about 10, about 12, about 15, about 18, about 20, about 22, 24, about 28, or about 32 hours.
  • the PK profile may include a C max ranging between about 1 and about 100, about 5 and about 70, about 5 and about 65, about 5 and about 60, about 5 and about 55, about 5 and about 50, about 5 and about 45, about 10 and about 70, about 10 and about 65, about 10 and about 60, about 10 and about 55, about 10 and about 50, about 10 and about 45, about 13 and about 60, about 13 and about 55, about 13 and about 50, about 20 and about 70, about 20 and about 65, or about 20 and about 63 ng/mL (dose-normalized to 10 mg).
  • C max ranging between about 1 and about 100, about 5 and about 70, about 5 and about 65, about 5 and about 60, about 5 and about 55, about 5 and about 50, about 5 and about 45, about 10 and about 70, about 10 and about 65, about 10 and about 60, about 10 and about 55, about 10 and about 50, about 10 and about 45, about 13 and about 60, about 13 and about 55, about 13 and about 50, about 20 and about 70, about 20 and
  • the PK profile includes a C max ranging between about 20 and about 45, about 22 and about 45, about 23 and about 45, or about 24 and about 44 ng/mL (dose-normalized to 10 mg) when administered after at least a 10-hour fast. In some embodiments, the PK profile includes a C max ranging between about 25 and about 50, about 27 and about 38, about 25 and about 40, or about 28 and about 38 ng/mL (dose-normalized to 10 mg) when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • the PK profile includes an AUC infinity ranging between about 50 and about 800, about 100 and about 500, about 100 and about 480, about 100 and about 450, about 100 and about 400, about 110 and about 500, about 110 and about 480, about 110 and about 450, about 110 and about 400, about 150 and about 700, about 200 and about 700, about 200 and about 650, about 250 and about 450, about 280 and about 420, about 290 and about 410, or about 210 and about 650 h*ng/mL (dose-normalized to 10 mg).
  • the PK profile includes an AUC infinity ranging between about 200 and about 400, about 210 and about 400, about 210 and about 398, about 220 and about 400, or about 220 and about 398 h*ng/mL (dose-normalized to 10 mg) when administered after at least a 10-hour fast.
  • the PK profile includes an AUC infinity ranging between about 300 and about 600, about 300 and 550, or about 320 and about 530 h*ng/mL (dose-normalized to 10 mg) when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • the PK profile includes an AUC last ranging between about 50 and about 800, about 100 and about 500, about 100 and about 480, about 100 and about 450, about 100 and about 400, about 110 and about 500, about 110 and about 480, about 110 and about 450, about 110 and about 400, about 150 and about 700, about 200 and about 700, about 200 and about 650, about 250 and about 450, about 280 and about 420, about 290 and about 410, or about 210 and about 650 h*ng/mL (dose-normalized to 10 mg).
  • the PK profile includes an AUC last ranging between about 300 and about 400 (dose-normalized to 10 mg).
  • the PK profile incudes a t max ranging between about 0.5 and about 5, between about 1 and about 4.5, about 1 and about 4, about 1 and about 3, about 1 and about 2.5, or about 1 and about 2 hours. In some embodiments, the PK profile includes a t max that ranges between about 1 and about 2.5, about 1 and about 2, or about 1 and about 3 hours when administered after at least a 10-hour fast. In some embodiments, the PK profile includes a t max that ranges between about 1 and about 4 hours when administered after about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • the PK profile incudes a t 1/2 ranging between about 5 and about 60, about 5 and about 55, about 5 and about 50, about 5 and about 45, about 5 and about 40, about 9 and about 60, about 9 and about 55, about 9 and about 50, about 9 and about 45, or about 9 and about 40 hours.
  • the PK profile includes a ⁇ z ranging between about 0.010 and about 0.080, about 0.010 and about 0.075, about 0.010 and about 0.070, about 0.015 and about 0.080, about 0.015 and about 0.075, about 0.015 and about 0.070, about 0.015 and about 0.065, about 0.015 and about 0.060, about 0.015 and about 0.055, or about 0.015 and about 0.050 l/hour.
  • the PK profile includes a CL/F ranging between about 10 and about 90, about 10 and about 85, about 10 and about 80, about 10 and about 75, about 10 and about 70, about 10 and about 60, about 10 and about 50, about 15 and about 90, about 15 and about 80, about 15 and about 70, about 15 and about 60, about 15 and about 50, about 20 and about 90, about 20 and about 80, about 20 and about 75, about 20 and about 70, about 20 and about 60, or about 20 and about 50 L/h.
  • the PK profile includes a Vd/F ranging between about 400 and about 6000, about 400 and about 5500, about 400 and about 5000, about 400 and about 4000, about 400 and about 3500, about 400 and about 3400, about 450 and about 3500, about 450 and about 3000, about 500 and about 3500, about 500 and about 3000, about 400 and about 2000, about 400 and about 1500, about 400 and about 1200, about 550 and about 3500, about 550 and about 3000, about 600 and about 3500, about 600 and about 3000, about 600 and about 2500, or about 450 and about 1200 L.
  • the PK profile may include a mean C max between about 20 and 45 ng/mL when dose-normalized to 10 mg.
  • the mean C max is about 20, about 21, about 22, about 23, about 24, about 25, about 26, about 27, about 28, about 29, about 30, about 31, about 32, about 33, about 34, about 35, about 36, about 37, about 38, about 39, about 40, about 41, about 42, about 43, about 44, or about 55 ng/mL (dose-normalized to 10 mg).
  • the mean C max is about 20 to about 40, about 20 to about 35, about 20 to about 30, about 20 to about 25, about 25 to about 45, about 25 to about 40, about 25 to about 35, about 25 to about 30, about 30 to about 45, about 30 to about 40, about 30 to about 35, about 35 to about 45, about 35 to about 40, or about 40 to about 45 ng/mL (dose-normalized to 10 mg).
  • the mean C max is between about 30 and 35 ng/mL, about 31 and 35 ng/mL, or about 31 and 34 ng/mL (dose-normalized to 10 mg) when administered after at least a 10-hour fast.
  • the mean C max is between about 35 and 40, about 36 and 39, or about 37 and 38 ng/mL (dose-normalized to 10 mg) when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • the PK profile also may have a mean AUC infinity between about 250 and 450 h*ng/mL (dose-normalized to 10 mg).
  • the AUC infinity is about 250, about 260, about 270, about 280, about 290, about 300, about 310, about 320, about 330, about 340, about 350, about 360, about 370, about 380, about 390, about 400, about 410, about 420, about 430, about 440, or about 450 h*ng/mL (dose-normalized to 10 mg).
  • the mean AUC infinity is about 250 to about 400, about 250 to about 375, about 250 to about 350, about 250 to about 325, about 250 to about 300, about 250 to about 275, about 275 to about 450, about 275 to about 425, about 275 to about 400, about 275 to about 375, about 275 to about 350, about 275 to about 325, about 275 to about 300, about 300 to about 450, about 300 to about 425, about 300 to about 400, about 300 to about 390, about 300 to about 380, about 300 to about 370, about 300 to about 360, about 300 to about 350, about 300 to about 340, about 300 to about 330, about 300 to about 320, about 300 to about 310, about 325 to about 450, about 325 to about 425, about 325 to about 400, about 325 to about 375, about 325 to about 350, about 350 to about 450, about 350 to about 425, about 400, about 350 to about 375, about 375 to about 375 to about 325 to
  • the mean AUC infinity is between about 300 and 320 h*ng/mL (dose-normalized to 10 mg) when administered after at least a 10-hour fast. In further embodiments, the mean AUC infinity is between about 320 and 530 h*ng/mL (dose-normalized to 10 mg) when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • the pharmaceutical composition has a PK profile comprising a mean AUC last between about 250 and 450 h*ng/mL (dose-normalized to 10 mg).
  • the AUC last is about 250, about 260, about 270, about 280, about 290, about 300, about 310, about 320, about 330, about 340, about 350, about 360, about 370, about 380, about 390, about 400, about 410, about 420, about 430, about 440, or about 450 h*ng/mL.
  • the mean AUC last is about 250 to about 400, about 250 to about 375, about 250 to about 350, about 250 to about 325, about 250 to about 300, about 250 to about 275, about 275 to about 450, about 275 to about 425, about 275 to about 400, about 275 to about 375, about 275 to about 350, about 275 to about 325, about 275 to about 300, about 300 to about 450, about 300 to about 425, about 300 to about 400, about 300 to about 390, about 300 to about 380, about 300 to about 370, about 300 to about 360, about 300 to about 350, about 300 to about 340, about 300 to about 330, about 300 to about 320, about 300 to about 310, about 325 to about 450, about 325 to about 425, about 325 to about 400, about 325 to about 375, about 325 to about 350, about 350 to about 450, about 350 to about 425, about 400, about 350 to about 375, about 375 to about 375 to about 325 to about
  • the pharmaceutical composition has a PK profile comprising a median t max between about 1 to 4 hours.
  • the median t max is about 1, about 1.1, about 1.2, about 1.3, about 1.4, about 1.5, about 1.6, about 1.7, about 1.8, about 1.9, about 2, about 2.1, about 2.2, about 2.3, about 2.4, about 2.5, about 2.6, about 2.7, about 2.8, about 2.9, about 3, about 3.1, about 3.2, about 3.3, about 3.4, about 3.5, about 3.6, about 3.7, about 3.8, about 3.9, or about 4 hours.
  • the median t max is about 1 to about 3.5, about 1 to about 3, about 1 to about 2.5, about 1 to about 2, about 1 to about 1.5, about 1.5 to about 4, about 1.5 to about 3.5, about 1.5 to about 3, about 1.5 to about 2.5, about 1.5 to about 2, about 2 to about 4, about 2 to about 3.5, about 2 to about 3, about 2 to about 2.5, about 2.5 to about 4, about 2.5 to about 3.5, about 2.5 to about 3, about 3 to about 4, about 3 to about 3.5, or about 3.5 to about 4 hours. In further embodiments, the median t max is about 1.5 hours.
  • the pharmaceutical composition comprises a PK profile of Treatment A, Treatment B, Treatment C, or Treatment D, as shown in Table 69.
  • the pharmaceutical composition has a PK profile including a mean C max of about 30, about 31, about 32, about 33, about 34, or about 35 ng/mL when administered after at least a 10-hour fast (dose-normalized to 10 mg).
  • the pharmaceutical composition comprises has a PK profile including a mean C max of about 31.2 ng/mL with standard deviation of about 6.9 ng/mL (dose-normalized to 10 mg).
  • the pharmaceutical composition comprises about 10 mg aticaprant and has a PK profile including a mean C max of about 34.1 ng/mL with standard deviation of about 10.0 ng/mL when administered after at least a 10-hour fast.
  • the pharmaceutical composition comprises about 5 mg aticaprant and has a PK profile including a mean Cmax of about 17.0 ng/mL with standard deviation of about 4.48 ng/mL when administered after at least a 10-hour fast.
  • the pharmaceutical composition has a PK profile including a mean Cmax of about 36, about 37, about 38, about 39, or about 35 ng/mL when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast (dose-normalized to 10 mg).
  • the pharmaceutical composition comprises about 10 mg aticaprant and has a PK profile including a mean Cmax of about 37.7 ng/mL with a standard deviation of about 9.18 ng/mL when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • the pharmaceutical composition has a PK profile comprising a mean AUCinfinity of about 300, about 305, about 310, about 315, or about 320 h*ng/mL when administered after a least a 10-hour fast (dose-normalized to 10 mg).
  • the pharmaceutical composition has a PK profile comprising a mean AUCinfinity of about 400, about 420, about 425, about 430, about 440, or about 450 h*ng/mL when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast (dose-normalized to 10 mg).
  • the pharmaceutical composition has a PK profile comprising a median t max of about 1.0, about 1.1, about 1.2, about 1.3, about 1.4, about 1.5, about 1.6, about 1.7, about 1.8, about 1.9, or about 2.0 hours when administered after at least a 10-hour fast. In some embodiments, the pharmaceutical composition has a PK profile comprising a median t max of about 1.5 hours when administered after at least a 10-hour fast.
  • the pharmaceutical composition has a PK profile comprising a median t of about 2.5, about 2.6, about 2.7, about 2.8, about 2.9 or about 3.0 hour when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast. In some embodiments, the pharmaceutical composition has a PK profile comprising a median t max of about 2.75 hours when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • the compositions contain a pharmaceutically acceptable excipient, one of which may be a filler.
  • the filler is the filler is microcrystalline cellulose, lactose monohydrate, or silicified microcrystalline cellulose, or a combination thereof.
  • the filler is microcrystalline cellulose.
  • the filler is lactose monohydrate.
  • the filler is silicified microcrystalline cellulose.
  • the composition comprises between about 10% to about 99.9% filler by weight, based on the weight of the composition.
  • the composition contains about 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, about 50, about 55, about 60, about 65, about 70, about 75, about 80, about 81, about 82, about 83, about 84, about 85, about 86, about 87, about 88, about 89, about 90, about 91, about 92, about 93, about 94, about 95, about 96, about 97, about 98, about 99, or about 99.9% by weight, based on the weight of the composition, of a filler
  • the composition comprises about 10 to about 90, about 10 to about 80, about 10 to about 70, about 10 to about 60, about 10 to about 50, about 10 to about 40, about 10 to about 30, about 10 to about 20, about 20 to about 99.9, about 20 to about 90, about 20 to about 80, about 20 to about 70, about 20 to about 60, about 20 to about 50, about 20 to about 40, about 20 to about 30, about 30 to about 99.9, about 30
  • the aticaprant to filler ratio is between about 0.005 and about 9 by weight. In some embodiments, the aticaprant to filler ratio is about 0.008 and 0.8 about by weight. In other embodiments, the aticaprant to filler ratio is about 0.005 to about 8, about 0.005 to about 7, about 0.005 to about 6, about 0.005 to about 5, about 0.005 to about 4, about 0.005 to about 3, about 0.005 to about 2, about 0.005 to about 1, about 0.005 to about 0.5, about 0.005 to about 0.1, about 0.005 to about 0.05, about 0.005 to about 0.01, about 0.01 to about 9, about 0.01 to about 8, about 0.01 to about 7, about 0.01 to about 6, about 0.01 to about 5, about 0.01 to about 4, about 0.01 to about 3, about 0.01 to about 2, about 0.01 to about 1, about 0.01 to about 0.5, about 0.01 to about 0.1, about 0.01 to about 0.05, about 0.05 to about 9, about 0.05 to about 8, about 0.05 to about 9, about 0.05 to
  • the composition may further comprise one or more of a filler, disintegrant, glidant, lubricant, solvent, coloring agent, binder. buffers, preservatives, penetration agents, wetting agents, surfactants, solubilizing agents, thickening agents, colorants, antioxidants, emulsifying agents, isotonizing agents, suspending agents, and/or viscosity increasing agents.
  • the composition further comprises one or more of a disintegrant.
  • disintegrants useful in the compositions include, e.g., the disintegrant is croscarmellose sodium.
  • the composition comprises between about 0.5% to about 50% by weight, based on the weight of the composition, of the disintegrant. In some embodiments, the composition comprises about 0.5, about 1, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, or about 50% by weight, based on the weight of the composition, of the disintegrant.
  • the composition comprises about 0.5 to about 40%, about 0.5 to about 30%, about 0.5 to about 20%, about 0.5 to about 10%, about 0.5 to about 5%, about 0.5 to about 4%, about 0.5 to about 3%, about 0.5 to about 2%, about 0.5 to about 1%, about 5 to about 50%, about 5 to about 40%, about 5 to about 30%, about 5 to about 20%, about 5 to about 10%, about 10 to about 50%, about 10 to about 40%, about 10 to about 30%, about 10 to about 20%, about 20 to about 50%, about 20 to about 40%, about 20 to about 30%, about 30 to about 50%, about 30 to about 40%, or about 40 to about 50% by weight, based on the weight of the composition of the disintegrant.
  • the composition comprises about 5% by weight, based on the weight of the composition, of the disintegrant.
  • the aticaprant to disintegrant ratio is between about 0.1 and 10 by weight. In some embodiments, the aticaprant to disintegrant ratio is about 0.1, about 0.5, about 1, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, or about 10 by weight.
  • the aticaprant to disintegrant ratio is about 0.1 to about 8, about 0.1 to about 7, about 0.1 to about 6, about 0.1 to about 5, about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 10, about 0.5 to about 9, about 0.5 to about 8, about 0.5 to about 7, about 0.5 to about 6, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 10, about 1 to about 9, about 1 to about 8, about 1 to about 7, about 1 to about 6, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 10, about 2 to about 9, about 2 to about 8, about 2 to about 7, about 2 to about 6, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 10, about 3 to about 9, about 3 to about 8, about 3 to about 7, about 6, about 3 to about 5, about 3 to about 4, about 4 to to to about 4 to to about
  • the composition further comprises one or more of a glidant.
  • glidants useful in the compositions include, e.g., silica, colloidal anhydrous.
  • the composition comprises between about 0.1% to about 10% glidant by weight, based on the weight of the composition. In some embodiment, the composition contains about 0.1, about 0.5, about 1, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, or about 10% by weight, based on the weight of the composition, of the glidant.
  • the composition contains about 0.1 to about 9, about 0.1 to about 8, about 0.1 to about 7, about 0.1 to about 6, about 0.1 to about 5, about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 10, about 0.5 to about 9, about 0.5 to about 8, about 0.5 to about 7, about 0.5 to about 6, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 10, about 1 to about 9, about 1 to about 8, about 1 to about 7, about 1 to about 6, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 10, about 2 to about 9, about 2 to about 8, about 2 to about 7, about 2 to about 6, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 10, about 3 to about 9, about 3 to about 8, about 3 to about 7, about 3, to about 3 to about 6, about 3 to about 6, about 3 to about 5, about 3 to about 4, about
  • the composition contains about 1% by weight, based on the weight of the composition, of the glidant.
  • the aticaprant to glidant ratio is between 0.5 and 50 by weight. In some embodiments, the aticaprant to glidant ratio is about 0.5, about 1, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, or about 50 by weight.
  • the aticaprant to glidant ratio is about 0.5 to about 50, about 0.5 to about 45, about 0.5 to about 40, about 0.5 to about 35, about 0.5 to about 30, about 0.5 to about 25, about 0.5 to about 20, about 0.5 to about 15, about 0.5 to about 10, about 0.5 to about 5, about 0.5 to about 1, about 1 to about 50, about 1 to about 45, about 1 to about 40, about 1 to about 35, about 1 to about 30, about 1 to about 25, about 1 to about 20, about 1 to about 15, about 1 to about 10, about 1 to about 5, about 5 to about 50, about 5 to about 45, about 5 to about 40, about 5 to about 35, about 5 to about 30, about 5 to about 25, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 50, about 10 to about 45, about 10 to about 40, about 10 to about 35, about 10 to about 30, about 10 to about 25, about 10 to about 20, about 10 to about 15, about 20 to about 50, about 20 to about 40, about 20 to about 30, about 30 to about about
  • the composition further comprises one or more of a lubricant.
  • lubricants useful in the compositions include, e.g., the lubricant is magnesium stearate.
  • the composition comprises between about 0.05% to about 5% lubricant by weight, based on the weight of the composition. In some embodiments, the composition comprises about 0.05, about 0.1, about 0.5, about 1, about 1.5, about 2, about 2.5, about 3, about 3.5, about 4, about 4.5 or about 5% by weight, based on the weight of the composition, of lubricant.
  • the composition comprises about 0.05 to about 4.5, about 0.05 to about 4, about 0.05 to about 3, about 0.05 to about 2, about 0.05 to about 1, about 0.05 to about 0.5, about 0.05 to about 0.1, about 0.1 to about 5, about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 5, about 3 to about 4, or about 4 to about 5% by weight, based on the weight of the composition, of lubricant.
  • the composition comprises about 0.5% by weight, based on the weight of the composition, of the lubricant.
  • the aticaprant to lubricant ratio is between about 1 and about 100 by weight. In some embodiments, the aticaprant to lubricant ratio is about 1, about 5, 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, about 50, about 55, about 60, about 65, about 70, about 75, about 80, about 85, about 90, about 95, or about 100 by weight.
  • the aticaprant to lubricant ratio is 1 to about 90, about 1 to about 80, about 1 to about 70, about 1 to about 60, about 1 to about 50, about 1 to about 40, about 1 to about 30, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 5 to about 100, about 1 to about 90, about 1 to about 80, about 1 to about 70, about 1 to about 60, about 1 to about 50, about 1 to about 40, about 1 to about 30, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 5 to about 100, about 5 to about 90, about 5 to about 80, about 5 to about 70, about 5 to about 60, about 5 to about 50, about 5 to about 40, about 5 to about 30, about 5 to about 20, about 5 to about 10, about 10 to about 100, about 10 to about 90, about 10 to about 80, about 10 to about 70, about 10 to about 60, about 10 to about 50, about 10 to about 40, about 10 to about 30, about 10 to about 20, about 20 to about 100, about 20 to about 90,
  • the composition comprises one or more of an aticaprant to filler ratio between 0.005 and 9 by weight; an aticaprant to disintegrant ratio between 0.1 and 10 by weight; an aticaprant to glidant ratio between 0.5 and 50 by weight; and an aticaprant to lubricant ratio between 1 and 100 by weight.
  • the composition comprises one or more of an aticaprant to filler ratio of about 0.06 by weight; an aticaprant to disintegrant ratio of about 1 by weight; an aticaprant to glidant ratio of about 5 by weight; and an aticaprant to lubricant ratio of about 10 by weight.
  • the composition comprises about 5% by weight of aticaprant, about 88.5% by weight of filler, about 5% by weight of disintegrant by weight, about 1% by weight of glidant, and about 0.5% by weight of lubricant, based on the weight of the composition.
  • the composition is formulated as a solid composition.
  • the solid composition is a tablet, capsule, or caplet.
  • the solid composition is a tablet such as an oral tablet.
  • the solid composition is a capsule such as an oral capsule.
  • the solid composition is a caplet such as an oral caplet.
  • the solid compositions are coated.
  • the coating is an enteric coating. By doing so, the coating provides a film coat on the solid composition.
  • the film coat comprises a coating powder.
  • the film coat comprises Opadry II Orange.
  • the coating powder is Opadry II Orange.
  • the tablet may comprise one or more layers.
  • the tablet comprises a core tablet and a film coat to provide a film coated tablet.
  • the ratio of the film coat to core tablet is between about 0.03 to 10 by weight. In some embodiments, the ratio of the film coat to core tablet is about 0.03, 0.05, 0.08, 0.1, 0.5, 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 by weight, based on the weigh of the composition.
  • the ratio of the film coat to core tablet is about 0.03 to about 9, about 0.03 to about 8, about 0.03 to about 7, about 0.03 to about 6, about 0.03 to about 6, about 0.03 to about 5, about 0.03 to about 4, about 0.03 to about 3, about 0.03 to about 2, about 0.03 to about 1, about 0.03 to about 0.5, about 0.03 to about 0.1, about 0.05 to about 10, 0.05 to about 9, about 0.05 to about 8, about 0.05 to about 7, about 0.05 to about 6, about 0.05 to about 6, about 0.05 to about 5, about 0.05 to about 4, about 0.05 to about 3, about 0.05 to about 2, about 0.05 to about 1, about 0.05 to about 0.5, about 0.05 to about 0.1, about 0.1 to about 10, 0.1 to about 9, about 0.1 to about 8, about 0.1 to about 7, about 0.1 to about 6, about 0.1 to about 6, about 0.1 to about 5, about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, 0.05 to about 0.1, about 0.1 to about 10,
  • the core tablet may contain one or more phases.
  • the core tablet comprises a first phase such as an intragranular phase.
  • the core tablet comprises a second phase such as an extragranular phase.
  • the core tablet comprises intragranular and extragranular phases.
  • the ratio of the intragranular phase to extragranular phase in the core tablet is between about 1.5 and about 3 by weight. In some embodiments, the ratio of the intragranular phase to extragranular phase in the core tablet is about 1.5, about 1.6, about 1.7, about 1.8, about 1.9, about 2, about 2.1, about 2.2, about 2.3, about 2.4, about 2.5, about 2.6, about 2.7, about 2.8, about 2.9, or about 3 by weight.
  • the ratio of the intragranular phase to extragranular phase in the core tablet is about 1.5 to about 2.8, about 1.5 to about 2.5, about 1.5 to about 2.3, about 1.5 to about 2, about 1.5 to about 1.8, about 1.8 to about 3, about 1.8 to about 2.8, about 1.8 to about 2.5, about 1.8 to about 2.3, about 2 to about 3, about 2 to about 2.8, about 2 to about 2.5, about 2 to about 2.3, about 2 to about 2.1, about 2.1 to about 3, about 2.1 to about 2.8, about 2.1 to about 2.5, about 2.1 to about 2.3, about 2.3 to about 3, about 2.3 to about 2.8, about 2.3 to about 2.5 to about 2.5 to about 3, about 2.5 to about 2.8, and about 2.8 to about 3 by weight.
  • the ratio of the intragranular phase to extragranular phase in the core tablet is about 2.1 by weight.
  • the solid composition contains aticaprant and one or more pharmaceutically acceptable excipients.
  • the intragranular phase comprises aticaprant, a filler, a disintegrant, and a glidant.
  • the intragranular phase comprises one filler.
  • the intragranular phase comprises two fillers.
  • the intragranular phase comprises about 10 to about 120 mg of the filler. In some embodiments, the intragranular phase comprises about 10, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, about 100, about 110, or about 120 mg of the filler.
  • the intragranular phase comprises about 10 to about 110, about 10 to about 100, about 10 to about 90, about 10 to about 80, about 10 to about 70, about 10 to about 60, about 10 to about 50, about 10 to about 40, about 10 to about 30, about 10 to about 20, about 20 to about 120, about 20 to about 110, about 20 to about 100, about 20 to about 90, about 20 to about 80, about 20 to about 70, about 20 to about 60, about 20 to about 50, about 20 to about 40, about 20 to about 30, about 30 to about 120, about 30 to about 110, about 30 to about 100, about 30 to about 90, about 30 to about 80, about 30 to about 70, about 30 to about 60, about 30 to about 50, about 30 to about 40, about 40 to about 120, about 40 to about 110, about 40 to about 100, about 40 to about 90, about 40 to about 80, about 40 to about 70, about 40 to about 60, about 40 to about 50, about 50 to about 100, about 50 to about 90, about
  • the intragranular phase contains about 60 mg of filler. In yet other embodiments, the intragranular phase contains about 30 mg of microcrystalline cellulose. In still further embodiments, the intragranular phase contains about 30 mg of lactose monohydrate. In other embodiments, the intragranular phase contains about 60 mg of microcrystalline cellulose. In further embodiments, the intragranular phase contains about 60 mg of lactose monohydrate.
  • the intragranular phase comprises an aticaprant to filler ratio of between about 0.008 and 0.8 by weight.
  • the intragranular phase contains an aticaprant to filler ratio of about 0.008, about 0.005, about 0.001, about 0.01, about 0.05, about 0.1, about 0.2, about 0.3, about 0.4, about 0.5, about 0.6, about 0.7, or about 0.8 by weight.
  • the intragranular phase comprises an aticaprant to filler ratio of about 0.008 to about 0.7, about 0.008 to about 0.6, about 0.008 to about 0.5, about 0.008 to about 0.6, about 0.008 to about 0.5, about 0.008 to about 0.4, about 0.008 to about 0.3, about 0.008 to about 0.2, about 0.008 to about 0.1, about 0.008 to about 0.05, about 0.008 to about 0.01, about 0.01 to about 0.8, about 0.01 to about 0.7, 0.01 to about 0.6, about 0.01 to about 0.5, about 0.01 to about 0.4, about 0.01 to about 0.5, about 0.01 to about 0.4, about 0.01 to about 0.3, about 0.01 to about 0.2, about 0.01 to about 0.1, about 0.01 to about 0.05, about 0.05 to about 0.8, about 0.05 to about 0.9, about 0.05 to about 0.8, about 0.05 to about 0.7, about 0.05 to about 0.6, about 0.05 to about 0.6, about 0.05 to
  • the intragranular phase also may contain a disintegrant.
  • the intragranular phase contains about 1 to about 10 mg of the disintegrant.
  • the intragranular phase contains about 1, about 1.5, about 2, about 2.5, about 3, about 3.5, about 4, about 4.5, about 5, about 5.5, about 6, about 6.5, 7, about 7.5, about 8, about 8.5, about 9, about 9.5 or about 10 mg of the disintegrant.
  • the intragranular phase contains about 1 to about 9, about 1 to about 8, about 1 to about 7, about 1 to about 6, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 10, about 2 to about 9, about 2 to about 8, about 2 to about 7, about 2 to about 6, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 2.5 to about 10, about 2.5 to about 9, about 2.5 to about 8, about 2.5 to about 7, about 2.5 to about 6, about 2.5 to about 5, about 2.5 to about 4, about 2.5 to about 3, about 3 to about 10, about 3 to about 9, about 3 to about 8, about 3 to about 7, about 3 to about 6, about 3 to about 5, about 3 to about 4, about 4 to about 10, about 4 to about 9, about 4 to about 8, about 4 to about 7, about 4 to about 6, about 4 to about 5, about 5 to about 10, about 5 to about 9, about 5 to about 8, about 5 to about 7, about 5 to about 6, about 6 to about 10, about 6 to about 9, about 6 to about 8, about 6 to about 7, about 7 to about 10, about 7 to about 9, about 7 to about 9, about 7 to
  • the intragranular phase contains about 2.5 mg of the disintegrant. In still further embodiments, the intragranular phase contains about 5 mg of the disintegrant. In other embodiments, the intragranular phase contains about 2.5 mg of croscarmellose sodium. In further embodiments, the intragranular phase contains about 5 mg of croscarmellose sodium.
  • the intragranular phase may further contain a glidant.
  • the intragranular phase contains about 0.1 to about 5 mg of a glidant.
  • the intragranular phase contains about 0.1, about 0.5, about 1, about 1.5, about 2, about 2.5, about 3, about 3.5, about 4, about 4.5, or about 5 mg of a glidant.
  • the intragranular phase contains about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 5, about 3 to about 4, or about 4 to about 5 mg of a glidant.
  • the intragranular phase contains about 0.5 mg of the glidant.
  • the intragranular phase contains about 1 mg of the glidant.
  • the intragranular phase contains about 0.5 mg of silica, colloidal anhydrous.
  • the intragranular phase contains about 1 mg of silica, colloidal anhydrous.
  • the intragranular phase has an aticaprant to disintegrant ratio of between about 0.2 and 20 by weight; In some embodiments, the intragranular phase has an aticaprant to disintegrant ratio of about 0.2, about 0.3, about 0.4, about 0.5, about 0.6, about 0.7, about 0.8, about 0.9, about 1, about 1.1, about 1.2, about 1.3, about 1.4, about 1.5, about 1.6, about 1.7, about 1.8, about 1.9, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 11, about 12, about 13, about 14, about 15, about 16, about 17, about 18, about 19, or about 20 by weight.
  • the intragranular phase comprises an aticaprant to disintegrant ratio of about 0.2 to about 18, about 0.2 to about 16, about 0.2 to about 14, about 0.2 to about 12, about 0.2 to about 10, about 0.2 to about 8, about 0.2 to about 6, about 0.2 to about 4, about 0.2 to about 3, about 0.2 to about 2, about 0.2 to about 1, about 0.2 to about 0.5, about 0.5 to about 20, about 0.5 to about 18, about 0.5 to about 16, about 0.5 to about 14, about 0.5 to about 12, about 0.5 to about 10, about 0.5 to about 8, about 0.5 to about 6, about 0.5 to about 4, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 20, about 1 to about 18, about 1 to about 16, about 1 to about 14, about 1 to about 12, about 1 to about 10, about 1 to about 8, about 1 to about 6, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 1 to about 1.5, about 2 to about 20, about 2 to about 18, about 2 to about 16, about 2 to about 14, about 2 to about 12, about 2 to about 10, about 2 to about 10, about
  • the intragranular phase comprises an aticaprant to glidant ratio of between about 1 and 100 by weight. In some embodiments, the intragranular phase comprises an aticaprant to glidant ratio of about 1, about 5, about 10, about 15, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, or about 100 by weight.
  • the intragranular phase comprises an aticaprant to glidant ratio of about 1 to about 80, about 1 to about 60, about 1 to about 40, about 1 to about 20, about 1 to about 15, about 1 to about 10, about 1 to about 5, about 2 to about 80, about 2 to about 60, about 2 to about 40, about 2 to about 20, about 2 to about 15, about 2 to about 10, about 2 to about 5, about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 80, about 40 to about 60, or about 60 to about 80 by weight.
  • the intragranular phase comprises an aticaprant to glidant ratio of 10 by weight.
  • the extragranular phase comprises one or more of a filler, a disintegrant, a glidant, and a lubricant.
  • the extragranular phase comprises a filler.
  • the extragranular phase comprises a disintegrant.
  • the extragranular phase comprises a glidant.
  • the extragranular phase comprises a lubricant.
  • the extragranular phase may comprise a filler.
  • the extragranular phase contains one filler.
  • the extragranular phase contains about 10 to about 80 mg of a filler.
  • the extragranular phase contains about 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, about 50, about 55, about 60, about 70, or about 80 mg of a filler.
  • the extragranular phase contains about 10 to about 70, about 10 to about 60, about 10 to about 50, about 10 to about 40, about 10 to about 30, about 10 to about 20, about 10 to about 15, about 15 to about 80, about 15 to about 70, about 15 to about 60, about 15 to about 50, about 15 to about 40, about 15 to about 30, about 15 to about 20, about 20 to about 80, about 20 to about 70, about 20 to about 60, about 20 to about 50, about 20 to about 40, about 20 to about 30, about 25 to about 80, about 25 to about 70, about 25 to about 60, about 25 to about 50, about 25 to about 40, about 25 to about 30, about 30 to about 80, about 30 to about 70, about 30 to about 60, about 30 to about 50, about 30 to about 40, about 35 to about 80, about 35 to about 70, about 35 to about 60, about 35 to about 50, about 35 to about 40, about 40 to about 80, about 40 to about 70, about 40 to about 60, about 40 to about 50, about 40 to about 80, about 40 to about 70, about 40 to
  • the extragranular phase contains about 28.5 mg of the filler. In other embodiments, the extragranular phase contains about 28.5 of silicified microcrystalline cellulose. In further embodiments, the extragranular phase contains about 57 mg of the filler. In still other embodiments, the extragranular phase contains about 57 mg of silicified microcrystalline cellulose.
  • the extragranular phase may additionally contain a disintegrant.
  • the disintegrant is croscarmellose sodium.
  • the extragranular phase contains about 1 to about 10 mg of a disintegrant.
  • the extragranular phase contains about 1, about 2, about 2.5, about 3, about 4, about 5, about 6, about 7, about 7.5, about 8, about 9, or about 10 mg of a disintegrant.
  • the extragranular phase contains about 1 to about 10, about 1 to about 9, about 1 to about 8, about 1 to about 7, about 1 to about 6, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2.5, about 1 to about 2, about 2 to about 10, about 2 to about 9, about 2 to about 8, about 2 to about 7, about 2 to about 6, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 2.5 to about 10, about 2.5 to about 9, about 2.5 to about 8, about 2.5 to about 7, about 2.5 to about 6, about 2.5 to about 5, about 2.5 to about 4, about 2.5 to about 3, about 3 to about 10, about 3 to about 9, about 3 to about 8, about 3 to about 7, about 3 to about 6, about 3 to about 5, about 3 to about 4, about 4 to about 10, about 4 to about 9, about 4 to about 8, about 4 to about 7, about 4 to about 6, about 4 to about 5, about 5 to about 10, about 5 to about 9, about 5 to about 8, about 5 to about 7, about 6 to about 10, about 9, about 6 to about 8, about 6 to about 9, about 6 to about 8, about 6 to about 7, about 7 about 7 about
  • the extragranular phase contains about 2.5 mg of a disintegrant. In other embodiments, the extragranular phase contains about 5 mg of a disintegrant. In further embodiments, the extragranular phase contains about 2.5 mg of croscarmellose sodium. In still other embodiments, the extragranular phase contains about 5 mg of croscarmellose sodium.
  • the extragranular phase comprises a filler to disintegrant ratio of between about 1 and 100 by weight. In some embodiments, the extragranular phase comprises a filler to disintegrant ratio of 1, 5, 10, 20, 30, 40, 50, 60, 70, 80, 90, or 100 by weight.
  • the extragranular phase comprises a filler to disintegrant ratio of about 1 to about 90, about 1 to about 80, about 1 to about 70, about 1 to about 60, about 1 to about 50, about 1 to about 40, about 1 to about 30, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 5 to about 100, about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 10 to about 15, about 20 to about 100, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 100, about 40 to about 80, about 40 to about 60, about 60 to about 100, about 60 to about 80, or about 80 to about 100 by weight.
  • the extragranular phase comprises a filler to disintegrant ratio of about 11.4.
  • the extragranular phase further may contain a glidant.
  • the glidant is silica, colloidal anhydrous.
  • the extragranular phase contains about 0.1 to about 5 mg of the glidant.
  • the extragranular phase contains about 0.1, 0.25, 0.5, 0.75, 1, 2, 3, 4, or 5 mg of a glidant.
  • the extragranular phase contains about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 5, about 3 to about 4, or about 4 to about 5 mg of a glidant.
  • the extragranular phase contains about 0.5 mg of a glidant.
  • the extragranular phase contains about 1 mg of a glidant.
  • the extragranular phase contains about 0.5 mg of silica, colloidal anhydrous.
  • the extragranular phase contains about 1 mg of silica, colloidal anhydrous.
  • the extragranular phase comprises a filler to glidant ratio of between about 5 and 500 by weight. In other embodiments, the extragranular phase comprises a filler to glidant ratio of about 5, about 10, about 25, about 50, about 100, about 150, about 200, about 250, about 300, about 350, about 400, about 450, or about 500.
  • the extragranular phase comprises a filler to glidant ratio of about 5 to about 400, about 5 to about 300, about 5 to about 200, about 5 to about 100, about 5 to about 75, about 5 to about 50, about 10 to about 500, about 10 to about 400, about 10 to about 300, about 10 to about 200, about 10 to about 100, about 10 to about 50, about 25 to about 500, about 25 to about 400, about 25 to about 300, about 25 to about 200, about 25 to about 100, about 25 to about 75, about 25 to about 50, about 50 to about 500, about 50 to about 400, about 50 to about 300, about 50 to about 200, about 50 to about 100, about 100 to about 500, about 100 to about 400, about 100 to about 300, about 100 to about 200, about 200 to about 500, about 200 to about 400, about 200 to about 300, about 300 to about 500, about 300 to about 400, or about 400 to about 500 by weight.
  • the extragranular phase comprises a filler to glidant ratio of about 57
  • the extragranular phase may also contain a lubricant.
  • the lubricant is magnesium stearate.
  • the extragranular phase contains about 0.1 to about 5 mg of the lubricant.
  • the extragranular phase contains about 0.1, 0.25, 0.5, 0.75, 1, 2, 3, 4, or 5 mg of a lubricant.
  • the extragranular phase contains about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 5, about 3 to about 4, or about 4 to about 5 mg of a lubricant.
  • the extragranular phase contains about 0.5 mg of a lubricant.
  • the extragranular phase contains about 1 mg of a lubricant.
  • the extragranular phase contains about 0.5 mg of magnesium stearate.
  • the extragranular phase contains about 1 mg of magnesium stearate.
  • the extragranular phase comprises a filler to lubricant ratio of between about 5 and 500 by weight. In other embodiments, the extragranular phase comprises a filler to lubricant ratio of about 5, about 10, about 25, about 50, about 100, about 150, about 200, about 250, about 300, about 350, about 400, about 450, or about 500.
  • the extragranular phase comprises a filler to lubricant ratio of about 5 to about 400, about 5 to about 300, about 5 to about 200, about 5 to about 100, about 5 to about 75, about 5 to about 50, about 10 to about 500, about 10 to about 400, about 10 to about 300, about 10 to about 200, about 10 to about 100, about 10 to about 50, about 25 to about 500, about 25 to about 400, about 25 to about 300, about 25 to about 200, about 25 to about 100, about 25 to about 75, about 25 to about 50, about 50 to about 500, about 50 to about 400, about 50 to about 300, about 50 to about 200, about 50 to about 100, about 100 to about 500, about 100 to about 400, about 100 to about 300, about 100 to about 200, about 200 to about 500, about 200 to about 400, about 200 to about 300, about 300 to about 500, about 300 to about 400, or about 400 to about 500 by weight.
  • the extragranular phase comprises a filler to lubricant ratio of about 57
  • the intragranular phase comprises one or more of: an aticaprant to filler ratio of between about 0.008 and 0.8 by weight; an aticaprant to disintegrant ratio of between about 0.2 and 20 by weight; and an aticaprant to glidant ratio of between about 1 and 100 by weight.
  • the extragranular phase comprises one or more of: a filler to disintegrant ratio of between about 1 and 100 by weight; a filler to glidant ratio of between about 5 and 500 by weight; and a filler to lubricant ratio of between about 5 and 500 by weight.
  • the extragranular phase comprises a filler to disintegrant ratio of about 11.4 by weight.
  • the extragranular phase comprises a filler to glidant ratio of about 57 by weight.
  • the extragranular phase comprises a filler to lubricant ratio of about 57 by weight.
  • the core tablet comprises about 5% aticaprant by weight, about 88.5% filler by weight, about 5% disintegrant by weight, about 1% glidant by weight, and about 0.5% lubricant by weight.
  • the oral tablet may be of weight that is suitable for administration by a patient.
  • the oral tablet has a core tablet of about 10 to about 1000 mg.
  • the core tablet is about 10, about 25, about 50, about 100, about 200, about 300, about 400, about 500, about 600, about 700, about 800, about 900, or about 1000 mg.
  • the core tablet is about 10 to about 900, about 10 to about 800, about 10 to about 700, about 10 to about 600, about 10 to about 500, about 10 to about 400, about 10 to about 300, about 10 to about 200, about 10 to about 100, about 10 to about 50, about 25 to about 1000, about 25 to about 900, about 25 to about 800, about 25 to about 700, about 25 to about 600, about 25 to about 500, about 25 to about 400, about 25 to about 300, about 25 to about 200, about 25 to about 100, about 25 to about 75, about 50 to about 1000, about 50 to about 900, about 50 to about 800, about 50 to about 700, about 50 to about 600, about 50 to about 500, about 50 to about 400, about 50 to about 300, about 50 to about 200, about 50 to about 100, about 100 to about 1000, about 100 to about 900, about 100 to about 800, about 100 to about 700, about 100 to about 600, about 100 to about 500, about 100 to about 400, about 100 to about 300, about 100 to about 200, about 200, about 50 to
  • the core tablet contains a disintegrant.
  • the core tablet contains about 5 to about 100 mg of a disintegrant.
  • the core tablet contains about 5, about 10, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, or about 100 mg of a disintegrant.
  • the core tablet contains about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 100, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 20 to about 100, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 100, about 40 to about 80, about 40 to about 60, about 60 to about 100, about 60 to about 80, or about 80 to about 100 mg of a disintegrant.
  • the core tablet contains about 5 mg of the disintegrant.
  • the core tablet contains about 10 mg of the disintegrant.
  • the core tablet contains a glidant.
  • the core tablet contains about 1 to about 100 mg of a glidant.
  • the core tablet contains about 1, about 2, about 3, about 4, about 5, about 10, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, or about 100 mg of a glidant.
  • the core tablet contains about 1 to about 100, about 1 to about 80, about 1 to about 60, about 1 to about 40, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 2 to about 100, about 2 to about 80, about 2 to about 60, about 2 to about 40, about 2 to about 20, about 2 to about 10, about 2 to about 5, about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 100, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 20 to about 100, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 100, about 40 to about 80, about 40 to about 60, about 60 to about 100, about 60 to about 80, or about 80 to about 100 mg of a glidant. In further embodiments, the core tablet contains about 1 mg of the glidant. In yet other embodiments, the core tablet contains about 2 mg of the glid
  • the core tablet contains a lubricant.
  • the core tablet contains about 0.5 to about 100 mg of a lubricant.
  • the core tablet contains about 0.5, about 1, about 2, about 3, about 4, about 5, about 10, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, or about 100 mg of a lubricant.
  • the core tablet contains about 0.5 to about 80, about 0.5 to about 60, about 0.5 to about 40, about 0.5 to about 20, about 0.5 to about 10, about 0.5 to about 5, about 0.5 to about 1, about 1 to about 100, about 1 to about 80, about 1 to about 60, about 1 to about 40, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 2 to about 100, about 2 to about 80, about 2 to about 60, about 2 to about 40, about 2 to about 20, about 2 to about 10, about 2 to about 5, about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 100, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 20 to about 100, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 100, about 40 to about 80, about 40 to about 60, about 60 to about 100, about 60 to about 80, or about 80 to about 100 mg
  • the core tablet contains a filler.
  • the core tablet contains about 1 to about 200 mg of a filler.
  • the core tablet contains about 1, about 2, about 3, about 4, about 5, about 10, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, about 100, about 110, about 120, about 130, about 140, about 150, about 160, about 170, about 180, about 190, or about 200 mg of a filler.
  • the core tablet contains about 1 to about 180, about 1 to about 160, about 1 to about 140, about 1 to about 120, 1 to about 100, about 1 to about 80, about 1 to about 60, about 1 to about 40, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 2 to about 200, about 2 to about 180, about 2 to about 160, about 2 to about 140, about 2 to about 120, about 2 to about 100, about 2 to about 80, about 2 to about 60, about 2 to about 40, about 2 to about 20, about 2 to about 10, about 2 to about 5, about 5 to about 200 m, about 5 to about 180, about 5 to about 160, about 5 to about 140, about 5 to about 120, about 5 to about 100, about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 200, about 10 to about 180, about 10 to about 160, about 10 to about 140, about 10 to about 120, about 10 to about 100, about 10 to about 80, about 10 to about 10 to
  • the oral tablet comprises a core tablet of about 100 mg and comprising about 5 mg aticaprant, about 5 mg disintegrant, about 88.5 mg filler, about 1 mg glidant, and about 0.5 mg lubricant.
  • oral tablet comprising a core tablet of about 200 mg, the core tablet comprising about 10 mg aticparant, about 10 mg disintegrant, about 177 mg filler, about 2 mg glidant, and about 1 mg lubricant.
  • the core tablet may be coated with a film coat.
  • the oral tablet comprises about 3 mg of film coat. In other embodiments, the oral tablet comprises about 6 mg of film coat.
  • the film coated oral tablet comprises about 80 to about 99.9% by weight of the core tablet and about 0.1 to about 20% by weight, based on the weight of the film coated oral tablet, of the core tablet.
  • the film coated oral tablet comprises about 80, about 81, about 82, about 83, about 84, about 85, about 86, about 87, about 88, about 89, about 90, about 91, about 92, about 93, about 94, about 95, about 96, about 97, about 98, about 99, or 99.9% by weight, based on the weight of the film coated oral tablet.
  • the film coated oral tablet comprises about 80 to about 99, about 80 to about 96, about 80 to about 94, about 80 to about 92, about 80 to about 90, about 80 to about 88, about 80 to about 86, about 80 to about 84, about 80 to about 82, about 82 to about 99, about 82 to about 96, about 82 to about 94, about 82 to about 92, about 82 to about 90, about 82 to about 88, about 82 to about 86, about 82 to about 84, about 84 to about 99, about 84 to about 99, about 84 to about 96, about 84 to about 94, about 84 to about 92, about 84 to about 90, about 84 to about 88, about 84 to about 86, about 86 to about 99, about 86 to about 96, about 86 to about 94, about 86 to about 92, about 86 to about 90, about 86 to about 92, about 86 to about 90, about 86 to about 88, about 88
  • the film coated oral tablet comprises about 97% core tablet by weight, based on the weight of the film coated oral tablet. In yet other embodiments, the film coated oral tablet comprises about 0.1 to about 20% by weight, based on the weight of the film coated oral tablet, of film coat. In still further embodiments, film coated oral tablet comprises about 0.1, about 0.5, about 1, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 11, about 12, about 13, about 14, about 15, about 16, about 17, about 18, about 19, or about 20% by weight, based on the weight of the film coated oral tablet, of the film coat.
  • the film coated oral tablet comprises about 0.1 to about 18, about 0.1 to about 16, about 0.1 to about 14, about 0.1 to about 12, about 0.1 to about 10, about 0.1 to about 8, about 0.1 to about 6, about 0.1 to about 4, about 0.1 to about 2, about 0.1 to about 1, about 0.5 to about 20, about 0.5 to about 18, about 0.5 to about 16, about 0.5 to about 14, about 0.5 to about 12, about 0.5 to about 10, about 0.5 to about 8, about 0.5 to about 6, about 0.5 to about 4, about 0.5 to about 2, about 1 to about 20, about 1 to about 18, about 1 to about 16, about 1 to about 14, about 1 to about 12, about 1 to about 10, about 1 to about 8, about 1 to about 6, about 1 to about 4, about 1 to about 2, about 2 to about 20, about 2 to about 18, about 2 to about 16, about 2 to about 14, about 2 to about 12, about 2 to about 10, about 2 to about 8, about 2 to about 8, about 2 to about 6, about 2, about 4 to about 20, about 4 to about 18, about 18, about 4 to about 16, about 4 to about 12, about 4 to about 18, about 18, about 16,
  • the film coated oral tablet comprises about 3% by weight, based on the weight of the film coated oral tablet, of the film coat. In yet other embodiments, the film coated oral tablet comprises about 97% core tablet by weight and about 3% film coat by weight, based on the weight of the film coated oral tablet.
  • the disclosure provides oral tablets comprising about 5 mg aticaprant, wherein the oral tablet comprises a core tablet of about 100 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 30 mg microcrystalline cellulose, about 30 mg lactose monohydrate, about 2.5 mg croscarmellose sodium, and about 0.5 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 28.5 mg silicified microcrystalline cellulose, about 2.5 mg croscarmellose sodium, about 0.5 mg silica, colloidal anhydrous, and about 0.5 mg magnesium stearate.
  • the disclosure provides oral tablets comprising about 10 mg aticaprant, wherein the oral tablet comprises a core tablet of about 200 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 60 mg microcrystalline cellulose, about 60 mg lactose monohydrate, about 5 mg croscarmellose sodium, and about 1 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 57 mg silicified microcrystalline cellulose, about 5 mg croscarmellose sodium, about 1 mg silica, colloidal anhydrous, and about 1 mg magnesium stearate.
  • the solid compositions may also have a desirable dissolution profile that provide the desired release of aticaprant.
  • the solid composition contains about 2 mg and 20 mg of aticaprant and has a dissolution profile comprising a Q value of between about 60% and 90% at 45 minutes, under the dissolution operating conditions of (i) apparatus: Paddle (USP Type 2, Ph. Eur., JP), (ii) dissolution medium: 0.01 M hydrochloric acid, (iii) volume: 900 mL, (iv) temperature: 37 ⁇ 0.5° C., (v) rotation speed: 50 rpm, and (vi) analytical finish: UHPLC with UV detection at 247 nm.
  • the Q value is about 60, about 61, about 62, about 63, about 64, about 65, about 66, about 67, about 68, about 69, about 70, about 71, about 72, about 73, about 74, about 75, about 75, about 76, about 77, about 78, about 79, about 80, about 81, about 82, about 83, about 84, about 85, about 86, about 87, about 88, about 89, about 90, about 91, about 92, about 93, about 94, or about 95% at 45 minutes.
  • the Q value is about 60 to about 85, about 60 to about 80, about 60 to about 75, about 60 to about 70, about 70 to about 90, about 70 to about 85, about 70 to about 80, about 70 to about 75, about 75 to about 90, about 75 to about 85, about 75 to about 80, about 80 to about 90, about 80 to about 85, or about 85 to about 90% at 45 minutes.
  • the Q value is between about 70% and 80% at 45 minutes. In other aspects, the Q value is about 75% at 45 minutes.
  • Aticaprant may be administered once daily, or the total daily dosage may be administered in divided doses of two, three or four times daily.
  • the composition containing aticaprant is administered once daily.
  • the oral tablet containing aticaprant is administered once daily.
  • the solid pharmaceutical composition containing anticaprant is administered once daily.
  • the disclosure relates to aticaprant, for use as described herein, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with aticaprant.
  • the disclosure also relates to the use of aticaprant in the manufacture of a medicament, as described herein, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with of aticaprant.
  • the disclosure further relates to a package or pharmaceutical product as described herein, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with aticaprant.
  • antidepressant therapy can be in particular selected from a selective serotonin reuptake inhibitor (SSRI), serotonin-norepinephrine reuptake inhibitor (SNRI), or a combination thereof.
  • Aticaprant may be used as adjunctive treatment, or in other words, in conjunction, as an add-on, or in combination with one or more antidepressants, for example, the patient may be already, or also, administered one or more antidepressants.
  • the disclosure relates to aticaprant, for use as described herein, comprising administration of aticaprant, as adjunctive treatment with an effective amount of one or more antidepressants.
  • the disclosure relates to aticaprant, for use as described herein, comprising administration of aticaprant, in conjunction with an effective amount of one or more antidepressants.
  • the disclosure relates to aticaprant, for use as described herein, comprising administration of aticaprant, in combination with an effective amount of one or more antidepressants.
  • the disclosure also relates to the use of aticaprant, in the manufacture of a medicament, as described herein, wherein the treatment comprises administration of an effective amount of aticaprant, as adjunctive treatment with an effective amount of one or more antidepressants.
  • the disclosure also relates to the use of aticaprant, as described herein, wherein the treatment comprises administration of an effective amount of aticaprant, in conjunction with an effective amount of one or more antidepressants.
  • the disclosure also relates to the use of aticaprant, as described herein, wherein the treatment comprises administration of an effective amount of aticaprant, in combination with an effective amount of one or more antidepressants.
  • the disclosure further relates to a package or pharmaceutical product as described herein, wherein the instructions for treatment direct the administration of an effective amount of aticaprant, as adjunctive treatment with an effective amount of one or more antidepressants.
  • the disclosure further relates to a package or pharmaceutical product as described herein, wherein the instructions for treatment direct the administration of an effective amount of aticaprant, in conjunction with an effective amount of one or more antidepressants.
  • the disclosure further relates to a package or pharmaceutical as described herein, wherein the instructions for treatment direct administration of an effective amount of aticaprant, in combination with an effective amount of one or more antidepressants.
  • one or more antidepressants can be selected from a selective serotonin reuptake inhibitor (SSRI), serotonin-norepinephrine reuptake inhibitor (SNRI), or a combination thereof.
  • the disclosure relates to aticaprant, for use as described herein.
  • aticaprant is S-aticaprant.
  • aticaprant, in particular S-aticaprant, for use as described herein is to be administered in an amount of about 2 to about 35 mg, more in particular, of about 10 mg.
  • aticaprant, in particular S-aticaprant, for use as described herein is administered orally.
  • the disclosure relates to aticaprant, in particular S-aticaprant, for use as described herein, administered once daily.
  • the disclosure also relates to the use of aticaprant, in the manufacture of a medicament, as described herein.
  • Aticaprant is S-aticaprant.
  • about 2 to about 35 mg aticaprant is to be administered, more in particular, about 10 mg.
  • aticaprant is to be administered orally.
  • aticaprant in particular S-aticaprant is to be administered once daily.
  • the disclosure further relates to a package or pharmaceutical product as described herein, wherein aticaprant is in particular S-aticaprant.
  • the instructions for treatment direct administration of about 2 to about 35 mg aticaprant, more in particular, about 10 mg.
  • the instructions for treatment direct aticaprant in particular S-aticaprant
  • the instructions for treatment direct aticaprant, in particular S-aticaprant is for once daily administration.
  • administration of aticaprant does not result in weight gain during treatment, including clinically relevant weight gain.
  • the disclosure relates to aticaprant, for use as described herein, wherein the patient does not experience weight gain during the treatment with aticaprant.
  • the disclosure relates to a use as defined herein, wherein the patient does not experience weight gain during the treatment with aticaprant.
  • the disclosure further relates to a package or pharmaceutical product as described herein, wherein the patient does not experience weight gain during the treatment with aticaprant.
  • the body weight of the patient can in particular be assessed at the time of the initial administration of aticaprant.
  • the disclosure relates to aticaprant, for use as described herein, wherein the patient does not experience a decrease in sexual functioning during the treatment with aticaprant.
  • the disclosure relates to a use as described herein, wherein the patient does not experience a decrease in sexual functioning during the treatment with aticaprant.
  • the disclosure relates to a package or pharmaceutical product as described herein, wherein the patient does not experience a decrease in sexual functioning during the treatment with aticaprant.
  • Such term “sexual functioning” comprises sexual drive, sexual arousal, vaginal lubrication, erection, orgasm achievement, or orgasm satisfaction.
  • Sexual satisfaction can be assessed by methods known to the skilled person, for example, by applying the Arizona Sexual Experience Scale (ASEX).
  • the patient has anhedonia.
  • the anhedonia is moderate.
  • the anhedonia is severe.
  • Anhedonia can be measured, through an anhedonia scale, for example, the Snaith Hamilton Pleasure Scale (SHAPS).
  • SHAPS Hamilton Pleasure Scale
  • the disclosure relates to aticaprant, for use as described herein, wherein the anhedonia of the patient is reduced by at least 40%, as measured by the change from baseline in total score in an anhedonia scale following 6 weeks of the treatment with aticaprant, more in particular, the anhedonia of the patient is reduced within about 3 weeks to about 6 weeks as measured by the change from baseline in total score in an anhedonia scale.
  • the anhedonia scale is the Snaith Hamilton Pleasure Scale (SHAPS).
  • SHAPS Snaith Hamilton Pleasure Scale
  • the disclosure relates to the use as described herein, wherein the anhedonia of the patient is reduced by at least 40%, as measured by the change from baseline in total score in an anhedonia scale following 6 weeks of the treatment with aticaprant, more in particular, the anhedonia of the patient is reduced within about 3 weeks to about 6 weeks as measured by the change from baseline in total score in an anhedonia scale.
  • the anhedonia scale is the Snaith Hamilton Pleasure Scale (SHAPS).
  • the disclosure relates to the package or pharmaceutical product as described herein, wherein the anhedonia of the patient is reduced by at least 40%, as measured by the change from baseline in total score in an anhedonia scale following 6 weeks of the treatment with aticaprant, more in particular, the anhedonia of the patient is reduced within about 3 weeks to about 6 weeks as measured by the change from baseline in total score in an anhedonia scale.
  • the anhedonia scale is the Snaith Hamilton Pleasure Scale (SHAPS).
  • methods are provided for treating patients having a more severe type of depression, i.e., major depressive disorder, using the compounds, compositions, e.g., solid compositions, and tablets, e.g., oral tablets, described herein.
  • the patient also may be experiencing anhedonia.
  • MDD alone is difficult to treat, treatment patients having anhedonia are even more problematic since their ability to gauge pleasure is impaired.
  • antidepressants are known to have a variety of side effects such as weight gain, metabolic side effects, extrapyramidal symptoms, akathisia, cognitive impairment, among others.
  • patients may choose to refrain from or stop taking antidepressants to avoid or prevent any side-effects.
  • the methods described herein are effective in managing the patient's depression and anhedonia using aticaprant. Desirably, the methods successfully permit the patient to manage their depression while simultaneously reducing anhedonia.
  • the patients treated according to the described methods have moderate to severe anhedonia.
  • the term “anhedonia” as used herein refers to the lack of or decreased ability to experience pleasure in daily activities.
  • the term anhedonia includes loss of pleasure in sensory experiences (i.e., touch, taste, smell), as well as social interactions.
  • anhedonia and depressed mood are diagnostic criteria for a major depressive episode as part of MDD.
  • Anhedonia also describes deficits in one or more components of reward-related behavior, also known as the pleasure cycle, such as wanting, liking, and learning.
  • the pleasure cycle can be divided into three phases: the appetitive phase (dominated by wanting), the consummatory phase (dominated by liking), and the satiety phase (dominated by learning).
  • the appetitive phase is characterized by the initial energy expenditure to attain a reward; the consummatory phase is enjoyment of the reward; and the satiety phase is characterized by learning and feedback integration.
  • an anhedonia scale may be used.
  • the Snaith-Hamilton Pleasure Scale (SHAPS) analysis is a validated scale for the measurement of anhedonia.
  • the SHAPS is a subject completed scale in which subjects score whether or not they experience pleasure in performing a list of activities or experiences.
  • the SHAPS is a self-reported 14-item instrument, developed for the assessment of hedonic capacity. Subjects score whether they experience pleasure in performing a list of activities or experiences. Subjects can rate the answers as 1-4 where 1 indicates “Nonetheless agree”, 2 indicates “Agree”, 3 indicates “Disagree” and 4 indicates “Nonetheless disagree”.
  • the subject's item responses are summed to provide a total score ranging from 14 to 56.
  • a higher total SHAPS score indicates higher levels of current anhedonia.
  • Physician/clinical judgment can be used to assess anhedonia separately or in conjunction with an anhedonia scale.
  • the patient has moderate anhedonia. In other embodiments, the patient has severe anhedonia.
  • An assessment of moderate or severe anhedonia is typically determined physician/clinical judgment and/or by one or more tests that provide insight into whether a patient has anhedonia.
  • the severity of the anhedonia may be determined using the SHAPS method.
  • a patient with moderate or severe anhedonia is considered to have a high level of anhedonia.
  • a patient with a SHAPS score of 38 or greater is considered to have moderate to severe anhedonia that can be considered a high level of anhedonia.
  • a high level of anhedonia is reflected by a SHAPS score of at least about 40, about 42, about 44, about 46, about 48, about 50, about 52, about 54, about 56, about 58, or higher.
  • a patient with mild or no anhedonia would be considered to have a low level of anhedonia that is assessed by physician/clinical judgment and/or one or more tests.
  • a patient with a SHAPS score of less than 38 is considered to have low anhedonia.
  • a patient with mild anhedonia may have a SHAPS score of 20 to less than 38, for example, a SHAPS score of 20 to about 36, about 22 to about 36, about 24 to about 36, about 26 to about 36, about 26 to about 34, about 26 to about 32, about 26 to about 30, about 26 to about 28, about 28 to about 36, about 28 to about 36, about 30, to about 36, about 32 to about 36, about 34 to about 36, about 20 to about 34, about 22 to about 34, about 24 to about 34, about 26 to about 32, about 26 to about 30, about 26 to about 28, about 28 to about 36, about 28 to about 34, about 28 to about 32, about 28 to about 30, about 30 to about 36, about 30 to about 34, about 30 to about 32, about 32 to about 36, about 32 to about 34, or about 34 to about 36.
  • a SHAPS score of less than 20 can be considered to correspond to normal hedonic functioning, and for purposes of this disclosure, would fall into the low category of anhedonia, e.g.
  • the patient's anhedonia is reduced from a high level of anhedonia to a low level of anhedonia. In yet other embodiments, the patient's anhedonia is reduced by at least about 40%, as measured by the change from baseline in total score in an anhedonia scale following treatment with aticaprant. In yet other embodiments, the patient's anhedonia is reduced by at least about 40%, about 50%, about 60%, about 70%, about 80%, about 90%, or about 95%, as measured by the change from baseline in total score in an anhedonia scale following treatment with aticaprant.
  • the patient's anhedonia is reduced by about 40 to about 90%, about 50 to about 90%, about 60 to about 90%, about 70 to about 90%, about 80 to about 90%, about 40 to about 80%, about 50 to about 80%, about 60 to about 80%, about 70 to about 80%, about 40 to about 70%, about 50 to about 70%, about 60 to about 70%, about 40 to about 60%, about 50 to about 60%, or about 50 to about 60%, as measured by the change from baseline in total score in an anhedonia scale following treatment with aticaprant.
  • the patient's anhedonia is ameliorated, i.e., reduced by 100%, as measured by the change from baseline in total score in an anhedonia scale following treatment with aticaprant.
  • Reduction of anhedonia after initiating treatment with aticaprant may be measured relative to the anhedonia of the patient as measured before treatment with aticaprant, i.e., a baseline anhedonia measurement.
  • the treating clinician is able to calculate the change of anhedonia from the baseline to the real time anhedonia measurement at any point after treatment with aticaprant.
  • standard methods for measuring anhedonia may be used, such as an anhedonia scale, e.g., SHAPS.
  • a baseline anhedonia measurement is obtained no more than about 1 week before initiating treatment with aticaprant.
  • a baseline anhedonia measurement is obtained about 7 days, about 6 days, about 5 days, about 4 days, about 3 days, about 2 days, or about 1 day before treatment with aticaprant.
  • a baseline anhedonia measurement is obtained about 24 hours, about 18 hours, about 12 hours, about 8 hours, about 4 hours, about 2 hours, about 1 hours, about 30 minutes, or about 15 minutes before initiating treatment with aticaprant.
  • the patient's change of anhedonia will depend on several factors including, without limitation, anhedonia severity, patient's sensitivity to aticaprant, other pharmaceutical agents being administered, among others.
  • the patient's anhedonia is reduced after about 3 weeks of treatment with aticaprant. In other embodiments, the patient's anhedonia is reduced after about 3 weeks of treatment with aticaprant. In further embodiments, the patient's anhedonia is reduced after about 3 weeks to about 6 weeks, and, in certain embodiments, through week 6, of treatment with aticaprant.
  • the patient's anhedonia is reduced by at least about 40%, as measured by the change from baseline in total score in an anhedonia scale following about 6 weeks of the treatment with aticaprant.
  • the anhedonia of the patient is reduced within about 3 weeks, and in some embodiments within about 3 weeks to about 6 weeks, as measured by the change from baseline in total score in an anhedonia scale and/or by physician/clinical judgement.
  • the methods described herein were found to not only improve the patient's depression and anhedonia symptoms, but resulted in fewer antidepressant side effects. Doing so resulted in less absenteeism (i.e., more visits or interactions with physicians), greater cognitive functioning, improvements in health-related quality of life, more interest and engagement in everyday activities, improvement in family and inter-personal relationships, ability to function in the workplace, fewer hospitalizations, among others.
  • the disclosure provides methods for treating MDD in a human patient by administering to the patient a pharmaceutical composition comprising between about 2 mg and 20 mg aticaprant, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with aticaprant.
  • administration of the pharmaceutical composition to the patient achieves a pharmacokinetic (PK) profile comprising one or more of the PK parameters noted above (dose-normalized to 10 mg) after administration of the composition to a human after at least a 10-hour fast.
  • PK pharmacokinetic
  • the terms “subject” and “patient” refer to a human, who has been the object of treatment, observation or experiment. Preferably, the patient has experienced and/or exhibited at least one symptom of the disease or disorder to be treated and/or prevented. In some embodiments, the patient is an adult. As used herein, the term “adult” as used herein refers to a human that is about 18 years of age or older. In certain aspects, the patient is an elderly adult, i.e., greater than or equal to 65 years of age.
  • treating shall include the management and care of a subject or patient (preferably mammal, more preferably human) for the purpose of combating a disease, condition, or disorder and includes the administration of a compound described herein to prevent the onset of the symptoms or complications, alleviate one or more of the symptoms or complications, or eliminate the disease, condition, or disorder.
  • depression also referred to as depressive disorder
  • depression includes major depressive disorder, persistent depressive disorder, seasonal affective disorder, postpartum depression, premenstrual dysphoric disorder, situational depression, anhedonia, melancholic, mid-life depression, late-life depression, bipolar depression, depression due to identifiable stressors, treatment resistant depression, or combinations thereof.
  • the depression is major depressive disorder.
  • the major depressive disorder is with melancholic features or anxious distress.
  • the depression is treatment-resistant depression.
  • the depression is major depressive disorder with suicidal ideation.
  • a patient is considered to have major depressive disorder if exhibiting five or more symptoms during the same two week period that are a change from previous functioning; depressed mood and/or loss of interest/pleasure must be present; excluding symptoms clearly attributable to another medical condition. See, e.g., Table 4.
  • Depressed mood Most of the day, nearly every day; may be subjective (e.g., feels sad, empty, hopeless) or observed by others (e.g., appears tearful); in children and adolescents, can be irritable mood 2.
  • Loss of interest/pleasure Markedly diminished interest/pleasure in all (or almost all) activities most of the day, nearly every day; may be subjective or observed by others 3.
  • Weight loss or gain Significant weight loss (without dieting) or gain (change of >5% body weight in a month), or decrease or increase in appetite nearly every day; in children, may be failure to gain weight as expected 4.
  • Insomnia or hypersomnia Nearly every day 5.
  • the following criteria also are met:
  • Symptoms cause clinically significant distress or impairment in social, occupational, or other important areas of functioning 2. Episode not attributable to physiological effects of a substance or another medical condition 3. Episode not better explained by schizoaffective disorder, schizophrenia, schizophreniform disorder, delusional disorder, or other specified and unspecified schizophrenia spectrum and other psychotic disorders 4. No history of manic or hypomanic episode
  • Major depressive disorder may be categorized as mild, moderate, or severe.
  • the MDD is mild.
  • the MDD is moderate.
  • the MDD is severe.
  • “mild MDD” applies to a patient having few, if any, symptoms in excess of those required to make the diagnosis, the intensity of the symptoms is distressing but manageable, and the symptoms result in minor impairment in social or occupational functioning.
  • the mild MDD may be a single episode (ICD-10 F32.0) or a recurrent episode (ICD-10 F33.0).
  • Mode MDD applies to a patient having a number of symptoms, intensity of symptoms, and/or functional impairment are between those specified for “mild” and “severe.”
  • the moderate MDD may be a single episode (ICD-10 F32.1) or a recurrent episode (ICD-10 F33.1).
  • severe MDD applies to a patient where the number of symptoms is substantially in excess of that required to make the diagnosis, the intensity of symptoms is seriously distressing and unmanageable, and the symptoms markedly interfere with social and occupational functioning, and urgent symptom control is necessary.
  • the severe MDD may be a single episode (ICD-10 F32.2) or a recurrent episode (ICD-10 F33.2).
  • MDD is classified according to the DSM-5 definition of Table 5.
  • MGH Multiple- ⁇ sberg Depression Rating Scale
  • CGI-S Clinical Global Impression—Severity
  • SATE Self-Assessment of Treatment Experience
  • MGH Massachusetts General Hospital
  • ATRQ Antidepressant Treatment Response Questionnaire
  • MADRS is utilized to diagnose and/or monitor the patient.
  • MADRS is a 10-item rating scale that is used in antidepressant studies. It is clinician-administered and designed to be used in subjects with MDD to measure the overall severity of depressive symptoms.
  • the MADRS scale is validated, reliable, and acceptable to regulatory health authorities as a primary scale to determine efficacy in major depression.
  • MADRS is administered using the Structured Interview Guide for the MADRS (SIGMA).
  • the scale consists of 10 items, each of which is scored from 0 (item not present or normal) to 6 (severe or continuous presence of the symptoms), summed for a total possible score of 60. Higher scores represent a more severe condition.
  • the MADRS evaluates apparent sadness, reported sadness, inner tension, sleep appetite, concentration, lassitude, inability to feel (interest level), pessimistic thoughts, and suicidal thoughts.
  • CGI-S is utilized to diagnose and/or monitor the patient's depression.
  • CGI-S is a scale that rates the severity of the subject's illness at the time of assessment, relative to the clinician's past experience with subjects who have the same diagnosis and improvement with treatment.
  • CGI-S provides an overall clinician-determined summary measure of severity of subject's illness that considers all available information, including knowledge of subject's history, psychosocial circumstances, symptoms, behavior, and impact of symptoms on subject's ability to function.
  • CGI-S evaluates severity of psychopathology on scale of 0 to 7.
  • SMDDS is utilized to diagnose and/or monitor the patient's depression.
  • SMDDS is a subjective rating of the patient.
  • the SMDDS is a 16-item PRO measure. Each item is rated by the subject according to a 5-point Likert scale. Subjects respond to each question using a rating scale between 0 (“Not at all” or “Never”) to 4 (“Extremely” or “Always”). The total score ranges from 0 to 60.
  • the SMDDS uses a 7-day recall period and verbal rating scales. Higher score indicates more severe depressive symptomatology.
  • SATE is utilized to diagnose and/or monitor the patient's depression.
  • SATE is a one to three questionnaire administered when the subject is unable to complete other evaluations, i.e., away from the clinical setting such as at home.
  • SATE is useful to evaluate improvement or deterioration of depressive symptoms of the subjects over a short period of time. For rating overall depression, subject selected one option out of Improved, not changed or got worse; for depression improvement, subject selected one option out of slightly improved, much improved, very much improved and for depression worsen subject selected slightly worse, much worse, very much worse. See, Table 6.
  • the MGH-ATRQ is a self-rated scale used to determine treatment resistance in patient's having MDD. This questionnaire examines the antidepressant treatment history, using specific anchor points to define the adequacy of both dose and duration of each antidepressant trial, and the degree of symptomatic improvement.
  • the MGH-ATRQ permits determining treatment resistance in depression and is known to those skilled in the art.
  • the patient had an inadequate response to other antidepressant therapy.
  • “Inadequate response” as used herein refers to a patient experiencing a less than about 50% reduction in depressive symptom severity from the start of initiating treatment. Typically, the inadequate response is during a current/active episode of the depression. In some embodiments, an inadequate response refers to a patient experiencing about 26 to less than about 50% reduction in depressive symptom severity from the start of initiating treatment.
  • an inadequate response refers to a patient experiencing about 26 to about 49, about 26 to about 45, about 26 to about 40, about 26 to about 35, about 26 to about 30, about 30 to about 49, about 30 to about 45, about 30 to about 40, about 30 to about 35, about 35 to about 49, about 35 to about 45, about 35 to about 40, about 40 to about 49, or about 40 to about 45% reduction in depressive symptom severity from the start of initiating treatment.
  • a patient's response may be measured by one or more scales described herein and/or by physician/clinical judgment.
  • an inadequate response is measured by MGH-ATRQ, MADRS, or SHAPS.
  • an inadequate response is measured by MGH-ATRQ.
  • a patient is said to have a partial response to treatment, this refers to some minor to moderate symptomatic improvement since the initiation of treatment, but some of the initial symptoms are still present and troubling to the patient and these persistent symptoms still affect behavior and function. For instance, the patient's motivation, productivity, and interest in his or her usual activities may still be impaired.
  • other antidepressant therapy refers to an antidepressant medication or non-pharmacological treatment that is used to treat patients having depression.
  • the other antidepressant therapy is an antidepressant medication.
  • the other antidepressant therapy is a non-pharmacological treatment.
  • the other antidepressant therapy is an antidepressant medication other than aticaprant.
  • the antidepressant medication is any pharmaceutical agent which can be used to treat depression. Suitable examples include, without limitation, mono-amine oxidase inhibitors, tricyclics, tetracyclics, non-cyclics, triazolopyridines, selective serotonin reuptake inhibitors (SSRI), serotonin receptor antagonists, serotonin noradrenergic reuptake inhibitors (SNRI), noradrenergic and specific serotonergic agents, noradrenaline reuptake inhibitors, or antipsychotics (typical or atypical antipsychotics).
  • mono-amine oxidase inhibitors include phenelzine, tranylcypromine, moclobemide, and the like.
  • Examples of tricyclics include imipramine, amitriptyline, desipramine, nortriptyline, doxepin, protriptyline, trimipramine, clomipramine, amoxapine, and the like.
  • Examples of tetracyclics includes maprotiline, and the like.
  • Examples of non-cyclics include nomifensine, and the like.
  • Examples of triazolopyridines include trazodone, and the like.
  • Examples of SSRIs include fluoxetine, sertraline, paroxetine, citalopram, citalopram, escitalopram, fluvoxamine, and the like.
  • Examples of serotonin receptor antagonists include nefazadone, and the like.
  • Examples of SNRIs include venlafaxine, milnacipran, desvenlafaxine, duloxetine, levomilnacipran and the like.
  • Examples of noradrenergic and specific serotonergic agents include mirtazapine, and the like.
  • Examples of noradrenaline reuptake inhibitors include reboxetine, edivoxetine and the like.
  • Typical antipsychotics include phenothiazines (e.g., chlorpromazine, thioridazine, fluphenazine, perphenazine, trifluoperazine, levomepromazin), thioxanthenes (e.g., thiothixene, flupentixol), butyrophenones (e.g., haloperidol), dibenzoxazepines (e.g., loxapine), dihydroindolones (e.g., molindone), substituted benzamides (e.g., sulpride, amisulpride), and the like.
  • phenothiazines e.g., chlorpromazine, thioridazine, fluphenazine, perphenazine, trifluoperazine, levomepromazin
  • thioxanthenes e.g., thiothixene, flupentixol
  • antidepressant medication includes natural products such as Kava-Kava, St.
  • the antidepressant medication includes neuropeptides such as thyrotropin-releasing hormone and the like or compounds targeting neuropeptide receptors such as neurokinin receptor antagonists and the like.
  • the antidepressant medication is a hormone such as triiodothyronine, and the like.
  • the antidepressant medication is SSRI, SNRI, or a combination thereof.
  • the antidepressant is a SSRI that is escitalopram, sertraline, paroxetine, fluoxetine or citalopram.
  • the antidepressant medication is a SNRI that is venlafaxine, duloxetine, vortioxeine or desvenlafaxine.
  • the non-pharmacologic treatment for use herein may be selected by one skilled in the art.
  • the non-pharmacologic treatment is psychotherapy, transcranial magnetic stimulation, or the like.
  • Therapeutically effective amounts/dosage levels and dosage regimens for the other antidepressant therapy may be readily determined by one of ordinary skill in the art.
  • therapeutic dosage amounts and regimens for pharmaceutical agents approved for sale are publicly available, for example as listed on packaging labels, in standard dosage guidelines, in standard dosage references such as the Physician's Desk Reference (Medical Economics Company or online at http:///www.pdrel.com) or other sources.
  • other antidepressant therapy may include one antidepressant medication.
  • other antidepressant therapy includes two or more antidepressant medications.
  • other antidepressant therapy includes two antidepressant medications.
  • other antidepressant therapy includes three antidepressant medications. The attending physician would be able to select suitable antidepressant therapies for use as described herein.
  • the patient was receiving treatment with other antidepressant therapy prior to receiving aticaprant. In some embodiments, the patient was receiving treatment with other antidepressant therapy that comprised a SSRI, SNRT, or a combination thereof. In other embodiments, the patient stopped treatment with other antidepressant therapy before initiating treatment with aticaprant.
  • adjunctive treatment with an effective amount of one or more antidepressants.
  • adjuctive treatment and “adjunctive therapy” shall mean treatment of a patient in need thereof by administering aticaprant in combination with one or more antidepressant(s), wherein aticaprant and the antidepressant(s) are administered by any suitable means, simultaneously, sequentially, separately, or in a single pharmaceutical formulation.
  • Aticaprant is administered adjunctively with other antidepressant(s) currently being administered to the patient, including current antidepressant(s) to which the patient had an inadequate response, i.e., the antidepressant failed to treat the patient's depression.
  • aticaprant is administered adjunctively with an antidepressant(s) not previously administered to the patient, i.e., a new antidepressant.
  • aticaprant is administered in a regimen with an antidepressant(s) previously administered to the patient.
  • the number of dosages administered per day for each active compound may be the same or different and more typically different.
  • the antidepressant may be dosed as prescribed by the attending physician and/or by its label and aticaprant is dosed as described herein.
  • a patient is under concurrent treatment with both an antidepressant and aticaprant, where both are administered by their prescribed dosing regimens.
  • the aticaprant and antidepressant(s) may be administered according to simultaneous or alternating regimens, at the same or different times during the course of the therapy, concurrently in divided or single forms.
  • Aticaprant and the antidepressant(s) may be administered via the same or different routes of administration.
  • suitable methods of administration include, but are not limited to, oral, intravenous (iv), intranasal (in) intramuscular (im), subcutaneous (sc), transdermal, buccal, or rectal.
  • aticaprant is administered orally.
  • the patient does not experience many of the side effects that are associated with other antidepressants, i.e., antidepressants other than aticaprant.
  • the patient does not experience weight gain during the treatment with aticaprant.
  • weight gain refers to an increase in the weight of patient, relative to the weight of the patient before taking aticaprant or the weight of the patient that is assessed at the time of the initial administration of aticaprant.
  • the patient may actually see a decrease in overall weight, relative to the weight of the patient before taking aticaprant.
  • the patient's weight is stable, i.e., does not increase or decrease.
  • the patient does not experience a clinically relevant weight gain which is characterized as a weight increase of ⁇ 7%.
  • the patient does not experience a decrease in sexual functioning during the treatment with aticaprant.
  • the term “decrease in sexual functioning” refers to reducing or lessening of one or more components of the human sex drive, i.e., sexual functioning.
  • the sexual functioning comprises one or more of sexual drive, sexual arousal, vaginal lubrication, erection, orgasm achievement, or orgasm satisfaction.
  • the sexual functioning comprises sexual drive.
  • the sexual functioning comprises vaginal lubrication satisfaction.
  • the sexual functioning comprises orgasm achievement.
  • the sexual functioning comprises orgasm satisfaction.
  • the patient's sexual functioning is assessed at the time of initial administration of aticaprant.
  • the patient's sexual functioning while taking aticaprant can be compared to the patient's sexual functioning before administration of aticaprant.
  • Sexual functioning may be assessed by using standard scales and techniques such as the Arizona Sexual Experience Scale (ASEX).
  • ASEX Arizona Sexual Experience Scale
  • the ASEX is used to investigate whether aticaprant has a further positive or negative effect on sexual function.
  • the ASEX is 5 item rating scale administered to patients that quantifies sexual drive, sexual arousal, vaginal lubrication or penile erection, ability to reach orgasm and satisfaction. Scores range from 5 to 30, and two different versions of the scale are available (males and females).
  • CPFQ Cognitive and Physical Functioning Questionnaire
  • KSS Karolinska Sleepiness Scale
  • TEPS Temporal Experience of Pleasure Scale
  • the CPFQ is a brief self-report scale that provides additional information regarding the impact of adjunctive treatment on aspects of cognitive and executive function including attention, memory and mental acuity. Subjects with MDD are often reported to have difficulties with functioning in this area.
  • the KSS is a subject-reported assessment used to rate sleepiness on a scale of 1 to 9, ranging from “extremely alert” (1) to “very sleepy, great effort to keep awake, fighting sleep” (9).
  • the TEPS includes 18 items, 2 subscales designed to distinguish between anticipatory and consummatory pleasure.
  • the methods described herein include administering an effective amount of aticaprant to the patient.
  • effective amount means that amount of active compound or pharmaceutical agent that elicits the biological or medicinal response in a human that is being sought by a researcher, medical doctor or other clinician, which includes alleviation of one or more of the symptoms of the disease or disorder being treated.
  • aticaprant is utilized in an effective amount as determined by the attending physician.
  • other antidepressant(s) is utilized in an effective amount either separately or in combination with aticaprant.
  • XRPD diffractograms were collected on a Bruker D8 diffractometer using Cu K ⁇ radiation (40 kV, 40 mA) and a ⁇ -2 ⁇ goniometer fitted with a Ge monochromator.
  • the incident beam passes through a 2.0 mm divergence slit followed by a 0.2 mm anti-scatter slit and knife edge.
  • the diffracted beam passes through an 8.0 mm receiving slit with 2.5° Soller slits followed by the Lynxeye Detector.
  • the software used for data collection and analysis was Diffrac Plus XRD Commander and Diffrac Plus EVA respectively.
  • Samples were run under ambient conditions as flat plate specimens using powder as received.
  • the sample was prepared on a polished, zero-background ( 510 ) silicon wafer by gently pressing onto the flat surface or packed into a cut cavity. The sample was rotated in its own plane.
  • XRPD diffractograms were collected on a PANalytical Empyrean diffractometer using Cu K ⁇ radiation (45 kV, 40 mA) in transmission geometry.
  • a 0.5° slit, 4 mm mask and 0.04 rad Soller slits with a focusing mirror were used on the incident beam.
  • a PIXcel 3D detector, placed on the diffracted beam, was fitted with a receiving slit and 0.04 rad Soller slits.
  • the software used for data collection was X'Pert Data Collector using X'Pert Operator Interface. The data were analyzed and presented using Diffrac Plus EVA or HighScore Plus.
  • Samples were prepared and analyzed in either a metal or Millipore 96 well-plate in transmission mode. X-ray transparent film was used between the metalsheets on the metal well-plate and powders (approximately 1-2 mg) were used as received.
  • the Millipore plate was used to isolate and analyze solids from suspensions by adding a small amount of suspension directly to the plate before filtration under a light vacuum.
  • the scan mode for the metal plate used the gonio scan axis, whereas a 2 ⁇ scan was utilized for the Millipore plate.
  • the software used for data collection was X'Pert Data Collector and the data analyzed and presented using Diffrac Plus EVA.
  • DSC Differential Scanning calorimetry
  • DSC data were collected on a TA Instruments Q2000 equipped with a 50 position auto-sampler. Typically, 0.5-3 mg of each sample, in a pin-holed aluminum pan, was heated at 10° C./min from 25° C. to 275° C. A purge of dry nitrogen at 50 mL/min was maintained over the sample.
  • Modulated temperature DSC was carried out using an underlying heating rate of 2° C./min and temperature modulation parameters of ⁇ 0.636° C. (amplitude) every 60 seconds.
  • the instrument control software was Advantage for Q Series and Thermal Advantage and the data were analyzed using Universal Analysis or TRIOS.
  • DSC data were collected on a TA Instruments Discovery DSC equipped with a 50 position auto-sampler. Typically, 0.5-3 mg of each sample, in a pin-holed aluminum pan, was heated at 10° C./min from 25° C. to 275° C. A purge of dry nitrogen at 50 mL/min was maintained over the sample.
  • the instrument control software was TRIOS and the data were analyzed using TRIOS or Universal Analysis.
  • Aqueous sodium hydroxide was added to compound 1 in 2-methyltetrahydrofuran.
  • compound 2 i.e., the free base of compound 1 in 2-MeTHF was solvent switched to tetrahydrofuran (THF).
  • Reductive amination of compound 3 using compound 2 was carried out by adding sodium triacetoxyborohydride and THF. Upon reaction completion, the reaction mixture was washed with saturated sodium bicarbonate and sodium chloride. The organic phase containing crude compound 4 was concentrated and ethanol and water were added. The product was crystallized using THF, ethanol, and water to produce compound 4 as a solid.
  • Form III of aticaprant was found to be crystalline by XRPD.
  • 1 H NMR showed that the material was consistent with the proposed structure, with the presence of residual ethyl acetate.
  • Ion chromatography showed that there were no cations/anions present, and HPLC showed 99.8% purity.
  • the DSC (heating from 20 to 131° C. at 10° C./min) showed a peak temperature at 121° C. See, FIG. 3 .
  • Tablets containing aticaprant were prepared according to the scheme in FIG. 24 containing the components in Table 10.
  • Example 3 The tablets of Example 3 are tested to determine dissolution properties and chemical stability. See, Table 11 for dissolution conditions and Tables 12-13 for results.
  • Dissolution Medium 0.01M hydrochloric acid Volume 900 mL Temperature 37 ⁇ 0.5° C. Rotation Speed 50 rpm Analytical Finish UHPLC with UV detection at 247 nm
  • the chemical stability of the tablets is evaluated over a 28-day period using a Risk Based Predictive Stability (RiBPS) study.
  • the stability protocols for the studies are provided in Tables 14-15.
  • the primary objective was to evaluate the efficacy of aticaprant compared to placebo when administered as adjunctive treatment in subjects with MDD partially responsive to SSRI/SNRI treatment in terms of reduction of symptoms of depression, as assessed by the change from baseline on the MADRS in non-responders during the placebo lead-in period.
  • the secondary objectives are:
  • Secondary exploratory objectives include:
  • the study consisted of two phases: a screening phase of up to 5 weeks and a double-blind treatment phase lasting 11 weeks. See, FIG. 4 .
  • Subjects with MDD who have had treatment initiated with a permitted SSRI/SNRI and have had an inadequate or only partial response to this treatment were screened.
  • Assessments include the MINI, Antidepressant Treatment History Questionnaire (TRQ), and MADRS.
  • the treatment phase consisted of 3 periods. A placebo lead-in period of concealed duration, after which subjects entered the double-blind treatment period when they were randomly assigned to 10 mg aticaprant (two 5 mg capsules) or continue placebo for 6 weeks. Each capsule contained aticaprant (5 mg), microcrystalline cellulose (94.95 mg), and magnesium stearate (0.05 mg) in a hard gelatin capsule. Subjects who completed the treatment period, entered the withdrawal period and were treated with placebo for the remaining time of the treatment phase. The total duration for each subject was approximately 16 weeks. There were 11 scheduled visits, including screening. An overall flow diagram is shown in FIG. 4 .
  • Subjects were screened within 35 to 2 days prior to Day 1 to ascertain their eligibility per the inclusion and exclusion criteria.
  • the symptoms of depression were assessed using the structured interview guide for the MADRS.
  • the duration of the double-blind treatment phase was 11 weeks divided into 3 periods.
  • the subject received medication after completion of the visit on Day 1.
  • the first dose was taken at home on Day 2. All medication was taken in fasting condition.
  • Visits 3, 4 and 5 the subjects were re-randomized to blind subjects the duration of the placebo lead-in period.
  • the subjects visited the center for out-patient visits every 1 to 2 weeks. See, Table 17.
  • EW visit should be completed.
  • d At home In fasting condition.
  • At clinic visit days Use blisters dispensed at the previous visit. In fasting condition after completion of predose assessments.
  • j During the first screening visit and by telephone up to 4 days before Visit 2, if 2 weeks or more elapse between the MADRS rating at screening and Visit 2.
  • k Using Q1.6-app on subjects' smartphone. l Breakfast, lunch or dinner after drug intake at site.
  • Lead-in period Subjects who successfully complete the baseline examination visit at the clinical site/unit, were treated with placebo for the entire duration of the lead-in period.
  • Treatment period At the end of the lead-in period both placebo lead-in responders and placebo lead-in non-responders were randomized to receive either placebo or 10 mg aticaprant in a 1:1 ratio for 6 weeks. Subjects remained blinded to exact timing of the randomization, response criterion and drug treatment assignment for each subject.
  • Aticaprant was supplied as 5-mg capsules. Placebo was supplied as matching capsules. All subjects took 2 capsules QD. The capsules were taken daily from Day 2 to Day 78 in fasting condition with some water (fasting for at least 4 hours before dosing). Medication was taken before breakfast. If the subject has forgotten to take the medication before breakfast, this was done before the next following meal, at the latest at dinner of the same day. If the subject remembered later than dinner, the dose of that day was omitted, and the subject took the dose before breakfast on the next day.
  • Visit 11 was planned up to 3 days later, the subject continued medication until Visit 11.
  • the capsules were swallowed whole and not chewed, divided, dissolved or crushed. After having taken the medication, subjects did not to eat or drink for at least 30 minutes.
  • the first dose was taken in fasting condition on Day 2 of the double-blind phase.
  • the dose of the medication was:
  • Medication dose was adjusted as needed to 5 mg QD based on the results of a blinded review of the safety data. When a dose reduction has been decided on, this only applied to new subjects and the dose of medication was:
  • the Enriched ITT Analysis Set (eITT) is defined as all enrolled lead-in placebo non-responders who were randomized into a treatment period, received at least one dose of study medication in the treatment period and have at least one post-baseline MADRS assessment during the treatment period.
  • the Full ITT Analysis Set (fITT) is defined as all enrolled subjects who were randomized into a treatment period, received at least one dose of study medication in the treatment period and have at least one post-treatment baseline assessment of MADRS during the treatment period.
  • Standard safety assessments including physical and neurological examination, vital signs, 12-lead ECG, clinical chemistry, hematology, and urinalysis was performed. Based on observations of GI complaints in previous studies, a panel including PGI, PGII, G17 and Hp IgG was added to the clinical laboratory test panel to test for stomach mucosa status.
  • response status of the subjects was assessed according to the double-blind response criteria based on reduction in MADRS relative to lead-in baseline.
  • Both lead-in placebo responders and lead-in placebo non-responders were randomly assigned in a 1:1 ratio to either aticaprant or placebo in the treatment period. The randomization was stratified by lead-in response status (non-responders: ⁇ 30% reduction from baseline in MADRS total score at the end of the lead-in period vs responders: ⁇ 30% reduction from baseline at the end of the lead-in period) and presence/absence of anhedonia (presence defined as SHAPS total score ⁇ 20).
  • Treatment duration The study consisted of two periods: a screening phase of up to 5 weeks and a double-blind treatment phase of 11 weeks.
  • the first period was a placebo lead-in of 3 weeks, after which subjects entered the treatment period when they were randomly assigned to aticaprant or continuation on placebo for 6 weeks.
  • Subjects who successfully completed the treatment period were treated with placebo during a 2-week withdrawal period, i.e., Period 3.
  • the total duration for each subject was approximately 16 weeks.
  • the efficacy analysis is based on the eITT set defined as all enrolled lead-in placebo non-responders who were randomized into the treatment period, received at least one dose of medication, and have at least one post-baseline MADRS assessment during the treatment period.
  • the primary analysis set is used for all efficacy endpoints.
  • a secondary analysis set is the fITT set defined as all enrolled subjects who were randomized into the treatment period, received at least one dose of medication, and have at least one post-baseline MADRS assessment during the treatment period.
  • the secondary analysis set is used for all efficacy endpoints to examine the effect in the general population, which may be useful for designing subsequent studies in the development program.
  • the safety analysis is based on the full safety analysis set, defined as all enrolled subjects who received at least one dose of medication in the treatment period.
  • the mean (SD) MADRS total score at treatment baseline was 29.0 (4.61), ranging from 19 to 41. See, FIG. 5 .
  • the mean change from treatment baseline (SD) in MADRS total score at treatment week 6 was ⁇ 10.2 (8.44) for aticaprant and ⁇ 8.2 (8.53) for placebo.
  • the observed effect size was 0.23. See, Tables 20-22 and FIG. 8 .
  • the mean (SD) baseline MADRS total score at treatment baseline was 25.3 (7.86), ranging from 0 to 41. See, FIGS. 7 A and 7 B .
  • the mean changes from treatment baseline in MADRS total score at Treatment Week 6 for fITT were smaller than for eITT: ⁇ 9.7 (8.02) for aticaprant and ⁇ 6.6 (8.57) for placebo.
  • the observed effect size was 0.36.
  • the percentage of subjects with ⁇ 50% improvement in MADRS total score at treatment week 6 in the eITT population was 35.6% for aticaprant and 22.0% for placebo.
  • Treatment week 6 response rates in fITT population were 38.2% for aticaprant and 23.5% for placebo.
  • the mean (SD) SHAPS total score at treatment baseline was 36.6 (5.45), ranging from 20 to 50.
  • the mean change from treatment baseline (SD) in SHAPS total score at treatment week 6 was ⁇ 4.6 (6.23) for aticaprant and ⁇ 4.2 (5.04) for placebo.
  • the observed effect size was 0.07. See, Table 27 and FIGS. 17 and 37 .
  • the estimated LS mean differences with 80% 2-sided CI at treatment week 6 between aticaprant and placebo was ⁇ 0.8 [ ⁇ 1.79, 0.10].
  • the corresponding p-value was 0.250. See, FIGS. 7 and 8 .
  • the observed effect size was 0.38 and 0.11, respectively.
  • C max is defined as maximum plasma concentration of aticaprant.
  • the eITT population included all enrolled lead-in placebo non-responders who were randomized into a treatment period, received at least 1 dose of study medication, and had at least 1 post-baseline MADRS assessment during the treatment period.
  • N number of subjects analyzed
  • n number analyzed
  • the most common TEAEs during the treatment period were headache (experienced by 10/85 subjects—11.8% in the aticaprant group and by 6/84 subjects—7.1% in the placebo group) and diarrhea (experienced by 7/85 subjects—8.2% in the aticaprant group and by 2/84 subjects—2.4% in the placebo group). See, Table 40.
  • Subjects with Adverse 4 (4.8) 13 (15.3) 17 (10.1) Events of Special Interest Gastrointestinal Disorders 4 (4.8) 9 (10.6) 13 (7.7) deaths causally related to treatment/all Diarrhea 2 (2.4) 7 (8.2) 9 (5.3) Abdominal Pain Upper 2 (2.4) 0 2 (1.2) Dyspepsia 1 (1.2) 1 (1.2) 2 (1.2) Abdominal Pain 0 1 (1.2) 1 (0.6) Skin And Subcutaneous Tissue 0 5 (5.9) 5 (3.0) Disorders Pruritus 0 5 (5.9) 5 (3.0) Percentages calculated with the number of subjects in each group as denominator. Reported dictionary version: MedDRA 22.1. Subjects are presented by the treatment received during the Treatment period.
  • the results illustrate that the treatment effect is larger in patients with more anhedonia at baseline. See, FIGS. 20 -A and 20 -B.
  • the placebo+oral antidepressant group shows less placebo response as compared to the low anhedonia group in FIGS. 7 - 8 .
  • the treatment effect of the aticaprant+oral antidepressant group is higher in the high anhedonia group as compared to the low anhedonia group.
  • Overall the effect size is larger at every single time point (from week 1 onwards) in the high anhedonia group.
  • the LSMD in the high anhedonia group is more than double that of the low anhedonia group at week 6. Further, when looking at the symptom level, greater improvement in items related to anhedonia and dysphoria in subgroup with high anhedonia vs low anhedonia. See, FIG. 21 .
  • the mean weight for subjects in the placebo group was 76.17 kg compared to 78.66 in the aticaprant group.
  • the mean weight in the placebo group was 75.75 kg compared to 78.57 kg in the aticaprant group. This indicates that the weight in both groups remained relatively stable over the 6-week double blind treatment period. This is unexpected because other adjunctive treatments for MDD result in a mean weight increase. See, Thase M, et al. J Clin Psych. 2015: 76(9), 1224-1231; Thase, J Clin Psych. 2015, 76(9):1232-1240; El Khalili, Int J Neuropsychopharmacol.
  • Impairments in sexual functioning is a common side effect of antidepressant treatment and can be very upsetting to patients and their sexual partners.
  • Major depression itself is associated with increased sexual dysfunction, and many of the pharmacological treatments are known to worsen sexual functioning even further.
  • MDD In a large survey of nearly 5000 patients in France, it was estimated that in untreated patients with MDD, the prevalence of sexual dysfunction was 65%. The prevalence of sexual dysfunction increased to 71% for patients treated with antidepressant therapy.
  • the brain reward circuitry is controlled by several areas: nucleus accumbens, ventral tegmental area and the amygdala. It is hypothesized that treatment with kappa opioid receptors may restore the normal homeostatic balance in patients with overactivation. Treatment with aticaprant could potentially improve symptoms of anhedonia. Other symptoms associated with the reward circuitry includes: sexual pleasure, lack of interest and lack of enjoyment.
  • the mean change from treatment baseline (SD) in ASEX total score to week 6 was ⁇ 1.5 (4.02) points for aticaprant compared to ⁇ 0.7 (2.98) points for placebo.
  • a lower score on the ASEX indicates improvement.
  • the score reduction at week 6 was greater in the aticaprant group compared to placebo. This is unexpected because adjunctive treatments with other agents are expected to worsen sexual functioning, i.e., increase in ASEX score over time. See, FIG. 22 .
  • FIG. 10 -B depicts the least squares mean change from baseline. A significant treatment effect favoring aticaprant was seen as early as week 3. At this point, aticaprant showed a statistically superior effect compared to placebo.
  • Study Design A 6-week, multicenter, double-blind, randomized, placebo-controlled study to assess the efficacy, safety, and tolerability of aticaprant in adult and elderly subjects (18 to 74 years) who have MDD with prominent anhedonia (MDD ANH+), and who have had an inadequate response to a SSRI or a serotonin and SNRI in the current depressive episode. See, FIG. 34 .
  • this study will consist of 3 phases: an eligibility screening phase (up to 4 weeks prior to first dose administration), a double-blind treatment phase of 6 weeks, and a follow-up of 1-2 weeks. Subjects who have completed the double-blind phase may participate in an open-label long-term safety study.
  • MDD ANH+ Approximately 544 subjects with MDD with prominent anhedonia (MDD ANH+) and without prominent anhedonia (MDD ANH ⁇ ) will be randomized in a 1:1 ratio to adjunctive placebo or aticaprant to achieve a minimum of 314 adult subjects meeting predefined criteria for MDD ANH+ eligible to be included in the primary analysis. Randomization will be stratified by study site, age group (adults [ ⁇ 65 years], elderly [ ⁇ 65 years]), baseline anhedonia, and baseline MADRS total score. All subjects will continue their baseline antidepressant (SSRI/SNRT) during the entire study.
  • SSRI/SNRT baseline antidepressant
  • Inclusion Criteria 1. Age of 18 to 74 years (inclusive). 2. Be medically stable on the basis of physical examination (including a brief neurological examination), medical history, vital signs (including blood pressure), and 12-lead ECG performed at screening and baseline. If there are any abnormalities that are not specified in the inclusion and exclusion criteria, their significance must be determined. 3. Be medically stable on the basis of clinical laboratory tests performed at screening. If the results of the serum chemistry panel, hematology, or urinalysis are outside the normal reference ranges, retesting of an abnormal lab values that may lead to exclusion will be allowed once during the screening phase. 4.
  • An adequate trial is defined as an antidepressant treatment for at least 6 weeks (and no greater than 12 months in the current episode) at or above the stable therapeutic dose specified in the MGH-ATRQ, must include the subject's current antidepressant treatment. If the subject has received 2 SSRI/SNRI treatments of sufficient dose and duration in the current episode, and has shown ⁇ 25% improvement to both, then the subject would not qualify based on exclusion criterion (first exclusion criterion). 6. Current major depressive episode, depression symptom severity, presence of anhedonia and antidepressant treatment response in the current depressive episode must be confirmed.
  • SSRI or SNRI for depressive symptoms, in any formulation and available in the participating country: citalopram, duloxetine, escitalopram, fluvoxamine, fluoxetine, milnacipran, levomilnacipran, paroxetine, sertraline, venlafaxine, desvenlafaxine at a stable dose (at therapeutic dose level) for at least 6 weeks, and for no greater than 12 months in the current episode, at screening.
  • the above SSRI/SNRI needs to be approved for the treatment of MDD. Subjects using fluvoxamine as baseline SSRI and have normal renal and hepatic function are admitted. 7.
  • MDE symptoms Item 2 positive response for anhedonia
  • BMI between 18 and 40 kg/m 2 (inclusive).
  • a woman of childbearing potential must have a negative highly sensitive serum ( ⁇ - hCG) pregnancy test at screening and a negative urine pregnancy test predose on Day 1 of the double-blind phase prior to randomization. 12.
  • Contraceptive use by men or women should be consistent with local regulations regarding the use of contraceptive methods for subjects in clinical studies. 13.
  • a woman must be either: Postmenopausal Permanently sterile Of childbearing potential and practicing a highly effective method of contraception (failure rate of ⁇ 1% per year when used consistently and correctly).
  • a woman must not to donate eggs (ova, oocytes) or freeze for future use for the purposes of assisted reproduction during the study and for a period of at least 1 month after receiving the last dose of study medication. 15.
  • spermatogenesis cycle (defined as approximately 3 months) after receiving the last dose of study medication, a man: who is sexually active with a woman of childbearing potential must use a barrier method of contraception (e.g., condom with spermicidal foam/gel/film/cream/suppository) and his female partner must use a highly effective method of contraception.
  • a barrier method of contraception e.g., condom with spermicidal foam/gel/film/cream/suppository
  • his female partner must use a highly effective method of contraception.
  • who is sexually active with a woman who is pregnant must use a condom. must not to donate sperm.
  • Exclusion Criteria 1. History of treatment-resistant MDD, defined as a lack of response to 2 or more adequate antidepressant treatments in the current episode, as indicated by no or minimal improvement ( ⁇ 25% improvement) when treated with an antidepressant of adequate dose (per MGH-ATRQ) and duration (at least 6 weeks). 2. Current or prior DSM-5 diagnosis of a psychotic disorder or MDD with psychotic features, bipolar or related disorders (confirmed by the SCID-CT), intellectual disability (DSM-5 diagnostic codes 317, 318.0, 318.1, 318.2, 315.8, and 319), autism spectrum disorder, borderline personality disorder, antisocial personality disorder, histrionic personality disorder, narcissistic personality disorders or somatoform disorders. 3.
  • History of moderate to severe substance use disorder including alcohol use disorder according to DSM-5 criteria within 6 months before screening or positive test results for alcohol and/or drugs of abuse (e.g., opiates [including methadone], cocaine, amphetamines, methamphetamines, cannabinoids, CBD, barbiturates, MDMA) at screening or at baseline.
  • drugs of abuse e.g., opiates [including methadone], cocaine, amphetamines, methamphetamines, cannabinoids, CBD, barbiturates, MDMA
  • One retest during screening is allowed.
  • Tobacco and caffeine use are not exclusionary. 7.
  • Subjects reporting suicidal ideation with intent to act or suicidal behavior prior to the start of the double-blind treatment phase should be excluded.
  • Cognitive impairment that would render the informed consent invalid or limit the ability of the subject to comply with the study requirements.
  • Subject has neurodegenerative disorder (e.g., Alzheimer's disease, vascular dementia, Parkinson's disease with clinical evidence of cognitive impairment) or evidence of MCI.
  • Current or history of seizures uncomplicated childhood febrile seizures with no sequelae are not exclusionary). 11.
  • liver cirrhosis e.g., esophageal varices, ascites, and increased prothrombin time
  • ALT or AST values >3 ⁇ the ULN or total bilirubin >1.5 ⁇ the ULN in the screening phase. Repeat of screening test for abnormal ALT and AST is permitted during the screening period there is an alternative explanation for the out of range value. 13.
  • the subject may participate. 14.
  • Positive test result for drugs of abuse e.g., barbiturates, methadone, opiates, cocaine, PCP, MDMA, and amphetamine/methamphetamine
  • Subjects who have a positive test result at screening due to prescribed psychostimulants taken for any indication must discontinue the medication at least 2 weeks before Day 1 of the double-blind treatment phase (prior to randomization).
  • the result of the Day 1 (prior to randomization) test for drugs of abuse must be negative for the subject to be randomized.
  • Subjects who have a positive test result at screening due to prescribed/over-the-counter opiates or barbiturates may be permitted to continue in the screening phase if the medication is discontinued at least 1 week or 5 half-lives, whichever is longer, before Day 1 of the double-blind treatment phase (prior to randomization).
  • the result of the Day 1 (prior to randomization) test for drugs of abuse must be negative for the subject to be randomized. Intermittent use of cannabinoids prior to the start of the screening phase is not exclusionary as long as the subject does not meet the criteria for substance use disorder.
  • a positive test for cannabinoids at the start of the screening phase is not exclusionary; however, a positive test result for cannabinoids predose on Day 1 of the double-blind treatment phase is exclusionary. 16. Taking a total daily dose of benzodiazepines greater than the equivalent of 6 mg/day of lorazepam at the start of the screening phase. 17. Recent (last 3 months) history of, or current signs and symptoms of: Severe renal insufficiency (creatinine clearance ⁇ 30 mL/min) Clinically significant or unstable cardiovascular, respiratory, gastrointestinal, neurologic, hematologic, rheumatologic, immunologic or endocrine disorders. Uncontrolled Type 1 or Type 2 diabetes mellitus.
  • Subjects with Type 1 or Type 2 diabetes mellitus who are controlled may be eligible to participate if otherwise medically healthy, and if on a stable regimen of glucose-lowering medications for at least 2 months prior to screening). 18.
  • Current signs/symptoms of hypothyroidism or hyperthyroidism For subjects with a history of thyroid disease and for subjects who, regardless of thyroid history have the TSH value out of range, a FT 4 test will be conducted. If the FT4 value is abnormal and considered to be clinically significant the subject is not eligible. 19.
  • Subjects with a pre-existing history of thyroid disease/disorder who are treated with thyroid hormones need to be on a stable dosage for 3 months prior to the start of the screening phase.
  • Subjects taking thyroid supplementation for antidepressant purposes are not allowed.
  • Ongoing psychological treatments e.g., Cognitive Behavior Therapy, Interpersonal Psychotherapy, Psychodynamic Psychotherapy etc.
  • a subject who has been receiving ongoing psychological treatment for a period of greater than 6 weeks is eligible, if psychological treatment to be of stable duration and frequency.
  • an investigational drug including investigational vaccines
  • used an invasive investigational medical device within 60 days before the start of the screening phase, or has participated in 2 or more MDD or other psychiatric condition clinical interventional studies (with different investigational medication) in the previous 1 year before the start of the screening phase, or is currently enrolled in an investigational interventional study.
  • 29. A woman who is pregnant, breastfeeding, or planning to become pregnant while enrolled or within 6 weeks after the last dose of the study medication.
  • 30. Plans to father a child while enrolled or within 90 days after the last dose of study intervention.
  • 31. Diagnosis of acquired immunodeficiency syndrome. Human immunodeficiency virus testing is not required.
  • Any condition or situation/circumstance for which participation would not be in the best interest of the subject e.g., compromise the well-being) or that could prevent, limit, or confound the protocol specified assessments.
  • the assessment of primary and secondary (key and other) endpoints will be conducted on the FAS which includes adult (not elderly) subjects with MDD ANH+ who took at least 1 dose of study medication.
  • Safety Objectives (All): The following safety endpoints will be assessed separately for the adult and elderly subjects; the safety analysis set for each age group will include all randomized subjects who have received at least one dose of study medication:
  • Prohibited therapies Subjects must not use the following medications or food supplements prior to or during the study, as indicated, except to treat an AE or breakthrough symptoms, preferably after the EOT visit:
  • Example 8 a Randomized, Double-Blind, Multicenter, Placebo-Controlled Study to Evaluate the Efficacy, Safety, and Tolerability of Fixed Doses of Aticaprant 5 mg and 10 mg as Adjunctive Therapy in Adult and Elderly Subjects with MDD with Prominent Anhedonia and Inadequate Response to Current Antidepressant Therapy
  • Study Design An 8-week, multicenter, double-blind, randomized, placebo-controlled study to assess the efficacy, safety, and tolerability of aticaprant in adult and elderly subjects (18 to 74 years) who have MDD with prominent anhedonia and who have had an inadequate response to a SSRI or a SNRI in the current depressive episode. See, FIG. 35 .
  • Subjects who have completed the double-blind treatment phase may participate in an open-label long-term safety study.
  • Sample Size and Randomization Approximately 624 adult ( ⁇ 65 years) and elderly ( ⁇ 65 years) subjects with MDD with prominent anhedonia will be randomized in a 2:1:1 ratio to adjunctive placebo, 5-mg aticaprant, or 10-mg aticaprant to achieve a minimum of 556 adult subjects meeting predefined criteria for MDD with prominent anhedonia eligible to be included in the primary efficacy analysis set. Randomization will be stratified by study site, age group (adult, elderly) and baseline MADRS total score. All subjects will continue their baseline antidepressant (SSRI/SNRI) during the entire study.
  • SSRI/SNRI baseline antidepressant
  • Inclusion Criteria 1. Age of 18 to 74 years (inclusive). 2. Medically stable on the basis of physical examination (including a brief neurological examination), medical history, vital signs (including blood pressure), and 12-lead ECG performed at screening and baseline. 3. Medically stable on the basis of clinical laboratory tests performed at screening. If the results of the serum chemistry panel, hematology, or urinalysis are outside the normal reference ranges, retesting of an abnormal lab values that may lead to exclusion will be allowed once during the screening phase. 4. Meet DSM-5 diagnostic criteria for recurrent or single episode MDD, without psychotic features (DSM-5 296.22, 296.23, 296.32, or 296.33), based upon clinical assessment and confirmed by the SCID-CT.
  • SSRI/SNRI antidepressants
  • An inadequate response is defined as 26% to ⁇ 50% reduction in depressive symptom severity and overall good tolerability, as assessed by the MGH-ATRQ.
  • An adequate trial is defined as an antidepressant treatment for at least 6 weeks (and no greater than 12 months in the current episode) at or above the stable therapeutic dose specified in the MGH-ATRQ, must include the subject's current antidepressant treatment. If the subject has received 2 SSRI/SNRI treatments of sufficient dose and duration in the current episode, and has shown ⁇ 25% improvement to both, then the subject would not qualify based on exclusion criterion (first exclusion criterion). 8. The current major depressive episode, depression symptom severity, presence of anhedonia and antidepressant treatment response in the current depressive episode, must be confirmed.
  • any one of the following SSRI or SNRI for depressive symptoms in any formulation and available in the participating country citalopram, duloxetine, escitalopram, fluvoxamine, fluoxetine, milnacipran, levomilnacipran, paroxetine, sertraline, venlafaxine, desvenlafaxine at a stable dose (at therapeutic dose level) for at least 6 weeks, and for no greater than 12 months in the current episode, at screening.
  • the SSRI/SNRI needs to be approved for the treatment of MDD. 9.
  • BMI between 18 and 40 kg/m 2 (inclusive).
  • Postmenopausal A postmenopausal state is defined as no menses for 12 months without an alternative medical cause.
  • a high FSH level in the postmenopausal range based on the reference range of the central laboratory may be used to confirm a postmenopausal state in women not using hormonal contraception or hormonal replacement therapy, however in the absence of 12 months of amenorrhea, a single FSH measurement is insufficient.
  • Permanently sterile Of childbearing potential and practicing a highly effective method of contraception (failure rate of ⁇ 1% per year when used consistently and correctly). Remains on a highly effective method and for at least 1 month after the last dose of study medication.
  • a woman must not donate eggs (ova, oocytes) or freeze for future use for the purposes of assisted reproduction during the study and for a period of at least 1 month after receiving the last dose of study medication.
  • a man (a) who is sexually active with a woman of childbearing potential must use a barrier method of contraception and his female partner must use a highly effective method of contraception; (b) who is sexually active with a woman who is pregnant must use a condom; (c) must not donate sperm.
  • Exclusion Criteria 1. History of treatment-resistant MDD, defined as a lack of response to 2 or more adequate antidepressant treatments in the current episode, as indicated by no or minimal improvement ( ⁇ 25% improvement) when treated with an antidepressant of adequate dose (per MGH-ATRQ) and duration (at least 6 weeks). 2. Current or prior DSM-5 diagnosis of a psychotic disorder or MDD with psychotic features, bipolar or related disorders (confirmed by the SCID-CT), intellectual disability (DSM-5 diagnostic codes 317, 318.0, 318.1, 318.2, 315.8, and 319), autism spectrum disorder, borderline personality disorder, antisocial personality disorder, histrionic personality disorder, narcissistic personality disorders or somatoform disorders. 3.
  • History of moderate to severe substance use disorder including alcohol use disorder according to DSM-5 criteria within 6 months before screening or positive test results for alcohol and/or drugs of abuse (e.g., opiates [including methadone], cocaine, amphetamines, methamphetamines, cannabinoids, CBD, barbiturates, MDMA) at screening or at baseline.
  • drugs of abuse e.g., opiates [including methadone], cocaine, amphetamines, methamphetamines, cannabinoids, CBD, barbiturates, MDMA
  • One retest during screening is allowed.
  • Tobacco and caffeine use are not exclusionary. 7.
  • Subjects reporting suicidal ideation with intent to act or suicidal behavior prior to the start of the double-blind treatment phase should be excluded.
  • Cognitive impairment that would render the informed consent invalid or limit the ability of the subject to comply with the study requirements.
  • Subject has neurodegenerative disorder (e.g., Alzheimer's disease, vascular dementia, Parkinson's disease with clinical evidence of cognitive impairment) or evidence of MCI.
  • Current or history of seizures uncomplicated childhood febrile seizures with no sequelae are not exclusionary). 11.
  • ECG electrocardiogram
  • liver cirrhosis e.g., esophageal varices, ascites, and increased prothrombin time
  • ALT or AST values ⁇ 3 ⁇ the ULN or total bilirubin >1.5 ⁇ the ULN in the screening phase. Repeat of screening test for abnormal ALT and AST is permitted during the screening period provided there is an alternative explanation for the out of range value. 13.
  • the subject may participate in the study. 14.
  • Positive test results for drugs of abuse e.g., barbiturates, methadone, opiates, cocaine, PCP, MDMA, and amphetamine/methamphetamine
  • Subjects who have a positive test result at screening due to prescribed psychostimulants taken for any indication must discontinue the medication at least 2 weeks before Day 1 of the double-blind treatment phase (prior to randomization).
  • the result of the Day 1 (prior to randomization) test for drugs of abuse must be negative for the subject to be randomized.
  • subjects who have a positive test result at screening due to prescribed/over-the-counter opiates or barbiturates may be permitted to continue in the screening phase if the medication is discontinued at least 1 week or 5 half-lives, whichever is longer, before Day 1 of the double-blind treatment phase (prior to randomization).
  • the result of the Day 1 (prior to randomization) test for drugs of abuse must be negative for the subject to be randomized. 16.
  • Intermittent use of cannabinoids prior to the start of the screening phase is not exclusionary as long as the subject does not meet the criteria for substance use disorder.
  • a positive test for cannabinoids at the start of the screening phase is not exclusionary; however, a positive test result for cannabinoids predose on Day 1 of the double-blind treatment phase is exclusionary. 17. Taking a total daily dose of benzodiazepines greater than the equivalent of 6 mg/day of lorazepam at the start of the screening phase. 18. Recent (last 3 months) history of, or current signs and symptoms of: Severe renal insufficiency (creatinine clearance ⁇ 30mL/min) Clinically significant or unstable cardiovascular, respiratory, gastrointestinal, neurologic, hematologic, rheumatologic, immunologic or endocrine disorders. Uncontrolled Type 1 or Type 2 diabetes mellitus.
  • Subjects with Type 1 or Type 2 diabetes mellitus who are controlled may be eligible to participate if otherwise medically healthy, and if on a stable regimen of glucose- lowering medications for at least 2 months prior to screening). 19. Current signs/symptoms of hypothyroidism or hyperthyroidism. For subjects with a history of thyroid disease and for subjects who, regardless of thyroid history have the TSH value out of range, a FT 4 test will be conducted. If the FT4 value is abnormal and considered to be clinically significant the subject is not eligible. 20.
  • Subjects with a pre-existing history of thyroid disease/disorder who are treated with thyroid hormones need to be on a stable dosage for 3 months prior to the start of the screening phase. Subjects taking thyroid supplementation for antidepressant purposes are not allowed. 21. Cushing's Disease, Addison's Disease, primary amenorrhea, or other evidence of significant medical disorders of the hypothalamic-pituitary-adrenal axis. 22. Significant medical illness, particularly unstable medical problem 23. Ongoing psychological treatments (e.g., Cognitive Behavior Therapy, Interpersonal Psychotherapy, Psychodynamic Psychotherapy etc.), initiated within 6 weeks prior to start of screening. A subject who has been receiving ongoing psychological treatment for a period of greater than 6 weeks is eligible. 24. Significant medical illness, particularly unstable medical problem. 25.
  • Clinically-relevant GI complaints (unless symptoms of Axis I disorder) at screening or baseline or history of gastric disease (including but not limited to documented peptic ulcer disease, gastritis [including atrophic gastritis], upper GI bleeding, Barret's esophagus, Crohn's disease, ulcerative colitis, GI precancerous conditions or any other clinically-relevant GI disease irritable bowel syndrome).
  • gastric disease including but not limited to documented peptic ulcer disease, gastritis [including atrophic gastritis], upper GI bleeding, Barret's esophagus, Crohn's disease, ulcerative colitis, GI precancerous conditions or any other clinically-relevant GI disease irritable bowel syndrome).
  • gastric disease including but not limited to documented peptic ulcer disease, gastritis [including atrophic gastritis], upper GI bleeding, Barret's esophagus, Crohn's disease, ulcerative colitis, GI pre
  • an investigational drug including investigational vaccines
  • used an invasive investigational medical device within 60 days before the start of the screening phase, or has participated in 2 or more MDD or other psychiatric condition clinical interventional studies (with different investigational medication) in the previous 1 year before the start of the screening phase, or is currently enrolled in an investigational interventional study.
  • 32. A woman who is pregnant, breastfeeding, or planning to become pregnant while enrolled in this study or within 6 weeks after the last dose of the study medication.
  • 33. Plans to father a child while enrolled in this study or within 90 days after the last dose of study intervention.
  • 34. Diagnosis of acquired immunodeficiency syndrome. Human immunodeficiency virus testing is not required for this study.
  • Any condition or situation/circumstance for which participation would not be in the best interest of the subject e.g., compromise the well-being) or that could prevent, limit, or confound the protocol specified assessments.
  • FAS full analysis set
  • Safety Objectives (All): The following safety endpoints will be assessed separately for the adult and elderly subjects; the safety analysis set for each age group will include all randomized subjects who have received at least one dose of study medication:
  • Subjects must not use the following medications or food supplements prior to or during the study, as indicated, except to treat an AE or breakthrough symptoms, preferably after the EOT visit:
  • a total of approximately 80 qualified healthy adult participants are planned to be enrolled in this study: 24 participants each are to be enrolled to ensure at least 20 participants in each part complete all required PK assessments. Eligible participants can be enrolled in more than one part of the study if sufficient wash-out period is completed between periods by participants.
  • PK sampling will be done up to 120 hours (Day 6).
  • Each dosed participant will have a safety follow-up on Day 10 to Day 14 after last dose of the study intervention.
  • Part 1 of the study involves determination of relative bioavailability for tablet (Formulation Concept 1, i.e., unmilled aticaprant formulation, see Table 10) and capsule formulations (see Example 6, study design, for description of capsule formulation) and dose proportionality and food effect for tablet formulation (Formulation Concept 1) in healthy adult participants ( FIG. 25 ).
  • Part 1 will consist of Subpart 1A and Subpart 1B consisting of a total of 4 periods.
  • Subpart 1A is a randomized, open label, 3-way crossover, 3-period study to be conducted in 24 healthy participants to evaluate the relative bioavailability of a single dose of 10 mg aticaprant administered as 1 ⁇ 10 mg oral tablet (Formulation Concept 1) under fasted conditions (Treatment B) compared to 10 mg aticaprant administered as 2 ⁇ 5 mg oral capsules under fasted conditions (Treatment A) and to evaluate the dose proportionality of a single dose of 5 mg aticaprant administered as 1 ⁇ 5 mg oral tablet (Formulation Concept 1) under fasted conditions (Treatment C) compared to the potential Phase 3 oral tablet (Formulation Concept 1) under fasted conditions (1 ⁇ 10 mg, Treatment B; Table 49).
  • Subpart 1B consists of a fourth period to evaluate the food effect of a single dose of 10 mg aticaprant administered as 1 ⁇ 10 mg oral tablet (Formulation Concept 1) under fed conditions (Treatment D; Table 50 and Table 52).
  • a preliminary PK analysis will be conducted at the end of the food effect part (Subpart 1B) for all the periods from Part 1 and will include the food effect data.
  • Treatment Formulation Dose Food D Formulation Concept 1 10 mg Fed (10 mg oral tablet) (1 ⁇ 10 mg) Treatment D: 1 ⁇ 10 mg Formulation Concept 1 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
  • Treatment D 1 ⁇ 10 mg Formulation Concept 1 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
  • Part 2 of the study involves determination of relative bioavailability for tablet (Formulation Concept 2, i.e., milled (microfine) aticaprant formulation; see Table 10) and capsule formulations (see Example 6, study design, for description of capsule formulation) and dose proportionality and food effect for tablet formulation (Formulation Concept 2) in healthy adult participants ( FIG. 26 ).
  • Part 2 will consist of Subpart 2A and Subpart 2B consisting of a total of 4 periods.
  • Subpart 2A is a randomized, open label, 3-way crossover, 3-period study to be conducted in 24 healthy participants to evaluate the relative bioavailability of a single dose of 10 mg aticaprant administered as 1 ⁇ 10 mg oral tablet (Formulation Concept 2) under fasted conditions (Treatment F) compared to 10 mg aticaprant administered as 2 ⁇ 5 mg oral capsules under fasted conditions (Treatment E) and to evaluate the dose proportionality of a single dose of 5 mg aticaprant administered as 1 ⁇ 5 mg oral tablet (Formulation Concept 2) under fasted conditions (Treatment G) compared to the potential Phase 3 oral tablet (Formulation Concept 2) under fasted conditions (1 ⁇ 10 mg, Treatment F; Table 53).
  • Subpart 2B consists of a fourth period to evaluate the food effect of a single dose of 10 mg aticaprant administered as 1 ⁇ 10 mg oral tablet (Formulation Concept 2) under fed conditions (Treatment H; Tables 54 and 56).
  • a preliminary PK analysis will be conducted at the end of the food effect part (Subpart 2B) for all the periods from Part 2 and will include the food effect data.
  • Treatment Formulation Dose Food H Formulation Concept 2 10 mg Fed (10 mg oral tablet) (1 ⁇ 10 mg) Treatment H: 1 ⁇ 10 mg Formulation Concept 2 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
  • Treatment H 1 ⁇ 10 mg Formulation Concept 2 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
  • Day 1 of a treatment period is the first day of the washout period (also in between the study parts, if applicable).
  • Participants will be fasting in Part 1A and Part 2A. Participants will have been fed in Parts 1B and 2B. For a fasted condition, participants will fast (nothing to eat or drink except noncarbonated water) overnight for at least 10 hours before and until 4 hours after study intervention administration during each fasted treatment period. Approximately, 4 hours post-dose and after the 4-hour PK sampling, a standard lunch will be served at the study-site. Intake of water is allowed until 2 hours before the intake of the study intervention. Thereafter, water intake is only allowed for study intervention intake and for breakfast, if applicable. Drinking of water is allowed ad libitum from approximately 2 hours after dosing.
  • participant will consume, after an overnight fast (at least 10 hours), a standardized high-fat breakfast within a 20-minute period.
  • a high-fat (approximately 50 percent of total caloric content of the meal) and high-calorie (approximately 800 to 1000 calories) meal is recommended for food effect bioavailability studies (e.g., 2 strips of fried bacon, 2 eggs fried in butter, 4 ounces [120 gram] hash brown potatoes fried in butter, 2 buttered pieces of whole wheat bread, and 240 mL whole milk). Study intervention will be administered approximately 30 minutes after the start of the breakfast.
  • Plasma concentrations will be determined for aticaprant. Blood samples for determination of plasma concentrations of aticaprant will be collected predose and at the postdose time points starting on Day 1 as indicated in the Tables 57-58.
  • Parts 1 and 2 of the study will start at any time, irrespective of other parts of the study.
  • the study will consist of a screening phase (within 28 days before study intervention administration), an open-label treatment phase (Day ⁇ 1 until Day 5, with single-dose treatment on Day 1 and at least 96 hours of PK for Part 1 and 120 hours of PK (Day 6) for Part 2).
  • a total of approximately 80 qualified healthy adult participants are planned to be enrolled in this study: 24 participants each are to be enrolled in Parts 1 and 2 to ensure at least 20 participants in each part complete all required PK assessments. Eligible participants can be enrolled in more than one part of study if sufficient wash-out period is completed between periods by participants.
  • Type of Participant and Disease Characteristic Healthy on the basis of physical examination, medical history (screening only), vital signs, and 12-lead ECG performed at screening and admission to the clinical unit on Day ⁇ 1 of the first treatment period. Minor abnormalities in ECG, which are not considered to be of clinical significance are acceptable. Healthy on the basis of clinical laboratory tests performed at screening and at admission to the study center. If the results of the serum chemistry panel, hematology, or urinalysis are outside the normal reference ranges, the participant may be included.
  • retesting of an abnormal lab value(s) that may lead to exclusion will be allowed once during the screening phase.
  • ALT, AST, alkaline phosphatase and bilirubin must be within 1.5 times of upper limit of normal range and not clinically significant.
  • Weight BMI weight [kg]/height 2 [m] 2 ) between 18 and 29.9 kg/m 2 (inclusive), and body weight not less than 50 kg.
  • Sex and Contraceptive/Barrier Requirements Male or female All women participants must have a negative highly sensitive serum ⁇ -hCG pregnancy test at screening and all women participants must have a negative urine pregnancy test on Day ⁇ 1 of each treatment period. A woman must be a. Not of childbearing potential b. Of childbearing potential and Practicing a highly effective method of contraception (failure rate of ⁇ 1% per year when used consistently and correctly) and agrees to remain on a highly effective method while receiving study intervention and until 90 days after last dose - the end of relevant systemic exposure. A woman must agree not to donate eggs (ova, oocytes) or freeze for future use for the purposes of assisted reproduction during the study and for a period of at least 90 days after receiving the last dose of study intervention.
  • a male participant must agree to use a barrier method of contraception (e.g., condom) when engaging in any activity that allows for passage of ejaculate to another person.
  • a barrier method of contraception e.g., condom
  • a male participant who is sexually active with a woman who is pregnant must use a condom.
  • Male participants should also be advised of the benefit for a female partner to use a highly effective method of contraception as condom may break or leak.
  • a male participant must agree not to donate sperm for the purpose of reproduction during the study and for a minimum of 1 spermatogenesis cycle (defined as approximately 3 months) after receiving the last dose of study intervention.
  • Blood pressure (after the participant is [supine] for 5 minutes) between 90 mmHg and 140 mmHg systolic, inclusive, and no higher than 90 mmHg diastolic at screening and Day ⁇ 1 of each treatment period.
  • a 12-lead ECG consistent with normal cardiac conduction and function, at screening and Day ⁇ 1 of each treatment period, including: Sinus rhythm Heart rate between 40 and 100 beats per minute, extremes included QTc interval ⁇ 450 ms for males, ⁇ 470 for females (corrected cf. Fridericia 1920; ICH E14 2005) QRS interval of ⁇ 120 ms PR interval ⁇ 210 ms Morphology consistent with healthy cardiac conduction and function
  • Medical Conditions History of or current significant medical illness including (but not limited to) cardiac arrhythmias or other cardiac disease, hematological disease, lipid abnormalities, bronchospastic respiratory disease, diabetes mellitus, renal or hepatic insufficiency, thyroid disease, neurologic or psychiatric disease, seizure disorder (uncomplicated childhood febrile seizures with no sequelae are not exclusionary) Parkinson's disease, infection, hypertension, vascular disorder, significant pulmonary disease, or any other illness. History of malignancy within 5 years before screening (exceptions are squamous and basal cell carcinomas of the skin and carcinoma in situ of the cervix, or malignancy, which is considered cured with minimal risk of recurrence).
  • GI complaints per clinical judgment at screening or baseline or history of documented gastric disease (including but not limited to documented peptic ulcer disease, gastritis [including atrophic gastritis], upper GI bleeding, Barret's esophagus, Crohn disease, ulcerative colitis, GI precancerous conditions or any other clinically relevant GI disease irritable bowel syndrome).
  • Participant has current or past homicidal ideation/intent within the last 6 months, or has current or past suicidal ideation with some intent to act within 6 months prior to the start of the screening phase, corresponding to a response of “Yes” on Item 4 (active suicidal ideation with some intent to act, without specific plan) or Item 5 (active suicidal ideation with specific plan and intent) for suicidal ideation on the C-SSRS, or a history of suicidal behavior within the past year prior to the start of the screening phase. Participants reporting suicidal ideation with intent to act or suicidal behavior on Day ⁇ 1 prior to the start of the treatment should be excluded. Serology positive for HbsAg, HCV antibodies or HIV antibodies at screening.
  • any prescription or nonprescription medication including vitamins, herbal supplements, and mineral supplements
  • Prior/Concurrent Clinical Study Experience Received an investigational intervention (including investigational vaccines) or used an invasive investigational medical device within at least 1 month, before the planned first dose of study intervention or is currently enrolled in an investigational study. Pregnant, or breast-feeding, or planning to become pregnant while enrolled in this study or within 1 month after the last dose of study intervention. Plans to father a child while enrolled in this study or within 3 months after the last dose of study intervention. Diagnostic Assessments Had major surgery, (e.g., requiring general anesthesia) within 12 weeks before screening, or will not have fully recovered from surgery, or has surgery planned during the time the participant is expected to participate in the study.
  • major surgery e.g., requiring general anesthesia
  • Study intervention will be taken in the morning on Day 1 of each treatment period with 240 mL of noncarbonated water. Study intervention must be swallowed whole and not chewed, divided, dissolved, or crushed.
  • Participants receiving study intervention in the fed condition will fast overnight (at least 10 hours) followed by the consumption of a high-fat breakfast within a 20-minute period.
  • the high-fat breakfast will be the same on the day of dosing in the fed period (Period 4 for Part 1 and Part 2).
  • Study intervention will be administered approximately 30 minutes after the start of the breakfast.
  • Noncarbonated water will be allowed up to 2 hours before study intervention administration. Participants will continue fasting until at least 4 hours after study intervention administration. At approximately 2 hours after dosing (but not earlier), drinking of water is allowed ad-libitum onwards. A standardized lunch will be served on Day 1 for all participants after collection of the 4-hour PK blood sample. Participant can resume their normal diet after 4 hours.
  • the exact composition of breakfast and the lunch will be recorded.
  • the lunch will be the same in all intervention periods.
  • the exact start and end time of breakfast, as well as the start time of lunch will be recorded, together with any deviation regarding the timing of the meals.
  • Aticaprant will be supplied for this study as 5 mg capsule and 5 mg and 10 mg tablet formulation.
  • All therapies prescription or over-the-counter medications, including vaccines, vitamins, herbal supplements; non-pharmacologic therapies such as electrical stimulation, acupuncture, special diets, exercise regimens, or other specific categories of interest
  • Recorded information will include a description of the type of therapy, duration of use, dosing regimen, route of administration, and indication. Modification of an effective preexisting therapy should not be made for the explicit purpose of entering a participant into the study.
  • All concomitant therapies that are considered to be a CYP inhibitor or inducer or a transport inhibitor or inducer are disallowed during the study and disallowed for at least 1 month before receiving the first intake of study intervention.
  • Women using hormonal contraceptives as a means of birth control must continue to use the same hormonal contraceptives throughout the study. Women using hormone replacement therapy must continue to use the same hormone replacement therapy throughout the study.
  • Tables 59-60 summarize the frequency and timing of PK measurements applicable to this study.
  • assessments should preferably take place in the following order: 12-lead ECG, vital signs (supine blood pressure, pulse/heart rate), blood/CSF draws for PK or laboratory measurements, and C-SSRS. Blood collections for PK assessments should be kept as close to the specified time as possible. Other measurements may be done earlier than specified timepoints, if needed.
  • the maximum amount of blood drawn from each participant will not exceed 500 mL.
  • the total volume of CSF collected per participant enrolled in CSF PK will not exceed 52.3 mL which is considered to be acceptable considering the daily CSF production rate.
  • Body temperature, pulse/heart rate, respiratory rate, blood pressure will be assessed.
  • Blood pressure and pulse/heart rate measurements will be assessed with a completely automated device consisting of an inflatable cuff and an oscillatory detection system. All values will be registered on a built-in recorder so that measurements are observer-independent. Blood pressure and pulse/heart rate measurements will be recorded after 5 minutes rest in a quiet setting without distractions (e.g., television, cell phones) in a supine position.
  • distractions e.g., television, cell phones
  • participant During the collection of ECGs, participants should be in a quiet setting without distractions (e.g., television, cell phones). Participants should rest in a supine position for at least 5 minutes before ECG collection and should refrain from talking or moving arms or legs. If blood sampling or vital sign measurement is scheduled for the same time point as ECG recording, they should preferably take place in the following order: 12-lead ECG, vital signs (supine blood pressure, pulse/heart rate), blood/CSF draws for PK, or laboratory measurements, and C-SSRS.
  • a quiet setting without distractions (e.g., television, cell phones). Participants should rest in a supine position for at least 5 minutes before ECG collection and should refrain from talking or moving arms or legs. If blood sampling or vital sign measurement is scheduled for the same time point as ECG recording, they should preferably take place in the following order: 12-lead ECG, vital signs (supine blood pressure, pulse/heart rate), blood/CSF draws for PK, or laboratory measurements, and C-SS
  • the C-SSRS is a measure of the spectrum of suicidal ideation and behavior that was developed to assess severity and track suicidal events through any treatment studies. It is a clinical interview to assess the risk of treatment-emergent suicidal ideation/behavior.
  • a baseline/screening version of the C-SSRS will be completed at screening, and subsequently a since-your-last-visit version of the C-SSRS will be completed predose on Day ⁇ 1, prior to discharge on Day 5 of each treatment period (for Part 1), prior to discharge on Day 6 of each treatment period (for Part 2) and at end-of-study or early withdrawal.
  • Fundoscopy is a form of examination of the fundus of the eye.
  • the WelchAllyn® PanOpticTM Ophthalmoscope (model 11810) is used according to the internal standard operating procedure.
  • Plasma and CSF samples will be used to evaluate the PK of aticaprant.
  • Blood samples (4 mL each) for determination of aticaprant plasma concentrations will be collected at the time points indicated in Tables 59-60.
  • Plasma samples will be analyzed to determine concentrations of aticaprant using a validated, specific, and sensitive Liquid chromatography coupled to tandem mass spectrometry (LC-MS/MS) method.
  • LC-MS/MS Liquid chromatography coupled to tandem mass spectrometry
  • the following plasma PK parameters of aticaprant will be determined.
  • a noncompartmental model with extravascular input will be used for the pharmacokinetic analysis.
  • the intra-participant coefficient of variation (CV) for PK parameters (AUC ⁇ and C max ) is estimated to be between 8.3% and 10.4% for AUC ⁇ and between 14.4% and 24.3% for C max .
  • CV intra-participant coefficient of variation
  • the statistical analysis plan will be finalized prior to DBL and it will include a more technical and detailed description of the statistical analyses described in this section. This section is a summary of the planned statistical analyses of the most important endpoints.
  • Factors that may influence the plasma concentrations e.g., vomiting, high predose concentration
  • Reasons for exclusion of a participant or a sample from the analysis include, but are not limited, to the following:
  • descriptive statistics including arithmetic mean, standard deviation (SD), coefficient of variation (CV), geometric mean, median, minimum, and maximum will be calculated for the aticaprant plasma concentrations at each sampling time and for all PK parameters of aticaprant.
  • the primary objective of the statistical analysis will be to estimate the relative bioavailability of aticaprant test formulations with respect to aticaprant reference formulations, dose proportionality of aticaprant test formulations, and the effect of food on the PK of aticaprant test formulations.
  • the primary parameters of interest for the statistical analysis will be the log-transformed estimated AUCs, AUC last , AUC ⁇ , and C max .
  • the AUC ⁇ will be rejected as primary parameter for a group if more than half of the participants do not have a reliable value. If one of PK parameter of interest is not estimable for a given participant in one or more periods, the participant's data will not be included in the statistical analysis of that particular PK parameter.
  • This study included two parts with similar study design to investigate two different tablet formulation concepts with part 1 (unmilled API tablet) and part 2 (milled API tablet).
  • the evaluations included relative bioavailability of immediate-release tablet formulation (1 ⁇ 10 mg) versus API in capsule formulation (2 ⁇ 5 mg), dose-proportionality between 10 and 5 mg tablet strengths, and food effect assessment at 10 mg of tablet strength.
  • Each part consisted of a subpart A and subpart B with a total of 4 periods.
  • Subpart A was a randomized, open label, 3-way crossover, 3-period study conducted in 24 healthy participants to evaluate the relative bioavailability of a single dose of 10 mg aticaprant administered as 1 ⁇ 10 mg oral tablet under fasted conditions compared to 10 mg aticaprant administered as 2 ⁇ 5 mg oral capsules under fasted conditions and to evaluate the dose proportionality of a single dose of 5 mg aticaprant administered as 1 ⁇ 5 mg oral tablet under fasted conditions compared to the 1 ⁇ 10 mg oral tablet under fasted conditions.
  • the same 24 participants who completed subpart A were enrolled in subpart B which consisted of a fourth period to evaluate the food effect of a single dose of 10 mg aticaprant administered as 1 ⁇ 10 mg oral tablet under fed conditions.
  • the PK analysis results for part 1 including the PK parameters across treatments and statistical comparisons between treatments of interest are shown in Tables 62-65.
  • Table 62 summarizes PK parameters across treatments in Part 1.
  • Table 63 shows the statistical comparison results of the relative bioavailability of a 1 ⁇ 10 mg unmilled API tablet with 2 ⁇ 5 mg API in capsule formulation.
  • Table 64 shows the statistical comparison results of the dose-proportionality between 1 ⁇ 10 mg unmilled API tablet and 1 ⁇ 5 mg unmilled API tablet formulation.
  • Table 65 shows the statistical comparison results of food effect assessment with 1 ⁇ 10 mg unmilled API tablet when administered in the presence of high-fat diet to that of fasted condition.
  • PK parameters were comparable between unmilled API tablet (1 ⁇ 10 mg) and API in capsule (2 ⁇ 5 mg) formulation and the statistical assessment using calculated geometric mean ratios indicated that these two formulations are comparable and within the BE limits of criteria.
  • a dose-proportionality was established between 10 and 5 mg unmilled API tablet formulation strengths based on dose-dependent increase in PK parameters, a comparison of dose-normalized PK parameters and statistical assessment of calculated geometric mean ratios being within BE limits of 0.8 to 1.25.
  • unmilled API tablet formulation showed ⁇ 40% increase in AUC when 10 mg given in the presence of high-fat diet compared to fasted condition administration as evident from geometric mean ratio calculated for AUC.
  • Tables 66-73 The PK analysis results for part 2 (milled API tablet formulation) including the PK parameters across treatments and statistical comparisons between treatments of interest are shown in Tables 66-73.
  • Table 70 summarizes PK parameters across treatments in Part 2.
  • Table 71 shows the statistical comparison results of the relative bioavailability of a 1 ⁇ 10 mg milled API tablet with 2 ⁇ 5 mg API in capsule formulation.
  • Table 72 shows the statistical comparison results of the dose-proportionality between 1 ⁇ 10 mg milled API tablet and 1 ⁇ 5 mg milled API tablet formulation.
  • Table 73 shows the statistical comparison results of food effect assessment with 1 ⁇ 10 mg milled API tablet when administered in the presence of high-fat diet to that of fasted condition.
  • PK parameters were comparable between milled API tablet (1 ⁇ 10 mg) and API in capsule (2 ⁇ 5 mg) formulation and the statistical assessment using calculated geometric mean ratios indicated that these two formulations are comparable and within the BE limits of criteria.
  • a dose-proportionality was established between 10 and 5 mg milled API tablet formulation strengths based on dose-dependent increase in PK parameters, a comparison of dose-normalized PK parameters and statistical assessment of calculated geometric mean ratios being within BE limits of 0.8 to 1.25.
  • milled API tablet formulation showed ⁇ 30% increase in AUC when 10 mg given in the presence of high-fat diet compared to fasted condition administration as evident from geometric mean ratio calculated for AUC.
  • both the milled and unmilled API tablet formulations of 1 ⁇ 10 mg showed similar comparable exposures for aticaprant as those were observed with 10 mg reference API in capsule formulation (2 ⁇ 5 mg API in capsules) and were bioequivalent.
  • a dose-proportionality was observed between 10 and 5 mg tablet formulation strengths of each of the tablet formulation concepts of unmilled and milled API.
  • a modest food effect of ⁇ 30% (milled API tablet) and ⁇ 40% (unmilled API tablet) increase in AUC was observed at 10 mg with a slightly delayed median T max of 2.00 hours (milled API tablet) and 2.75 hours (unmilled API tablet) in presence of high-fat diet vs. 1.5 hours in the fasted condition administration.
  • a 40% food effect is not considered clinically relevant for many drugs given it is part of PK variability and no safety concerns exist at higher aticaprant exposures. Aticaprant can therefore be administered with or without food.
  • 1 ⁇ 10 mg unmilled API tablet concept may show similar exposures for aticaprant as those were observed with 10 mg reference API in capsule formulation (2 ⁇ 5 mg API in capsules)
  • Dose-proportionality may be observed between 1 ⁇ 10 mg unmilled API tablet vs. 1 ⁇ 5 mg unmilled API tablet
  • Treatment F 1 ⁇ 10 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting (Reference)
  • Treatment G 1 ⁇ 5 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting (Test)
  • Treatment G Dose Normalized to 10 mg Participants 100029 (incomplete PK profile) and 100031 (vomiting) from treatment F were excluded from the analysis.

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Abstract

The present disclosure relates to compositions, including oral compositions in the form of tablets, comprising aticaprant and methods of using the same.

Description

    CROSS REFERENCE TO RELATED APPLICATIONS
  • This application claims the benefit of U.S. Provisional Application No. 63/317,471, filed on Mar. 7, 2022, which is incorporated by reference herein.
    • TECHNICAL FIELD
  • The present disclosure relates to compositions, including oral compositions, comprising aticaprant and methods of using the same.
    • BACKGROUND
  • Kappa opioid receptors (KOR) and their native ligand dynorphin are localized in areas of the brain that effect reward and stress and may play a key role in mood, stress, and addictive disorders. Chronic stress, substance abuse, and acute withdrawal lead to increased dynorphin expression, activating KORs and subsequent downstream signaling pathways to inhibit mesolimbic dopamine surge, contributing to negative affective states. The behavioral pharmacology of KOR antagonism has been tested in animal models of anhedonia, depression, and anxiety and found to have meaningful effects that may translate to therapeutic benefit in humans. KOR antagonists may be effective for the treatment of patients with mood disorders, perhaps by modulating the negative affective state associated with stress response.
  • Anhedonia is one of the core symptoms of depression. At least mild symptoms of anhedonia are present in about 90% of patients suffering from major depressive disorder (MDD). Only about 50% of patients with MDD show a meaningful response (>50% improvement to a first line antidepressant treatment), leaving many patients with substantial persistent impairment. Therapeutic strategies such as switching antidepressants and using adjuvant drug treatments can improve response, however almost 40% of patients remain symptomatic and fail to achieve full remission.
  • What is needed are new compounds and treatments for patients having depression and, optionally, anhedonia.
    • SUMMARY
  • In some aspects, the disclosure provides pharmaceutical compositions comprising about 2 mg to about 20 mg aticaprant and a filler, wherein the composition comprises between about 0.1% to about 90% aticaprant by weight.
  • In other aspects, the disclosure provides oral tablets comprising about 5 mg aticaprant, wherein the oral tablet comprises a core tablet of about 100 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 30 mg microcrystalline cellulose, about 30 mg lactose monohydrate, about 2.5 mg croscarmellose sodium, and about 0.5 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 28.5 mg silicified microcrystalline cellulose, about 2.5 mg croscarmellose sodium, about 0.5 mg silica, colloidal anhydrous, and about 0.5 mg magnesium stearate.
  • In further aspects, the disclosure provides oral tablets comprising about 10 mg aticaprant, wherein the oral tablet comprises a core tablet of about 200 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 60 mg microcrystalline cellulose, about 60 mg lactose monohydrate, about 5 mg croscarmellose sodium, and about 1 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 57 mg silicified microcrystalline cellulose, about 5 mg croscarmellose sodium, about 1 mg silica, colloidal anhydrous, and about 1 mg magnesium stearate.
  • In yet other aspects, the disclosure provides pharmaceutical compositions comprising between about 2 mg and 20 mg aticaprant, wherein the composition has a pharmacokinetic (PK) profile comprising one or more of the following parameters after administration of the composition to a human after at least a 10-hour fast (dose-normalized to 10 mg): (a) a mean Cmax between about 20 and 45 ng/mL; (b) a mean AUCinfinity between about 250 and 450 h*ng/mL; (c) a mean AUClast between about 250 and 450 h*ng/mL; and (d) a median tmax between about 1 to 4 hours.
  • In still further aspects, the disclosure provides methods for treating major depressive disorder (MDD) in a human patient, the method comprising administering to the patient a pharmaceutical composition comprising between about 2 mg and 20 mg aticaprant, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with aticaprant, and wherein the administration of the pharmaceutical composition to the patient achieves a pharmacokinetic (PK) profile comprising one or more of the following PK parameters (dose-normalized to 10 mg) after administration of the composition to a human after at least a 10-hour fast: (a) a mean Cmax between about 30 and 40 ng/mL; (b) a mean AUCinfinity between about 300 and 430 h*ng/mL; (c) a mean AUClast between about 280 and 430 h*ng/mL; and (d) a median tmax between about 1 to 4 hours.
  • In other aspects, the disclosure provides solid pharmaceutical compositions comprising between about 2 mg and 20 mg aticaprant, wherein the composition has a dissolution profile comprising a Q value of between about 60% and 90% at 45 minutes, under the following dissolution operating conditions: Apparatus: Paddle (USP Type 2, Ph. Eur., JP); Dissolution medium: 0.01 M hydrochloric acid; Volume: 900 mL; Temperature: 37+/−0.5° C.; Rotation Speed: 50 rpm; and Analytical Finish: UHPLC with UV detection at 247 nm.
  • In further aspects, the disclosure provides methods of treating major depressive disorder (MDD) in a human patient comprising administering to the patient the pharmaceutical composition, oral tablet, or solid pharmaceutical composition described herein.
    • BRIEF DESCRIPTION OF THE DRAWINGS
  • FIG. 1 is the x-ray powder diffraction (XRPD) pattern of polymorph Form III of aticaprant (transmission mode).
  • FIG. 2 is the differential scanning calorimetry (DSC) thermogram of polymorph Form III of aticaprant.
  • FIG. 3 is the mDSC thermogram of polymorph Form III of aticaprant.
  • FIG. 4 is the trial design of Example 1.
  • FIG. 5 is a line graph showing the MADRS (Montgomery-Åsberg Depression Rating Scale) total score: least squares mean changes from baseline (±SE) during the treatment period for the enriched intent-to-treat (eITT) analysis set.
  • FIG. 6 is a plot showing MADRS total score changes at treatment week 6 for enriched and full population: MMRM results—estimated LS means and comparison versus placebo.
  • FIG. 7 is a line graph showing SHAPS (Snaith-Hamilton Pleasure Scale) total score: least squares mean changes from baseline (±SE) during the treatment period for the eITT analysis set.
  • FIG. 8 is a plot showing SHAPS total score changes at treatment week 6 for enriched and full population: MMRM (Mixed-effects Model for Repeated Measures) Results—estimated LSMeans and comparison versus placebo
  • FIG. 9 is a line graph showing MADRS total score: mean values (±SE) over time for the eITT analysis set.
  • FIG. 10 -A is a line graph showing MADRS total score: mean values (±SE) over time for the full intent-to-treat (fITT) analysis set. FIG. 10 -B is an excerpt from FIG. 10 -A for treatment weeks 0-6.
  • FIG. 11 is a line graph showing MADRS total score: percentage of subjects with remission of depressive symptoms (total score ≤10) during the treatment period for the eITT analysis set.
  • FIG. 12 is a line graph showing MADRS total score: percentage of subjects with remission of depressive symptoms (total score ≤10) during the treatment period for the fITT analysis set.
  • FIG. 13 is a line graph showing MADRS total score: percentage of responders (≥30% improvement from baseline) during the treatment period for the eITT analysis set.
  • FIG. 14 is a line graph showing MADRS total score: percentage of responders (≥30% improvement from baseline) during the treatment period for the fITT analysis set.
  • FIG. 15 is a line graph showing MADRS total score: percentage of responders (≥50% improvement from baseline) during the treatment period for the eITT analysis set.
  • FIG. 16 is a line graph showing MADRS total score: percentage of responders (≥50% improvement from baseline) during the treatment period for the fITT analysis set.
  • FIG. 17 is a line graph showing SHAPS total score: mean values (±SE) over time for the eITT analysis set.
  • FIG. 18 is a line graph showing SHAPS total score: mean values (±SE) over time for the fITT analysis set.
  • FIG. 19 illustrates the MADRS change from baseline by anhedonia severity.
  • FIG. 20 -A is a line graph showing MADRS change from baseline for patients with high anhedonia, i.e., SHAPS ≥38. FIG. 20 -B is a line graph showing MADRS change from baseline for patients with low anhedonia, i.e., SHAPS <38.
  • FIG. 21 is bar graph showing the comparison of MADRS in patients having low and high anhedonia.
  • FIG. 22 is a line graph showing the ASEX total score mean change from baseline.
  • FIG. 23 is a bar graph showing ASEX item level change total score mean change from baseline.
  • FIG. 24 is the flow chart for the process for preparing tablets containing aticaprant. In this figure, a refers to microfine, i.e., milled aticaprant.
  • FIG. 25 is the schematic overview of part 1 of the study. In this figure, Treatment A=2×5 mg capsule; Treatment B=1×10 mg tablet concept 1; Treatment C=1×5 mg tablet concept 1; Treatment D=1×10 mg tablet concept 1 with high-fat diet.
  • FIG. 26 is the schematic overview of part 2 of the study. In this figure, a) Day 1 of a treatment period is the first day of the washout period. Treatment E: 2×5 mg oral capsule administered in the morning, after at least 10-hour overnight fasting. Treatment F: 1×10 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting. Treatment G: 1×5 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting. Treatment H: 1×10 mg Formulation Concept 2 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
  • FIGS. 27 and 28 show the relative bioavailability results for aticaprant PK profiles relative to BA.
  • FIGS. 29 and 30 show the relative bioavailability results for aticaprant PK profile, dose-proportionality.
  • FIGS. 31-33 show the relative bioavailability results for aticaprant PK profile, food effect.
  • FIG. 34 is the study scheme for Example 7. All patients will continue their oral antidepressant SSRI/SNRI during the entire study. Approximately an additional 34 elderly participants will be randomized.
  • FIG. 35 is the study scheme for Example 8. All patients will continue their oral antidepressant SSRI/SNRI during the entire study. Approximately an additional 68 elderly participants will be randomized.
  • FIG. 36 is a bar graph showing the SHAPS items: LS means for change from baseline at week 6 by baseline SHAPS total score for the fITT analysis set. In this figure and going from top to bottom, the bars alternatively refer to placebo or aticaprant. For example, the first bar refers to aticaprant, the second bar refers to placebo, the third bar refers to aticaprant, etc.
  • FIG. 37 is a plot showing MADRS total score: difference of LSMeans (60% at Weeks 6 by different subgroups for the fITT analysis set. In this plot, <17 indicates mild severity; 18-24 indicates mild to moderate severity, and 25-30 indicates moderate to severe.
    •  DETAILED DESCRIPTION OF ILLUSTRATIVE EMBODIMENTS
  • All individual features (e.g., particular embodiments or specific preferred features) mentioned herein may be taken in isolation or in combination with any other feature (including particular embodiment or preferred feature) mentioned herein; hence, preferred features may be taken in conjunction with other preferred features, or independently of them (and likewise with particular embodiments).
  • The disclosure provides compositions comprising pure crystalline Form of III aticaprant that are anhydrous and stable in the solid form.
  • The term “crystalline” refers to a solid form of a chemical moiety that contains a highly ordered intermolecular structure.
  • The term “polymorph” refers to a crystalline form of a molecule having one specific crystal structure. A crystalline compound may have one crystal form or may have two or more crystal forms, i.e., polymorphs. As is understood to those skilled in the art, polymorphs of a chemical compound may distinguished from each other by compared physicochemical properties such as solubility, dissolution rate, stability, bioavailability, among others. Polymorphs also may have different spectra selected from, without limitation, x-ray powder diffraction (XRPD), single crystal x-ray diffraction, thermogravimetric analysis (TGA), infrared spectroscopy, Raman spectroscopy, solid state nuclear magnetic resonance (NMR), differential scanning calorimetry (DSC), polarized light microscopy (PLM), hot stage microscopy, or dynamic solvent sorption.
  • The term “crystalline” refers to solid state form of a chemical moiety wherein the atoms, molecules, or ions are assembled in a highly ordered structure that extends in all directions. Thus, “crystalline” includes all crystalline forms of Compound I, including salts thereof. Characterization of crystalline forms may be performed by those skilled in the art including, without limitation, XRPD or DSC. Typically, the XRPD pattern contains sharp intensity peaks. This contrasts to the XRPD pattern of an amorphous form that often contains a broad, peak, without no identifying peaks. A crystalline form may be completely crystalline or partially crystalline. In some aspects, a crystalline sample may be 100% w/w crystalline. A crystalline sample may also contain solids that are amorphous. In certain aspects, a crystalline form may contain solids such that the sample is at least about 99% w/w crystalline, at least about 95% w/w amorphous, at least about 90% w/w crystalline, at least about 85% w/w crystalline, at least about 80% w/w crystalline, or the like.
  • The term “anhydrous” or “anhydrate” as used herein refers to a crystalline as described herein that substantially lacks water. In some aspects, an anhydrous form contains less than about 1% w/w of water. In other aspects, an anhydrous form contains less than about 0.9%, about 0.8%, about 0.7%, about 0.6%, about 0.5%, about 0.4%, about 0.3%, about 0.2%, about 0.1% w/w of water.
  • As provided herein, all temperature values may vary. Such variations may depend on instrument type, instrument parameters, laboratory techniques, and/or laboratory conditions. Unless otherwise defined, a recited temperature may vary. In some aspects, the temperatures noted herein vary by about 0.1°, about 0.5°, about 1°, about 2°, about 3°, about 4°, or about 5°.
  • Similarly, 2θ values obtained from the XRPD patterns also may vary. Such variations may depend on instrument type, instrument parameters, laboratory techniques, sample (including particle size, impurities, etc.), and/or laboratory conditions. Unless otherwise defined, the XRPD patterns and/or the 2θ peak values may vary. In certain aspects, the 2θ peak values vary (higher or lower) by about 0.05°, about 0.1°, about 0.15°, or about 0.2°. In other aspects, one or more of the 2θ peak values are higher by about 0.05°, about 0.1°, about 0.15°, or about 0.2°. In further aspects, one or more of the 2θ peak values are lower by about 0.05°, about 0.1°, about 0.15°, or about 0.2°.
  • As used herein, the term “corresponds to” may be used in reference to certain spectra. Thus, “corresponds to” includes a spectrum that is identical or substantially similar to another spectrum. One skilled in the art would be able to compare such spectra and determine if a spectrum corresponds to another. Thus, the term “corresponds to” is used herein to compare XRPD patterns, DSC thermograms, among others. In some aspects, one XRPD pattern corresponds to another XRPD pattern when their 2θ values are within the margin of error as described above. In other aspects, one XRPD pattern corresponds to another XRPD pattern when the peaks have the same 2θ peak value, but one or more peaks have a different height (intensity). In further aspects, one XRPD pattern corresponds to another XRPD pattern when the peaks have the same 2θ peak value, but one or more peaks have a different peak area. In yet other aspects, one XRPD pattern corresponds to another XRPD pattern when the peaks have the same 2θ peak value, but one or more peak is obscured. Such obscured peaks may be due to impurities, excipients, or the like. Such obscured peaks typically do not prevent characterization of the crystalline form.
  • As used herein, unless otherwise noted, the term “aticaprant” refers to 3-fluoro-4-4-2-(3,5-dimethylphenyl)pyrrolidin-1-yl-methylphenoxybenzamide, i.e., the following compound:
  • Figure US20230277500A1-20230907-C00001
  • and is also known as JNJ-67953964, 67953964-AAA, CERC-501, and LY-2456302. In some embodiments, “aticaprant” refers to the (S)-enantiomer of aticaprant, i.e., the following compound:
  • Figure US20230277500A1-20230907-C00002
  • also known as (S)-aticaprant or (S)-3-fluoro-4-4-2-(3,5-dimethylphenyl)pyrrolidin-1-yl-methylphenoxybenzamide. In other embodiments, the aticaprant used in the methods described herein is substantially free of the (R)-enantiomer, i.e., (R)-aticaprant or (R)-3-fluoro-4-4-2-(3,5-dimethylphenyl)pyrrolidin-1-yl-methylphenoxybenzamide having the following structure:
  • Figure US20230277500A1-20230907-C00003
  • In other embodiments, the aticaprant contains less than about 10% by weight, based on the weight of aticaprant, of the (R)-enantiomer of aticaprant. In further embodiments, aticaprant contains less than about 10, about 9, about 8, about 7, about 6, about 5, about 4, about 3, about 2, about 1, about 0.5, about 0.1, about 0.005, or about 0.001% by weight, based on the weight of aticaprant, of the (R)-enantiomer of aticaprant. In yet other embodiments, the aticaprant contains about 0.001 to about 10% by weight, based on the weight of aticaprant, of the (R)-enantiomer of aticaprant. In still further embodiments, the aticaprant contains about 0.001 to about 10%, about 0.001 to about 5%, about 0.001 to about 1%, about 0.001 to about 0.5%, about 0.001 to about 0.1%, about 0.1 to about 5%, about 0.1 to about 1%, about 0.1 to about 5%, or about 0.5 to about 5% by weight, based on the weight of aticaprant.
  • Pharmaceutically acceptable salts of aticaprant are also contemplated by the present invention, which may be readily selected by those skilled in the art. A “pharmaceutically acceptable salt” refers a salt of aticaprant that is non-toxic, biologically tolerable, or otherwise biologically suitable for administration to the subject. See, generally, G. S. Paulekuhn, “Trends in Active Pharmaceutical Ingredient Salt Selection based on Analysis of the Orange Book Database”, J. Med. Chem., 2007, 50:6665-72, S. M. Berge, “Pharmaceutical Salts”, J. Pharm. Sci., 1977, 66:1-19, and Handbook of Pharmaceutical Salts, Properties, Selection, and Use, Stahl and Wermuth, Eds., Wiley-VCH and VHCA, Zurich, 2002. Examples of pharmaceutically acceptable salts are those that are pharmacologically effective and suitable for administration to patients without undue toxicity, irritation, or allergic response.
  • Examples of pharmaceutically acceptable salts include sulfates, pyrosulfates, bisulfates, sulfites, bisulfites, phosphates, monohydrogen-phosphates, dihydrogenphosphates, metaphosphates, pyrophosphates, bromides (such as hydrobromides), iodides (such as hydroiodides), acetates, propionates, decanoates, caprylates, acrylates, formates, isobutyrates, caproates, heptanoates, propiolates, oxalates, malonates, succinates, suberates, sebacates, fumarates, maleates, butyne-1,4-dioates, hexyne-1,6-dioates, benzoates, chlorobenzoates, methylbenzoates, dinitrobenzoates, hydroxybenzoates, methoxybenzoates, phthalates, sulfonates, xylenesulfonates, phenylacetates, phenylpropionates, phenylbutyrates, citrates, lactates, γ-hydroxybutyrates, glycolates, tartrates, methane-sulfonates, propanesulfonates, naphthalene-1-sulfonates, naphthalene-2-sulfonates, and mandelates.
  • In some embodiments, the aticaprant is crystalline Form III of aticaprant. Crystalline Form III of aticaprant may be characterized by a number of techniques including, without limitation, x-ray diffraction and differential scanning calorimetry. In some embodiments, crystalline Form III of aticaprant is characterized by x-ray diffraction. In other embodiments, crystalline Form III of aticaprant is characterized by four or more x-ray diffraction pattern peaks at 2θ (±0.2) of 4.1°, 9.0°, 17.6°, 18.0°, or 21.4°. In further embodiments, crystalline Form III of aticaprant is characterized by four or more x-ray diffraction pattern peaks at 2θ (±0.2) of 4.1°, 9.0°, 17.6°, 18.0°, or 21.4° and one or more additional peaks at 16.4°, 20.1°, 20.3°, 24.1°, and 25.7°. In yet other embodiments, crystalline Form III of aticaprant is characterized by four or more x-ray diffraction pattern peaks at 2θ (±0.2) of 4.1°, 9.0°, 17.6°, 18.0°, or 21.4° and one or more additional peaks at 15.1°, 16.4°, 20.0°, 20.1°, 20.3°, 24.1°, 25.0°, 25.7°, 26.2°, and 28.8°. In still further embodiments, crystalline Form III of aticaprant is characterized by four or more x-ray diffraction pattern peaks at 2θ (±0.2) of 4.1°, 9.0°, 17.6°, 18.0°, or 21.4° and one or more additional peaks at 8.2°, 9.7°, 12.0°, 13.5°, 15.1°, 16.4°, 19.4°, 28.4°, 20.0°, 20.1°, 20.3°, 24.1°, 25.0°, 25.7°, 26.2°, 28.8°, and 30.0°. In other embodiments, crystalline Form III of aticaprant is characterized by four or more x-ray diffraction pattern peaks at 2θ (±0.2) of 3.1°, 19.0°, 24.0°, 24.3°, or 26.2 and one or more additional peaks of Table 1.
  • TABLE 1
    Position (2θ)
    4.1
    8.2
    9.0
    9.7
    10.7
    12.0
    12.3
    13.5
    15.1
    16.4
    16.8
    17.6
    18.0
    18.6
    19.4
    19.7
    20.1
    20.3
    20.6
    21.4
    22.2
    24.1
    24.4
    25.0
    25.2
    25.7
    26.23
    26.4
    27.1
    28.4
    28.6
    28.8
    20.0
    30.2
    30.5
    31.2
    31.8
    32.2
    32.5
    33.0
    33.2
    33.6
    33.9
    34.4
    35.4
    36.0
    36.4
    37.0
    38.2
    38.5
    39.5
  • In still other embodiments, crystalline Form III of aticaprant is characterized the x-ray diffraction pattern peaks in Table 2.
  • TABLE 2
    Position (2θ)
    4.1
    8.2
    9.0
    9.7
    12.0
    13.5
    15.1
    16.4
    17.6
    18.0
    19.4
    19.7
    20.1
    20.3
    21.4
    24.1
    25.0
    25.7
    26.3
    28.4
    28.8
    30.0
  • In still other embodiments, crystalline Form III of aticaprant is characterized the x-ray diffraction pattern peaks in Table 3.
  • TABLE 3
    Position (2θ)
    4.1
    8.2
    9.0
    9.7
    10.7
    12.0
    12.3
    13.5
    15.1
    16.4
    16.8
    17.6
    18.0
    18.6
    19.4
    19.7
    20.1
    20.3
    20.6
    21.4
    22.2
    24.1
    24.4
    25.0
    25.2
    25.7
    26.3
    26.4
    27.1
    28.4
    28.6
    28.8
    30.0
    30.2
    30.5
    31.2
    31.8
    32.2
    32.5
    33.0
    33.2
    33.6
    33.9
    34.4
    35.4
    36.0
    36.4
    37.0
    38.2
    38.5
    39.5

    In further embodiments, crystalline Form III of aticaprant is characterized by an x-ray powder diffraction pattern that corresponds to FIG. 1 .
  • Crystalline Form III of aticaprant may also be characterized by differential scanning calorimetry. In some embodiments, the differential scanning calorimetry thermogram comprises a peak temperature (Tm) at about 121° C. In other embodiments, crystalline Form III of aticaprant is characterized by a differential scanning calorimetry thermogram that corresponds to FIG. 2 .
    • Pharmaceutical Compositions
  • The disclosure also contemplates pharmaceutical composition comprising aticaprant and one or more pharmaceutically acceptable excipient. As used herein, the term “composition” is intended to encompass a product comprising the specified ingredients in the specified amounts, as well as any product which results, directly or indirectly, from combinations of the specified ingredients in the specified amounts. The preferred pharmaceutical composition contains crystalline Form III of aticaprant as the active ingredient intimately admixed with a pharmaceutical carrier according to conventional pharmaceutical compounding techniques, which carrier may take a wide variety of forms depending on the form of preparation desired for administration. Suitable pharmaceutically acceptable carriers are well known in the art. Descriptions of some of these pharmaceutically acceptable carriers may be found in The Handbook of Pharmaceutical Excipients, published by the American Pharmaceutical Association and the Pharmaceutical Society of Great Britain.
  • The amount of aticaprant present in the compositions is about 2 mg to about 60 mg. In some embodiments, the composition contains about 2 mg to about 20 mg of aticaprant. In some embodiments, the composition contains about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 11, about 12, about 13, about 14, about 15, about 16, about 17, about 18, about 19, or about 20 mg of aticaprant. In other embodiments, the composition contains about 5 to about 20 mg, about 10 to about 20 mg, about 15 to about 20 mg, about 1 to about 15 mg, about 2 to about 15 mg, about 5 to about 15 mg, about 10 to about 15 mg, about 1 to about 10 mg, about 2 to about 10 mg, or about 5 to about 10 mg of aticaprant. In yet other embodiments, the effective amount of aticaprant is about 5 to about 15 mg. In further embodiments, the amount of aticaprant is about 5 or 10 mg. In other embodiments, the amount of aticaprant is about 5 mg. In still further embodiments, the amount of aticaprant is about 10 mg. The composition contains about 0.1% to about 90% by weight of aticaprant. In some embodiments, the composition contains about 0.1, about 0.5, about 1, 5, about 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, about 50, about 55, about 60, about 65, about 70, about 75, about 80, about 85, about 90% by weight, based on the weight of the composition, of aticaprant. In other embodiments, the composition contains about 0.1 to about 80, about 0.1 to about 70, about 0.1 to about 60, about 0.1 to about 50, about 0.1 to about 40, about 0.1 to about 30, about 0.1 to about 20, about 0.1 to about 10, about 0.1 to about 5, about 0.1 to about 1, about 0.1 to about 0.5, about 1 to about 90, about 1 to about 80, about 1 to about 70, about 1 to about 60, about 1 to about 50, about 1 to about 40, about 1 to about 30, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 5 to about 90, about 5 to about 80, about 5 to about 70, about 5 to about 60, about 5 to about 50, about 5 to about 40, about 5 to about 30, about 5 to about 20, about 5 to about 10, about 10 to about 90, about 10 to about 80, about 10 to about 70, about 10 to about 60, about 10 to about 60, about 10 to about 50, about 10 to about 40, about 10 to about 30, about 10 to about 20, about 20 to about 90, about 20 to about 80, about 20 to about 70, about 20 to about 60, about 20 to about 50, about 20 to about 40, about 20 to about 30, about 30 to about 90, about 30 to about 80, about 30 to about 70, about 30 to about 60, about 30 to about 50, about 30 to about 40, about 40 to about 90, about 40 to about 80, about 40 to about 70, about 40 to about 60, about 40 to about 50, about 50 to about 90, about 50 to about 80, about 50 to about 70, about 50 to about 60, about 60 to about 90, about 60 to about 80, about 60 to about 70, about 70 to about 90, about 70 to about 80, or about 80 to about 90% by weight, based on the weight of the composition, of aticaprant. In further embodiments, the composition contains about 5% by weight of aticaprant. In yet other embodiments, the composition contains about 6% by weight of aticaprant. In still further embodiments, the composition contains about 7% by weight of aticaprant. In other embodiments, the composition contains about 8% by weight of aticaprant. In further embodiments, the composition contains about 9% by weight of aticaprant. In still other embodiments, the composition contains about 10% by weight of aticaprant. The amount of aticaprant for administration according to the methods described herein may be determined by one skill in the art and, unless otherwise noted, are set forth on an aticaprant free base basis. That is, the amounts indicate that amount of the aticaprant molecule administered, exclusive of, for example, solvent (such as in solvates) or counterions (such as in pharmaceutically acceptable salts).
  • In some embodiments, the pharmaceutical compositions have a particular pharmacokinetic (PK) profile at a specific dose. In some embodiments, the pharmaceutical compositions have a PK profile that is dose-proportional. In other embodiments, the pharmaceutical compositions have a PK profile comprising parameters, e.g., exposure parameters such as Cmax or AUC, that are dose-proportional. In further embodiments, the pharmaceutical compositions have a PK profile or PK parameter that is dose-proportional between about 1 mg to 60 mg aticaprant, between about 2 mg to 60 mg aticaprant, between about 2 mg to 40 mg aticaprant, between about 2 mg to 20 mg aticaprant, between about 2 mg to 15 mg aticaprant, between about 2 mg to 10 mg aticaprant, and between about 5 mg to 10 mg aticaprant.
  • Some embodiments include pharmaceutical compositions comprising aticaprant that are bioequivalent to any one of the pharmaceutical compositions described herein. In some embodiments, the pharmaceutical composition comprises between about 2 mg and about 60 mg, between about 2 mg and about 20 mg aticaprant, between about 5 mg and about 10 mg aticaprant, or about 5 mg or about 10 mg aticaprant, wherein the composition is bioequivalent to a pharmaceutical composition comprising aticaprant which when administered to a human after at least a 10-hour fast yields a PK profile that includes one or more of: a mean Cmax of between about 30 and 35 ng/mL, a mean AUCinfinity of between about 300 and 320 ng/mL, and a median tmax of about 1.5 hour (dose-normalized to 10 mg). Bioequivalence may be demonstrated by any method known to one skilled in the art, for example, as described in Example 9 herein, or as described in Chow, Bioavailability and Bioequivalence in Drug Development, Wiley interdisciplinary reviews, Computational statistics, 6, 4 (2014): 304-312. doi:10.1002/wics.1310.
  • In some embodiments, the pharmaceutical composition comprises between about 2 mg and about 20 mg aticaprant, about 5 mg aticaprant, or about 10 mg aticaprant, wherein when the pharmaceutical composition is compared to a reference composition, the 90% confidence interval of the ratio of geometric means of one or more PK parameters of the pharmaceutical composition and reference composition is within the bioequivalence limits of 80% and 125%. In some embodiments, the reference composition is a composition comprising aticaprant which when administered to a human after at least a 10-hour fast yields a PK profile that includes one or more of: a mean Cmax of between about 30 and 35 ng/mL, a mean AUCinfinity of between about 300 and 320 ng/mL, and a median tmax of about 1.5 hour (dose-normalized to 10 mg). In some other embodiments, the reference composition has a PK profile of any one of Treatment A, Treatment B, Treatment C, or Treatment D described in Table 69.
  • In some embodiments, the PK profile is based on administration of the composition, containing about 2 mg to about 60 mg aticaprant, to a human after at least a 10-hour fast. In some other embodiments, the PK profile is based on administration of the composition, containing about 2 mg to about 60 mg aticaprant, to a human about 30 minutes after the start of a high-fat meal following at least a 10-hour fast. As another example, the PK profile is based on administration of the composition, containing about 2 mg to about 20 mg aticaprant, to a human after at least a 10-hour fast. In some embodiments, the PK profile is based on administration of a composition containing about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 11, about 12, about 13, about 14, about 15, about 16, about 17, about 18, about 19, or about 20 mg of aticaprant to a human. In further embodiments the PK profile is based on administration of a composition containing about 2 to about 19, about 2 to about 18, about 2 to about 16, about 2 to about 14, about 2 to about 12, about 2 to about 10, about 2 to about 8, about 2 to about 6, about 2 to about 4, about 4 to about 20, about 4 to about 18, about 4 to about 16, about 4 to about 14, about 4 to about 12, about 4 to about 10, about 4 to about 8, about 4 to about 6, about 6 to about 20, about 6 to about 18, about 6 to about 16, about 6 to about 14, about 6 to about 12, about 6 to about 10, about 6 to about 8, about 8 to about 20, about 8 to about 18, about 8 to about 16, about 8 to about 14, about 8 to about 12, about 8 to about 10, about 10 to about 20, about 10 to about 18, about 10 to about 16, about 10 to about 14, about 10 to about 12, about 12 to about 20, about 12 to about 18, about 12 to about 16, about 12 to about 14, about 14 to about 20, about 14 to about 18, about 14 to about 16, about 16 to about 20, about 16 to about 18, or about 18 to about 20 mg of aticaprant to a human.
  • In certain aspects, the PK profile is determined after an at least 10-hour food fast. In some embodiments, the food fast is at least about 1, about 2, about 4, about 5, about 10, about 12, about 15, about 18, about 20, about 22, 24, about 28, or about 32 hours.
  • For example, the PK profile may include a Cmax ranging between about 1 and about 100, about 5 and about 70, about 5 and about 65, about 5 and about 60, about 5 and about 55, about 5 and about 50, about 5 and about 45, about 10 and about 70, about 10 and about 65, about 10 and about 60, about 10 and about 55, about 10 and about 50, about 10 and about 45, about 13 and about 60, about 13 and about 55, about 13 and about 50, about 20 and about 70, about 20 and about 65, or about 20 and about 63 ng/mL (dose-normalized to 10 mg). In some embodiments, the PK profile includes a Cmax ranging between about 20 and about 45, about 22 and about 45, about 23 and about 45, or about 24 and about 44 ng/mL (dose-normalized to 10 mg) when administered after at least a 10-hour fast. In some embodiments, the PK profile includes a Cmax ranging between about 25 and about 50, about 27 and about 38, about 25 and about 40, or about 28 and about 38 ng/mL (dose-normalized to 10 mg) when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • In some embodiments, the PK profile includes an AUCinfinity ranging between about 50 and about 800, about 100 and about 500, about 100 and about 480, about 100 and about 450, about 100 and about 400, about 110 and about 500, about 110 and about 480, about 110 and about 450, about 110 and about 400, about 150 and about 700, about 200 and about 700, about 200 and about 650, about 250 and about 450, about 280 and about 420, about 290 and about 410, or about 210 and about 650 h*ng/mL (dose-normalized to 10 mg). In some embodiments, the PK profile includes an AUCinfinity ranging between about 200 and about 400, about 210 and about 400, about 210 and about 398, about 220 and about 400, or about 220 and about 398 h*ng/mL (dose-normalized to 10 mg) when administered after at least a 10-hour fast. In some embodiments, the PK profile includes an AUCinfinity ranging between about 300 and about 600, about 300 and 550, or about 320 and about 530 h*ng/mL (dose-normalized to 10 mg) when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • In some embodiments, the PK profile includes an AUClast ranging between about 50 and about 800, about 100 and about 500, about 100 and about 480, about 100 and about 450, about 100 and about 400, about 110 and about 500, about 110 and about 480, about 110 and about 450, about 110 and about 400, about 150 and about 700, about 200 and about 700, about 200 and about 650, about 250 and about 450, about 280 and about 420, about 290 and about 410, or about 210 and about 650 h*ng/mL (dose-normalized to 10 mg). In some embodiments, the PK profile includes an AUClast ranging between about 300 and about 400 (dose-normalized to 10 mg).
  • In some embodiments, the PK profile incudes a tmax ranging between about 0.5 and about 5, between about 1 and about 4.5, about 1 and about 4, about 1 and about 3, about 1 and about 2.5, or about 1 and about 2 hours. In some embodiments, the PK profile includes a tmax that ranges between about 1 and about 2.5, about 1 and about 2, or about 1 and about 3 hours when administered after at least a 10-hour fast. In some embodiments, the PK profile includes a tmax that ranges between about 1 and about 4 hours when administered after about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • In some embodiments, the PK profile incudes a t1/2 ranging between about 5 and about 60, about 5 and about 55, about 5 and about 50, about 5 and about 45, about 5 and about 40, about 9 and about 60, about 9 and about 55, about 9 and about 50, about 9 and about 45, or about 9 and about 40 hours.
  • In some embodiments, the PK profile includes a λz ranging between about 0.010 and about 0.080, about 0.010 and about 0.075, about 0.010 and about 0.070, about 0.015 and about 0.080, about 0.015 and about 0.075, about 0.015 and about 0.070, about 0.015 and about 0.065, about 0.015 and about 0.060, about 0.015 and about 0.055, or about 0.015 and about 0.050 l/hour.
  • In some other embodiments, the PK profile includes a CL/F ranging between about 10 and about 90, about 10 and about 85, about 10 and about 80, about 10 and about 75, about 10 and about 70, about 10 and about 60, about 10 and about 50, about 15 and about 90, about 15 and about 80, about 15 and about 70, about 15 and about 60, about 15 and about 50, about 20 and about 90, about 20 and about 80, about 20 and about 75, about 20 and about 70, about 20 and about 60, or about 20 and about 50 L/h.
  • In some other embodiments, the PK profile includes a Vd/F ranging between about 400 and about 6000, about 400 and about 5500, about 400 and about 5000, about 400 and about 4000, about 400 and about 3500, about 400 and about 3400, about 450 and about 3500, about 450 and about 3000, about 500 and about 3500, about 500 and about 3000, about 400 and about 2000, about 400 and about 1500, about 400 and about 1200, about 550 and about 3500, about 550 and about 3000, about 600 and about 3500, about 600 and about 3000, about 600 and about 2500, or about 450 and about 1200 L.
  • For example, the PK profile may include a mean Cmax between about 20 and 45 ng/mL when dose-normalized to 10 mg. In some embodiments, the mean Cmax is about 20, about 21, about 22, about 23, about 24, about 25, about 26, about 27, about 28, about 29, about 30, about 31, about 32, about 33, about 34, about 35, about 36, about 37, about 38, about 39, about 40, about 41, about 42, about 43, about 44, or about 55 ng/mL (dose-normalized to 10 mg). In other embodiments, the mean Cmax is about 20 to about 40, about 20 to about 35, about 20 to about 30, about 20 to about 25, about 25 to about 45, about 25 to about 40, about 25 to about 35, about 25 to about 30, about 30 to about 45, about 30 to about 40, about 30 to about 35, about 35 to about 45, about 35 to about 40, or about 40 to about 45 ng/mL (dose-normalized to 10 mg). In further embodiments, the mean Cmax is between about 30 and 35 ng/mL, about 31 and 35 ng/mL, or about 31 and 34 ng/mL (dose-normalized to 10 mg) when administered after at least a 10-hour fast. In further embodiments, the mean Cmax is between about 35 and 40, about 36 and 39, or about 37 and 38 ng/mL (dose-normalized to 10 mg) when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • The PK profile also may have a mean AUCinfinity between about 250 and 450 h*ng/mL (dose-normalized to 10 mg). In some embodiments, the AUCinfinity is about 250, about 260, about 270, about 280, about 290, about 300, about 310, about 320, about 330, about 340, about 350, about 360, about 370, about 380, about 390, about 400, about 410, about 420, about 430, about 440, or about 450 h*ng/mL (dose-normalized to 10 mg). In other embodiments, the mean AUCinfinity is about 250 to about 400, about 250 to about 375, about 250 to about 350, about 250 to about 325, about 250 to about 300, about 250 to about 275, about 275 to about 450, about 275 to about 425, about 275 to about 400, about 275 to about 375, about 275 to about 350, about 275 to about 325, about 275 to about 300, about 300 to about 450, about 300 to about 425, about 300 to about 400, about 300 to about 390, about 300 to about 380, about 300 to about 370, about 300 to about 360, about 300 to about 350, about 300 to about 340, about 300 to about 330, about 300 to about 320, about 300 to about 310, about 325 to about 450, about 325 to about 425, about 325 to about 400, about 325 to about 375, about 325 to about 350, about 350 to about 450, about 350 to about 425, about 350 to about 400, about 350 to about 375, about 375 to about 450, about 375 to about 425 to about 375 to about 400, about 400 to about 450, about 400 to about 425, or about 425 to about 450 h*ng/mL (dose-normalized to 10 mg). In further embodiments, the mean AUCinfinity is between about 300 and 320 h*ng/mL (dose-normalized to 10 mg) when administered after at least a 10-hour fast. In further embodiments, the mean AUCinfinity is between about 320 and 530 h*ng/mL (dose-normalized to 10 mg) when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • In other aspects, the pharmaceutical composition has a PK profile comprising a mean AUClast between about 250 and 450 h*ng/mL (dose-normalized to 10 mg). In some embodiments, the AUClast is about 250, about 260, about 270, about 280, about 290, about 300, about 310, about 320, about 330, about 340, about 350, about 360, about 370, about 380, about 390, about 400, about 410, about 420, about 430, about 440, or about 450 h*ng/mL. In other embodiments, the mean AUClast is about 250 to about 400, about 250 to about 375, about 250 to about 350, about 250 to about 325, about 250 to about 300, about 250 to about 275, about 275 to about 450, about 275 to about 425, about 275 to about 400, about 275 to about 375, about 275 to about 350, about 275 to about 325, about 275 to about 300, about 300 to about 450, about 300 to about 425, about 300 to about 400, about 300 to about 390, about 300 to about 380, about 300 to about 370, about 300 to about 360, about 300 to about 350, about 300 to about 340, about 300 to about 330, about 300 to about 320, about 300 to about 310, about 325 to about 450, about 325 to about 425, about 325 to about 400, about 325 to about 375, about 325 to about 350, about 350 to about 450, about 350 to about 425, about 350 to about 400, about 350 to about 375, about 375 to about 450, about 375 to about 425 to about 375 to about 400, about 400 to about 450, about 400 to about 425, or about 425 to about 450 h*ng/mL (dose-normalized to 10 mg). In further embodiments, the PK profile has a mean AUClast of between about 280 and 310 h*ng/mL (dose-normalized to 10 mg).
  • In still further aspects, the pharmaceutical composition has a PK profile comprising a median tmax between about 1 to 4 hours. In some embodiments, the median tmax is about 1, about 1.1, about 1.2, about 1.3, about 1.4, about 1.5, about 1.6, about 1.7, about 1.8, about 1.9, about 2, about 2.1, about 2.2, about 2.3, about 2.4, about 2.5, about 2.6, about 2.7, about 2.8, about 2.9, about 3, about 3.1, about 3.2, about 3.3, about 3.4, about 3.5, about 3.6, about 3.7, about 3.8, about 3.9, or about 4 hours. In other embodiments, the median tmax is about 1 to about 3.5, about 1 to about 3, about 1 to about 2.5, about 1 to about 2, about 1 to about 1.5, about 1.5 to about 4, about 1.5 to about 3.5, about 1.5 to about 3, about 1.5 to about 2.5, about 1.5 to about 2, about 2 to about 4, about 2 to about 3.5, about 2 to about 3, about 2 to about 2.5, about 2.5 to about 4, about 2.5 to about 3.5, about 2.5 to about 3, about 3 to about 4, about 3 to about 3.5, or about 3.5 to about 4 hours. In further embodiments, the median tmax is about 1.5 hours.
  • In some embodiments, the pharmaceutical composition comprises a PK profile of Treatment A, Treatment B, Treatment C, or Treatment D, as shown in Table 69.
  • In some embodiments, the pharmaceutical composition has a PK profile including a mean Cmax of about 30, about 31, about 32, about 33, about 34, or about 35 ng/mL when administered after at least a 10-hour fast (dose-normalized to 10 mg). In some embodiments, the pharmaceutical composition comprises has a PK profile including a mean Cmax of about 31.2 ng/mL with standard deviation of about 6.9 ng/mL (dose-normalized to 10 mg). In some embodiments, the pharmaceutical composition comprises about 10 mg aticaprant and has a PK profile including a mean Cmax of about 34.1 ng/mL with standard deviation of about 10.0 ng/mL when administered after at least a 10-hour fast. In some embodiments, the pharmaceutical composition comprises about 5 mg aticaprant and has a PK profile including a mean Cmax of about 17.0 ng/mL with standard deviation of about 4.48 ng/mL when administered after at least a 10-hour fast.
  • In some embodiments, the pharmaceutical composition has a PK profile including a mean Cmax of about 36, about 37, about 38, about 39, or about 35 ng/mL when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast (dose-normalized to 10 mg). In some embodiments, the pharmaceutical composition comprises about 10 mg aticaprant and has a PK profile including a mean Cmax of about 37.7 ng/mL with a standard deviation of about 9.18 ng/mL when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • In some embodiments, the pharmaceutical composition has a PK profile comprising a mean AUCinfinity of about 300, about 305, about 310, about 315, or about 320 h*ng/mL when administered after a least a 10-hour fast (dose-normalized to 10 mg).
  • In some embodiments, the pharmaceutical composition has a PK profile comprising a mean AUCinfinity of about 400, about 420, about 425, about 430, about 440, or about 450 h*ng/mL when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast (dose-normalized to 10 mg).
  • In some embodiments, the pharmaceutical composition has a PK profile comprising a median tmax of about 1.0, about 1.1, about 1.2, about 1.3, about 1.4, about 1.5, about 1.6, about 1.7, about 1.8, about 1.9, or about 2.0 hours when administered after at least a 10-hour fast. In some embodiments, the pharmaceutical composition has a PK profile comprising a median tmax of about 1.5 hours when administered after at least a 10-hour fast.
  • In some embodiments, the pharmaceutical composition has a PK profile comprising a median t of about 2.5, about 2.6, about 2.7, about 2.8, about 2.9 or about 3.0 hour when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast. In some embodiments, the pharmaceutical composition has a PK profile comprising a median tmax of about 2.75 hours when administered about 30 minutes after the start of a high-fat meal following at least a 10-hour fast.
  • As noted, the compositions contain a pharmaceutically acceptable excipient, one of which may be a filler. In some embodiments, the filler is the filler is microcrystalline cellulose, lactose monohydrate, or silicified microcrystalline cellulose, or a combination thereof. In other embodiments, the filler is microcrystalline cellulose. In further embodiments, the filler is lactose monohydrate. In yet other embodiments, the filler is silicified microcrystalline cellulose. The composition comprises between about 10% to about 99.9% filler by weight, based on the weight of the composition. In some embodiments, the composition contains about 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, about 50, about 55, about 60, about 65, about 70, about 75, about 80, about 81, about 82, about 83, about 84, about 85, about 86, about 87, about 88, about 89, about 90, about 91, about 92, about 93, about 94, about 95, about 96, about 97, about 98, about 99, or about 99.9% by weight, based on the weight of the composition, of a filler In other embodiments, the composition comprises about 10 to about 90, about 10 to about 80, about 10 to about 70, about 10 to about 60, about 10 to about 50, about 10 to about 40, about 10 to about 30, about 10 to about 20, about 20 to about 99.9, about 20 to about 90, about 20 to about 80, about 20 to about 70, about 20 to about 60, about 20 to about 50, about 20 to about 40, about 20 to about 30, about 30 to about 99.9, about 30 to about 90, about 30 to about 80, about 30 to about 70, about 30 to about 60, about 30 to about 50, about 30 to about 40, about 40 to about 99.9, about 40 to about 90, about 40 to about 80, about 40 to about 70, about 40 to about 60, about 40 to about 50, about 50 to about 99.9, about 50 to about 90, about 50 to about 80, about 50 to about 70, about 50 to about 60, about 60 to about 99.9, about 60 to about 90, about 60 to about 80, about 60 to about 70, about 70 to about 99.9, about 70 to about 90, about 70 to about 80, about 80 to about 99.9, about 80 to about 90, or about 90 to about 99.9% by weight, based on the weight of the composition, of a filler. In further embodiments, the composition comprises about 90% by weight, based on the weight of the composition, of the filler. In other embodiments, the composition comprises about 88.5% by weight, based on the weight of the composition, of the filler.
  • The aticaprant to filler ratio is between about 0.005 and about 9 by weight. In some embodiments, the aticaprant to filler ratio is about 0.008 and 0.8 about by weight. In other embodiments, the aticaprant to filler ratio is about 0.005 to about 8, about 0.005 to about 7, about 0.005 to about 6, about 0.005 to about 5, about 0.005 to about 4, about 0.005 to about 3, about 0.005 to about 2, about 0.005 to about 1, about 0.005 to about 0.5, about 0.005 to about 0.1, about 0.005 to about 0.05, about 0.005 to about 0.01, about 0.01 to about 9, about 0.01 to about 8, about 0.01 to about 7, about 0.01 to about 6, about 0.01 to about 5, about 0.01 to about 4, about 0.01 to about 3, about 0.01 to about 2, about 0.01 to about 1, about 0.01 to about 0.5, about 0.01 to about 0.1, about 0.01 to about 0.05, about 0.05 to about 9, about 0.05 to about 8, about 0.05 to about 7, about 0.05 to about 6, about 0.05 to about 5, about 0.05 to about 4, about 0.05 to about 3, about 0.05 to about 2, about 0.05 to about 1, about 0.05 to about 0.5, about 0.05 to about 0.1, about 0.1 to about 9, about 0.1 to about 8, about 0.1 to about 7, about 0.1 to about 6, about 0.1 to about 5, about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 1 to about 9, about 1 to about 8, about 1 to about 6, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 9, about 2 to about 8, about 2 to about 7, about 2 to about 6, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 9, about 3 to about 8, about 3 to about 7, about 3 to about 6, about 3 to about 5, about 3 to about 4, about 4 to about 9, about 4 to about 8, about 4 to about 7, about 4 to about 6, about 4 to about 4, about 5 to about 9, about 5 to about 8, about 5 to about 7, about 5 to about 6, about 6 to about 9, about 6 to about 8, about 6 to about 7, about 7 to about 9, about 7 to about 8, or about 8 to about 9 by weight. In further embodiments, the aticaprant to filler ratio is about 0.056 by weight.
  • The composition may further comprise one or more of a filler, disintegrant, glidant, lubricant, solvent, coloring agent, binder. buffers, preservatives, penetration agents, wetting agents, surfactants, solubilizing agents, thickening agents, colorants, antioxidants, emulsifying agents, isotonizing agents, suspending agents, and/or viscosity increasing agents.
  • In some embodiments, the composition further comprises one or more of a disintegrant. Examples of disintegrants useful in the compositions include, e.g., the disintegrant is croscarmellose sodium. The composition comprises between about 0.5% to about 50% by weight, based on the weight of the composition, of the disintegrant. In some embodiments, the composition comprises about 0.5, about 1, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, or about 50% by weight, based on the weight of the composition, of the disintegrant. In other embodiments, the composition comprises about 0.5 to about 40%, about 0.5 to about 30%, about 0.5 to about 20%, about 0.5 to about 10%, about 0.5 to about 5%, about 0.5 to about 4%, about 0.5 to about 3%, about 0.5 to about 2%, about 0.5 to about 1%, about 5 to about 50%, about 5 to about 40%, about 5 to about 30%, about 5 to about 20%, about 5 to about 10%, about 10 to about 50%, about 10 to about 40%, about 10 to about 30%, about 10 to about 20%, about 20 to about 50%, about 20 to about 40%, about 20 to about 30%, about 30 to about 50%, about 30 to about 40%, or about 40 to about 50% by weight, based on the weight of the composition of the disintegrant. In further embodiments, the composition comprises about 5% by weight, based on the weight of the composition, of the disintegrant. The aticaprant to disintegrant ratio is between about 0.1 and 10 by weight. In some embodiments, the aticaprant to disintegrant ratio is about 0.1, about 0.5, about 1, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, or about 10 by weight. In other embodiments, the aticaprant to disintegrant ratio is about 0.1 to about 8, about 0.1 to about 7, about 0.1 to about 6, about 0.1 to about 5, about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 10, about 0.5 to about 9, about 0.5 to about 8, about 0.5 to about 7, about 0.5 to about 6, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 10, about 1 to about 9, about 1 to about 8, about 1 to about 7, about 1 to about 6, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 10, about 2 to about 9, about 2 to about 8, about 2 to about 7, about 2 to about 6, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 10, about 3 to about 9, about 3 to about 8, about 3 to about 7, about 3 to about 6, about 3 to about 5, about 3 to about 4, about 4 to about 10, about 4 to about 9, about 4 to about 8, about 4 to about 7, about 4 to about 6, about 4 to about 5, about 5 to about 10, about 5 to about 9, about 5 to about 8, about 5 to about 7, about 5 to about 6, about 6 to about 10, about 6 to about 9, about 6 to about 8, about 6 to about 7, about 7 to about 10, about 7 to about 9, about 7 to about 8, about 8 to about 10, about 8 to about 9, about 9 to about 10 by weight. In further embodiments, the aticaprant to disintegrant ratio is about 5 by weight. In other embodiments, the aticaprant to disintegrant ratio is about 1 by weight.
  • In other embodiments, the composition further comprises one or more of a glidant. Examples of glidants useful in the compositions include, e.g., silica, colloidal anhydrous. The composition comprises between about 0.1% to about 10% glidant by weight, based on the weight of the composition. In some embodiment, the composition contains about 0.1, about 0.5, about 1, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, or about 10% by weight, based on the weight of the composition, of the glidant. In other embodiments, the composition contains about 0.1 to about 9, about 0.1 to about 8, about 0.1 to about 7, about 0.1 to about 6, about 0.1 to about 5, about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 10, about 0.5 to about 9, about 0.5 to about 8, about 0.5 to about 7, about 0.5 to about 6, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 10, about 1 to about 9, about 1 to about 8, about 1 to about 7, about 1 to about 6, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 10, about 2 to about 9, about 2 to about 8, about 2 to about 7, about 2 to about 6, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 10, about 3 to about 9, about 3 to about 8, about 3 to about 7, about 3 to about 6, about 3 to about 5, about 3 to about 4, about 4 to about 10, about 4 to about 9, about 4 to about 8, about 4 to about 7, about 4 to about 6, about 4 to about 5, about 5 to about 10, about 5 to about 9, about 5 to about 8, about 5 to about 7, about 5 to about 6, about 6 to about 10, about 6 to about 9, about 6 to about 8, about 6 to about 7, about 7 to about 10, about 7 to about 9, about 7 to about 8, about 8 to about 10, about 8 to about 9, or about 9 to about 10% by weight, based on the weight of the composition, of the glidant. In further embodiments, the composition contains about 1% by weight, based on the weight of the composition, of the glidant. The aticaprant to glidant ratio is between 0.5 and 50 by weight. In some embodiments, the aticaprant to glidant ratio is about 0.5, about 1, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, or about 50 by weight. In other embodiments, the aticaprant to glidant ratio is about 0.5 to about 50, about 0.5 to about 45, about 0.5 to about 40, about 0.5 to about 35, about 0.5 to about 30, about 0.5 to about 25, about 0.5 to about 20, about 0.5 to about 15, about 0.5 to about 10, about 0.5 to about 5, about 0.5 to about 1, about 1 to about 50, about 1 to about 45, about 1 to about 40, about 1 to about 35, about 1 to about 30, about 1 to about 25, about 1 to about 20, about 1 to about 15, about 1 to about 10, about 1 to about 5, about 5 to about 50, about 5 to about 45, about 5 to about 40, about 5 to about 35, about 5 to about 30, about 5 to about 25, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 50, about 10 to about 45, about 10 to about 40, about 10 to about 35, about 10 to about 30, about 10 to about 25, about 10 to about 20, about 10 to about 15, about 20 to about 50, about 20 to about 40, about 20 to about 30, about 30 to about 50, about 23 to about 40, about 40 to about 50, or about 45 to about 50 by weight. In further embodiments, the aticaprant to glidant ratio is about 5 by weight.
  • In further embodiments, the composition further comprises one or more of a lubricant. Examples of lubricants useful in the compositions include, e.g., the lubricant is magnesium stearate. The composition comprises between about 0.05% to about 5% lubricant by weight, based on the weight of the composition. In some embodiments, the composition comprises about 0.05, about 0.1, about 0.5, about 1, about 1.5, about 2, about 2.5, about 3, about 3.5, about 4, about 4.5 or about 5% by weight, based on the weight of the composition, of lubricant. In other embodiments, the composition comprises about 0.05 to about 4.5, about 0.05 to about 4, about 0.05 to about 3, about 0.05 to about 2, about 0.05 to about 1, about 0.05 to about 0.5, about 0.05 to about 0.1, about 0.1 to about 5, about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 5, about 3 to about 4, or about 4 to about 5% by weight, based on the weight of the composition, of lubricant. In further embodiments, the composition comprises about 0.5% by weight, based on the weight of the composition, of the lubricant. The aticaprant to lubricant ratio is between about 1 and about 100 by weight. In some embodiments, the aticaprant to lubricant ratio is about 1, about 5, 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, about 50, about 55, about 60, about 65, about 70, about 75, about 80, about 85, about 90, about 95, or about 100 by weight. In other embodiments, the aticaprant to lubricant ratio is 1 to about 90, about 1 to about 80, about 1 to about 70, about 1 to about 60, about 1 to about 50, about 1 to about 40, about 1 to about 30, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 5 to about 100, about 1 to about 90, about 1 to about 80, about 1 to about 70, about 1 to about 60, about 1 to about 50, about 1 to about 40, about 1 to about 30, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 5 to about 100, about 5 to about 90, about 5 to about 80, about 5 to about 70, about 5 to about 60, about 5 to about 50, about 5 to about 40, about 5 to about 30, about 5 to about 20, about 5 to about 10, about 10 to about 100, about 10 to about 90, about 10 to about 80, about 10 to about 70, about 10 to about 60, about 10 to about 50, about 10 to about 40, about 10 to about 30, about 10 to about 20, about 20 to about 100, about 20 to about 90, about 20 to about 80, about 20 to about 70, about 20 to about 60, about 20 to about 50, about 20 to about 40, about 20 to about 30, about 30 to about 100, about 30 to about 90, about 30 to about 80, about 30 to about 70, about 30 to about 60, about 30 to about 50, about 30 to about 40, about 40, to about 100, about 40 to about 90, about 40 to about 80, about 40 to about 70, about 40 to about 60, about 40 to about 50, about 50 to about 100, about 50 to about 90, about 50 to about 80, about 50 to about 70, about 50 to about 60, about 60 to about 100, about 60 to about 90, about 60 to about 80, about 60 to about 70, about 70 to about 100, about 70 to about 90, about 70 to about 80, about 80 to about 100, about 80 to about 90, or about 90 to about 100 by weight. In further embodiments, the aticaprant to lubricant ratio is about 10 by weight.
  • In some aspects, the composition comprises one or more of an aticaprant to filler ratio between 0.005 and 9 by weight; an aticaprant to disintegrant ratio between 0.1 and 10 by weight; an aticaprant to glidant ratio between 0.5 and 50 by weight; and an aticaprant to lubricant ratio between 1 and 100 by weight.
  • In other aspects, the composition comprises one or more of an aticaprant to filler ratio of about 0.06 by weight; an aticaprant to disintegrant ratio of about 1 by weight; an aticaprant to glidant ratio of about 5 by weight; and an aticaprant to lubricant ratio of about 10 by weight.
  • In further aspects, the composition comprises about 5% by weight of aticaprant, about 88.5% by weight of filler, about 5% by weight of disintegrant by weight, about 1% by weight of glidant, and about 0.5% by weight of lubricant, based on the weight of the composition.
  • Desirably, the composition is formulated as a solid composition. In some embodiments, the solid composition is a tablet, capsule, or caplet. In other embodiments, the solid composition is a tablet such as an oral tablet. In further embodiments, the solid composition is a capsule such as an oral capsule. In yet other embodiments, the solid composition is a caplet such as an oral caplet. Optionally, the solid compositions are coated. For example, the coating is an enteric coating. By doing so, the coating provides a film coat on the solid composition. In some embodiments, the film coat comprises a coating powder. In other embodiments, the film coat comprises Opadry II Orange. In further embodiments, the coating powder is Opadry II Orange.
  • The tablet may comprise one or more layers. In some embodiments, the tablet comprises a core tablet and a film coat to provide a film coated tablet. The ratio of the film coat to core tablet is between about 0.03 to 10 by weight. In some embodiments, the ratio of the film coat to core tablet is about 0.03, 0.05, 0.08, 0.1, 0.5, 1, 2, 3, 4, 5, 6, 7, 8, 9, or 10 by weight, based on the weigh of the composition. In other embodiments, the ratio of the film coat to core tablet is about 0.03 to about 9, about 0.03 to about 8, about 0.03 to about 7, about 0.03 to about 6, about 0.03 to about 6, about 0.03 to about 5, about 0.03 to about 4, about 0.03 to about 3, about 0.03 to about 2, about 0.03 to about 1, about 0.03 to about 0.5, about 0.03 to about 0.1, about 0.05 to about 10, 0.05 to about 9, about 0.05 to about 8, about 0.05 to about 7, about 0.05 to about 6, about 0.05 to about 6, about 0.05 to about 5, about 0.05 to about 4, about 0.05 to about 3, about 0.05 to about 2, about 0.05 to about 1, about 0.05 to about 0.5, about 0.05 to about 0.1, about 0.1 to about 10, 0.1 to about 9, about 0.1 to about 8, about 0.1 to about 7, about 0.1 to about 6, about 0.1 to about 6, about 0.1 to about 5, about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, 0.5 to about 9, about 0.5 to about 8, about 0.5 to about 7, about 0.5 to about 6, about 0.5 to about 6, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 10, 1 to about 9, about 1 to about 8, about 1 to about 7, about 1 to about 6, about 1 to about 6, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 10, about 2 to about 9, about 2 to about 8, about 2 to about 7, about 2 to about 6, about 2 to about 6, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 10, about 3 to about 9, about 3 to about 8, about 3 to about 7, about 3 to about 6, about 3 to about 6, about 3 to about 5, about 3 to about 4, about 4 to about 10, about 4 to about 9, about 4 to about 8, about 4 to about 7, about 4 to about 6, about 4 to about 5, about 5 to about 10, about 5 to about 9, about 5 to about 8, about 5 to about 7, about 5 to about 6, about 6 to about 10, about 6 to about 9, about 6 to about 8, about 6 to about 7, about 7 to about 10, about 7 to about 9, about 7 to about 8, about 8 to about 10, about 8 to about 9, or about 9 to about 10.
  • The core tablet may contain one or more phases. In some embodiments, the core tablet comprises a first phase such as an intragranular phase. In other embodiments, the core tablet comprises a second phase such as an extragranular phase. In further embodiments, the core tablet comprises intragranular and extragranular phases.
  • The ratio of the intragranular phase to extragranular phase in the core tablet is between about 1.5 and about 3 by weight. In some embodiments, the ratio of the intragranular phase to extragranular phase in the core tablet is about 1.5, about 1.6, about 1.7, about 1.8, about 1.9, about 2, about 2.1, about 2.2, about 2.3, about 2.4, about 2.5, about 2.6, about 2.7, about 2.8, about 2.9, or about 3 by weight. In other embodiments, the ratio of the intragranular phase to extragranular phase in the core tablet is about 1.5 to about 2.8, about 1.5 to about 2.5, about 1.5 to about 2.3, about 1.5 to about 2, about 1.5 to about 1.8, about 1.8 to about 3, about 1.8 to about 2.8, about 1.8 to about 2.5, about 1.8 to about 2.3, about 2 to about 3, about 2 to about 2.8, about 2 to about 2.5, about 2 to about 2.3, about 2 to about 2.1, about 2.1 to about 3, about 2.1 to about 2.8, about 2.1 to about 2.5, about 2.1 to about 2.3, about 2.3 to about 3, about 2.3 to about 2.8, about 2.3 to about 2.5 to about 2.5 to about 3, about 2.5 to about 2.8, and about 2.8 to about 3 by weight. In further embodiments, the ratio of the intragranular phase to extragranular phase in the core tablet is about 2.1 by weight.
  • As for the composition, the solid composition contains aticaprant and one or more pharmaceutically acceptable excipients. In some aspects, the intragranular phase comprises aticaprant, a filler, a disintegrant, and a glidant. In other aspects, the intragranular phase comprises one filler. In further aspects, the intragranular phase comprises two fillers.
  • The intragranular phase comprises about 10 to about 120 mg of the filler. In some embodiments, the intragranular phase comprises about 10, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, about 100, about 110, or about 120 mg of the filler. In other embodiments, the intragranular phase comprises about 10 to about 110, about 10 to about 100, about 10 to about 90, about 10 to about 80, about 10 to about 70, about 10 to about 60, about 10 to about 50, about 10 to about 40, about 10 to about 30, about 10 to about 20, about 20 to about 120, about 20 to about 110, about 20 to about 100, about 20 to about 90, about 20 to about 80, about 20 to about 70, about 20 to about 60, about 20 to about 50, about 20 to about 40, about 20 to about 30, about 30 to about 120, about 30 to about 110, about 30 to about 100, about 30 to about 90, about 30 to about 80, about 30 to about 70, about 30 to about 60, about 30 to about 50, about 30 to about 40, about 40 to about 120, about 40 to about 110, about 40 to about 100, about 40 to about 90, about 40 to about 80, about 40 to about 70, about 40 to about 60, about 40 to about 50, about 50 to about 120, about 50 to about 110, about 50 to about 100, about 50 to about 90, about 50 to about 80, about 50 to about 70, about 50 to about 60, about 60 to about 120, about 60 to about 110, about 60 to about 100, about 60 to about 90, about 60 to about 80, about 60 to about 70, about 70 to about 120, about 70 to about 110, about 70 to about 100, about 70 to about 90, about 70 to about 80, about 80 to about 120, about 80 to about 110, about 80 to about 100, about 80 to about 90, about 90 to about 120, about 90 to about 110, about 90 to about 100, about 100 to about 120, about 100 to about 110, or about 110 to about 120. In further embodiments, the intragranular phase contains about 60 mg of filler. In yet other embodiments, the intragranular phase contains about 30 mg of microcrystalline cellulose. In still further embodiments, the intragranular phase contains about 30 mg of lactose monohydrate. In other embodiments, the intragranular phase contains about 60 mg of microcrystalline cellulose. In further embodiments, the intragranular phase contains about 60 mg of lactose monohydrate.
  • The intragranular phase comprises an aticaprant to filler ratio of between about 0.008 and 0.8 by weight. In some embodiments, the intragranular phase contains an aticaprant to filler ratio of about 0.008, about 0.005, about 0.001, about 0.01, about 0.05, about 0.1, about 0.2, about 0.3, about 0.4, about 0.5, about 0.6, about 0.7, or about 0.8 by weight. In other embodiments, the intragranular phase comprises an aticaprant to filler ratio of about 0.008 to about 0.7, about 0.008 to about 0.6, about 0.008 to about 0.5, about 0.008 to about 0.6, about 0.008 to about 0.5, about 0.008 to about 0.4, about 0.008 to about 0.3, about 0.008 to about 0.2, about 0.008 to about 0.1, about 0.008 to about 0.05, about 0.008 to about 0.01, about 0.01 to about 0.8, about 0.01 to about 0.7, 0.01 to about 0.6, about 0.01 to about 0.5, about 0.01 to about 0.4, about 0.01 to about 0.5, about 0.01 to about 0.4, about 0.01 to about 0.3, about 0.01 to about 0.2, about 0.01 to about 0.1, about 0.01 to about 0.05, about 0.05 to about 0.8, about 0.05 to about 0.9, about 0.05 to about 0.8, about 0.05 to about 0.7, about 0.05 to about 0.6, about 0.05 to about 0.6, about 0.05 to about 0.5, about 0.05 to about 0.4, about 0.05 to about 0.3, about 0.05 to about 0.2, about 0.05 to about 0.1, about 0.1 to about 0.8, about 0.1 to about 0.7, about 0.1 to about 0.6, about 0.1 to about 0.5, about 0.1 to about 0.4, about 0.1 to about 0.3, about 0.1 to about 0.2, about 0.2 to about 0.8, about 0.2 to about 0.7, about 0.2 to about 0.6, about 0.2 to about 0.5, about 0.2 to about 0.4, about 0.2 to about 0.3, about 0.3 to about 0.8, about 0.3 to about 0.7, about 0.3 to about 0.6, about 0.3 to about 0.5, about 0.3 to about 0.4, about 0.4 to about 0.8, about 0.4 to about 0.7, about 0.4 to about 0.6, about 0.4 to about 0.5, about 0.5 to about 0.8, about 0.5 to about 0.7, about 0.5 to about 0.6, about 0.6 to about 0.8, about 0.6 to about 0.7, or about 0.7 to about 0.8 by weight. In further embodiments, the intragranular phase comprises an aticaprant to filler ratio of about 0.08 by weight.
  • The intragranular phase also may contain a disintegrant. In some embodiments, the intragranular phase contains about 1 to about 10 mg of the disintegrant. In other embodiments, the intragranular phase contains about 1, about 1.5, about 2, about 2.5, about 3, about 3.5, about 4, about 4.5, about 5, about 5.5, about 6, about 6.5, 7, about 7.5, about 8, about 8.5, about 9, about 9.5 or about 10 mg of the disintegrant. In further embodiments, the intragranular phase contains about 1 to about 9, about 1 to about 8, about 1 to about 7, about 1 to about 6, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 10, about 2 to about 9, about 2 to about 8, about 2 to about 7, about 2 to about 6, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 2.5 to about 10, about 2.5 to about 9, about 2.5 to about 8, about 2.5 to about 7, about 2.5 to about 6, about 2.5 to about 5, about 2.5 to about 4, about 2.5 to about 3, about 3 to about 10, about 3 to about 9, about 3 to about 8, about 3 to about 7, about 3 to about 6, about 3 to about 5, about 3 to about 4, about 4 to about 10, about 4 to about 9, about 4 to about 8, about 4 to about 7, about 4 to about 6, about 4 to about 5, about 5 to about 10, about 5 to about 9, about 5 to about 8, about 5 to about 7, about 5 to about 6, about 6 to about 10, about 6 to about 9, about 6 to about 8, about 6 to about 7, about 7 to about 10, about 7 to about 9, about 7 to about 8, about 8 to about 10, about 8 to about 9, or about 0 to about 10. In yet other embodiments, the intragranular phase contains about 2.5 mg of the disintegrant. In still further embodiments, the intragranular phase contains about 5 mg of the disintegrant. In other embodiments, the intragranular phase contains about 2.5 mg of croscarmellose sodium. In further embodiments, the intragranular phase contains about 5 mg of croscarmellose sodium.
  • The intragranular phase may further contain a glidant. In some embodiments, the intragranular phase contains about 0.1 to about 5 mg of a glidant. In other embodiments, the intragranular phase contains about 0.1, about 0.5, about 1, about 1.5, about 2, about 2.5, about 3, about 3.5, about 4, about 4.5, or about 5 mg of a glidant. In further embodiments, the intragranular phase contains about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 5, about 3 to about 4, or about 4 to about 5 mg of a glidant. In yet other embodiments, the intragranular phase contains about 0.5 mg of the glidant. In still further embodiments, the intragranular phase contains about 1 mg of the glidant. In other embodiments, the intragranular phase contains about 0.5 mg of silica, colloidal anhydrous. In further embodiments, the intragranular phase contains about 1 mg of silica, colloidal anhydrous.
  • The intragranular phase has an aticaprant to disintegrant ratio of between about 0.2 and 20 by weight; In some embodiments, the intragranular phase has an aticaprant to disintegrant ratio of about 0.2, about 0.3, about 0.4, about 0.5, about 0.6, about 0.7, about 0.8, about 0.9, about 1, about 1.1, about 1.2, about 1.3, about 1.4, about 1.5, about 1.6, about 1.7, about 1.8, about 1.9, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 11, about 12, about 13, about 14, about 15, about 16, about 17, about 18, about 19, or about 20 by weight. In other embodiments, the intragranular phase comprises an aticaprant to disintegrant ratio of about 0.2 to about 18, about 0.2 to about 16, about 0.2 to about 14, about 0.2 to about 12, about 0.2 to about 10, about 0.2 to about 8, about 0.2 to about 6, about 0.2 to about 4, about 0.2 to about 3, about 0.2 to about 2, about 0.2 to about 1, about 0.2 to about 0.5, about 0.5 to about 20, about 0.5 to about 18, about 0.5 to about 16, about 0.5 to about 14, about 0.5 to about 12, about 0.5 to about 10, about 0.5 to about 8, about 0.5 to about 6, about 0.5 to about 4, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 20, about 1 to about 18, about 1 to about 16, about 1 to about 14, about 1 to about 12, about 1 to about 10, about 1 to about 8, about 1 to about 6, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 1 to about 1.5, about 2 to about 20, about 2 to about 18, about 2 to about 16, about 2 to about 14, about 2 to about 12, about 2 to about 10, about 2 to about 8, about 2 to about 6, about 2 to about 4, about 4 to about 20, about 4 to about 18, about 4 to about 16, about 4 to about 14, about 4 to about 12, about 4 to about 10, about 4 to about 6, about 4 to about 8, about 4 to about 6, about 5 to about 20, about 6 to about 18, about 6 to about 16, about 6 to about 14, about 6 to about 12, about 6 to about 10, about 6 to about 8, about 8 to about 20, about 8 to about 18, about 8 to about 16, about 8 to about 14, about 8 to about 12, about 8 to about 10, about 10 to about 20, about 10 to about 18, about 10 to about 16, about 10 to about 14, about 10 to about 12, about 12 to about 20, about 12 to about 18, about 12 to about 16, about 12 to about 14, about 14 to about 20, about 14 to about 18, about 14 to about 16, about 16 to about 20, about 16 to about 18, or about 18 to about 20 by weight. In further embodiments, the intragranular phase comprises an aticaprant to disintegrant ratio of about 2 by weight.
  • The intragranular phase comprises an aticaprant to glidant ratio of between about 1 and 100 by weight. In some embodiments, the intragranular phase comprises an aticaprant to glidant ratio of about 1, about 5, about 10, about 15, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, or about 100 by weight. In other embodiments, the intragranular phase comprises an aticaprant to glidant ratio of about 1 to about 80, about 1 to about 60, about 1 to about 40, about 1 to about 20, about 1 to about 15, about 1 to about 10, about 1 to about 5, about 2 to about 80, about 2 to about 60, about 2 to about 40, about 2 to about 20, about 2 to about 15, about 2 to about 10, about 2 to about 5, about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 80, about 40 to about 60, or about 60 to about 80 by weight. In further embodiments, the intragranular phase comprises an aticaprant to glidant ratio of 10 by weight.
  • The extragranular phase comprises one or more of a filler, a disintegrant, a glidant, and a lubricant. In some embodiments, the extragranular phase comprises a filler. In other embodiments, the extragranular phase comprises a disintegrant. In further embodiments, the extragranular phase comprises a glidant. In yet other embodiments, the extragranular phase comprises a lubricant.
  • The extragranular phase may comprise a filler. In some embodiments, the extragranular phase contains one filler. In other embodiment, the extragranular phase contains about 10 to about 80 mg of a filler. In further embodiments, the extragranular phase contains about 10, about 15, about 20, about 25, about 30, about 35, about 40, about 45, about 50, about 55, about 60, about 70, or about 80 mg of a filler. In still other embodiments, the extragranular phase contains about 10 to about 70, about 10 to about 60, about 10 to about 50, about 10 to about 40, about 10 to about 30, about 10 to about 20, about 10 to about 15, about 15 to about 80, about 15 to about 70, about 15 to about 60, about 15 to about 50, about 15 to about 40, about 15 to about 30, about 15 to about 20, about 20 to about 80, about 20 to about 70, about 20 to about 60, about 20 to about 50, about 20 to about 40, about 20 to about 30, about 25 to about 80, about 25 to about 70, about 25 to about 60, about 25 to about 50, about 25 to about 40, about 25 to about 30, about 30 to about 80, about 30 to about 70, about 30 to about 60, about 30 to about 50, about 30 to about 40, about 35 to about 80, about 35 to about 70, about 35 to about 60, about 35 to about 50, about 35 to about 40, about 40 to about 80, about 40 to about 70, about 40 to about 60, about 40 to about 50, about 40 to about 80, about 40 to about 70, about 45 to about 80, about 45 to about 70, about 45 to about 60, about 45 to about 50, about 50 to about 80, about 50 to about 70, about 50 to about 60, about 50 to about 55, about 55 to about 80, about 55 to about 70, about 55 to about 60, about 60 to about 80, about 60 to about 70, about 65 to about 80, about 65 to about 80, about 70 to about 80, or about 75 to about 80 mg of a filler. In yet further embodiments, the extragranular phase contains about 28.5 mg of the filler. In other embodiments, the extragranular phase contains about 28.5 of silicified microcrystalline cellulose. In further embodiments, the extragranular phase contains about 57 mg of the filler. In still other embodiments, the extragranular phase contains about 57 mg of silicified microcrystalline cellulose.
  • The extragranular phase may additionally contain a disintegrant. In some embodiments, the disintegrant is croscarmellose sodium. In other embodiments, the extragranular phase contains about 1 to about 10 mg of a disintegrant. In further embodiments, the extragranular phase contains about 1, about 2, about 2.5, about 3, about 4, about 5, about 6, about 7, about 7.5, about 8, about 9, or about 10 mg of a disintegrant. In yet other embodiments, the extragranular phase contains about 1 to about 10, about 1 to about 9, about 1 to about 8, about 1 to about 7, about 1 to about 6, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2.5, about 1 to about 2, about 2 to about 10, about 2 to about 9, about 2 to about 8, about 2 to about 7, about 2 to about 6, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 2.5 to about 10, about 2.5 to about 9, about 2.5 to about 8, about 2.5 to about 7, about 2.5 to about 6, about 2.5 to about 5, about 2.5 to about 4, about 2.5 to about 3, about 3 to about 10, about 3 to about 9, about 3 to about 8, about 3 to about 7, about 3 to about 6, about 3 to about 5, about 3 to about 4, about 4 to about 10, about 4 to about 9, about 4 to about 8, about 4 to about 7, about 4 to about 6, about 4 to about 5, about 5 to about 10, about 5 to about 9, about 5 to about 8, about 5 to about 7, about 5 to about 6, about 6 to about 10, about 6 to about 9, about 6 to about 8, about 6 to about 7, about 7 to about 10, about 7 to about 9, about 7 to about 8, about 7.5 to about 10, about 7.5 to about 9, about 7.5 to about 8, about 8 to about 10, about 8 to about 9, or about 9 to about 10 mg of a disintegrant. In still further embodiments, the extragranular phase contains about 2.5 mg of a disintegrant. In other embodiments, the extragranular phase contains about 5 mg of a disintegrant. In further embodiments, the extragranular phase contains about 2.5 mg of croscarmellose sodium. In still other embodiments, the extragranular phase contains about 5 mg of croscarmellose sodium.
  • The extragranular phase comprises a filler to disintegrant ratio of between about 1 and 100 by weight. In some embodiments, the extragranular phase comprises a filler to disintegrant ratio of 1, 5, 10, 20, 30, 40, 50, 60, 70, 80, 90, or 100 by weight. In further embodiments, the extragranular phase comprises a filler to disintegrant ratio of about 1 to about 90, about 1 to about 80, about 1 to about 70, about 1 to about 60, about 1 to about 50, about 1 to about 40, about 1 to about 30, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 5 to about 100, about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 10 to about 15, about 20 to about 100, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 100, about 40 to about 80, about 40 to about 60, about 60 to about 100, about 60 to about 80, or about 80 to about 100 by weight. In yet other embodiments, the extragranular phase comprises a filler to disintegrant ratio of about 11.4.
  • The extragranular phase further may contain a glidant. In some embodiments, the glidant is silica, colloidal anhydrous. In other embodiments, the extragranular phase contains about 0.1 to about 5 mg of the glidant. In further embodiments, the extragranular phase contains about 0.1, 0.25, 0.5, 0.75, 1, 2, 3, 4, or 5 mg of a glidant. In yet other embodiments, the extragranular phase contains about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 5, about 3 to about 4, or about 4 to about 5 mg of a glidant. In still further embodiments, the extragranular phase contains about 0.5 mg of a glidant. In other embodiments, the extragranular phase contains about 1 mg of a glidant. In further embodiments, the extragranular phase contains about 0.5 mg of silica, colloidal anhydrous. In yet other embodiments, the extragranular phase contains about 1 mg of silica, colloidal anhydrous.
  • The extragranular phase comprises a filler to glidant ratio of between about 5 and 500 by weight. In other embodiments, the extragranular phase comprises a filler to glidant ratio of about 5, about 10, about 25, about 50, about 100, about 150, about 200, about 250, about 300, about 350, about 400, about 450, or about 500. In further embodiments, the extragranular phase comprises a filler to glidant ratio of about 5 to about 400, about 5 to about 300, about 5 to about 200, about 5 to about 100, about 5 to about 75, about 5 to about 50, about 10 to about 500, about 10 to about 400, about 10 to about 300, about 10 to about 200, about 10 to about 100, about 10 to about 50, about 25 to about 500, about 25 to about 400, about 25 to about 300, about 25 to about 200, about 25 to about 100, about 25 to about 75, about 25 to about 50, about 50 to about 500, about 50 to about 400, about 50 to about 300, about 50 to about 200, about 50 to about 100, about 100 to about 500, about 100 to about 400, about 100 to about 300, about 100 to about 200, about 200 to about 500, about 200 to about 400, about 200 to about 300, about 300 to about 500, about 300 to about 400, or about 400 to about 500 by weight. In still further embodiments, the extragranular phase comprises a filler to glidant ratio of about 57.
  • The extragranular phase may also contain a lubricant. In some embodiments, the lubricant is magnesium stearate. In other embodiments, the extragranular phase contains about 0.1 to about 5 mg of the lubricant. In further embodiments, the extragranular phase contains about 0.1, 0.25, 0.5, 0.75, 1, 2, 3, 4, or 5 mg of a lubricant. In yet other embodiments, the extragranular phase contains about 0.1 to about 4, about 0.1 to about 3, about 0.1 to about 2, about 0.1 to about 1, about 0.1 to about 0.5, about 0.5 to about 5, about 0.5 to about 4, about 0.5 to about 3, about 0.5 to about 2, about 0.5 to about 1, about 1 to about 5, about 1 to about 4, about 1 to about 3, about 1 to about 2, about 2 to about 5, about 2 to about 4, about 2 to about 3, about 3 to about 5, about 3 to about 4, or about 4 to about 5 mg of a lubricant. In still further embodiments, the extragranular phase contains about 0.5 mg of a lubricant. In other embodiments, the extragranular phase contains about 1 mg of a lubricant. In further embodiments, the extragranular phase contains about 0.5 mg of magnesium stearate. In yet other embodiments, the extragranular phase contains about 1 mg of magnesium stearate.
  • The extragranular phase comprises a filler to lubricant ratio of between about 5 and 500 by weight. In other embodiments, the extragranular phase comprises a filler to lubricant ratio of about 5, about 10, about 25, about 50, about 100, about 150, about 200, about 250, about 300, about 350, about 400, about 450, or about 500. In further embodiments, the extragranular phase comprises a filler to lubricant ratio of about 5 to about 400, about 5 to about 300, about 5 to about 200, about 5 to about 100, about 5 to about 75, about 5 to about 50, about 10 to about 500, about 10 to about 400, about 10 to about 300, about 10 to about 200, about 10 to about 100, about 10 to about 50, about 25 to about 500, about 25 to about 400, about 25 to about 300, about 25 to about 200, about 25 to about 100, about 25 to about 75, about 25 to about 50, about 50 to about 500, about 50 to about 400, about 50 to about 300, about 50 to about 200, about 50 to about 100, about 100 to about 500, about 100 to about 400, about 100 to about 300, about 100 to about 200, about 200 to about 500, about 200 to about 400, about 200 to about 300, about 300 to about 500, about 300 to about 400, or about 400 to about 500 by weight. In still further embodiments, the extragranular phase comprises a filler to lubricant ratio of about 57.
  • In some embodiments, the intragranular phase comprises one or more of: an aticaprant to filler ratio of between about 0.008 and 0.8 by weight; an aticaprant to disintegrant ratio of between about 0.2 and 20 by weight; and an aticaprant to glidant ratio of between about 1 and 100 by weight.
  • In some embodiments, the extragranular phase comprises one or more of: a filler to disintegrant ratio of between about 1 and 100 by weight; a filler to glidant ratio of between about 5 and 500 by weight; and a filler to lubricant ratio of between about 5 and 500 by weight. In other embodiments, the extragranular phase comprises a filler to disintegrant ratio of about 11.4 by weight. In further embodiments, the extragranular phase comprises a filler to glidant ratio of about 57 by weight. In yet other embodiments, the extragranular phase comprises a filler to lubricant ratio of about 57 by weight.
  • In other aspects, the core tablet comprises about 5% aticaprant by weight, about 88.5% filler by weight, about 5% disintegrant by weight, about 1% glidant by weight, and about 0.5% lubricant by weight.
  • The oral tablet may be of weight that is suitable for administration by a patient. In some embodiments, the oral tablet has a core tablet of about 10 to about 1000 mg. In other embodiments, the core tablet is about 10, about 25, about 50, about 100, about 200, about 300, about 400, about 500, about 600, about 700, about 800, about 900, or about 1000 mg. In further embodiments, the core tablet is about 10 to about 900, about 10 to about 800, about 10 to about 700, about 10 to about 600, about 10 to about 500, about 10 to about 400, about 10 to about 300, about 10 to about 200, about 10 to about 100, about 10 to about 50, about 25 to about 1000, about 25 to about 900, about 25 to about 800, about 25 to about 700, about 25 to about 600, about 25 to about 500, about 25 to about 400, about 25 to about 300, about 25 to about 200, about 25 to about 100, about 25 to about 75, about 50 to about 1000, about 50 to about 900, about 50 to about 800, about 50 to about 700, about 50 to about 600, about 50 to about 500, about 50 to about 400, about 50 to about 300, about 50 to about 200, about 50 to about 100, about 100 to about 1000, about 100 to about 900, about 100 to about 800, about 100 to about 700, about 100 to about 600, about 100 to about 500, about 100 to about 400, about 100 to about 300, about 100 to about 200, about 200 to about 1000, about 200 to about 900, about 200 to about 800, about 200 to about 700, about 200 to about 600, about 200 to about 500, about 200 to about 400, about 200 to about 300, about 500 to about 1000, about 500 to about 800, about 500 to about 600, about 800 to about 1000, or about 800 to about 900 mg. In yet other embodiments, the core tablet is about 100 mg. In still further embodiments, the oral tablet comprises a core tablet of about 200 mg.
  • In some aspects, the core tablet contains a disintegrant. For example, the core tablet contains about 5 to about 100 mg of a disintegrant. In some embodiments, the core tablet contains about 5, about 10, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, or about 100 mg of a disintegrant. In other embodiments, the core tablet contains about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 100, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 20 to about 100, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 100, about 40 to about 80, about 40 to about 60, about 60 to about 100, about 60 to about 80, or about 80 to about 100 mg of a disintegrant. In further embodiments, the core tablet contains about 5 mg of the disintegrant. In yet other embodiments, the core tablet contains about 10 mg of the disintegrant.
  • In other aspects, the core tablet contains a glidant. For example, the core tablet contains about 1 to about 100 mg of a glidant. In some embodiments, the core tablet contains about 1, about 2, about 3, about 4, about 5, about 10, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, or about 100 mg of a glidant. In other embodiments, the core tablet contains about 1 to about 100, about 1 to about 80, about 1 to about 60, about 1 to about 40, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 2 to about 100, about 2 to about 80, about 2 to about 60, about 2 to about 40, about 2 to about 20, about 2 to about 10, about 2 to about 5, about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 100, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 20 to about 100, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 100, about 40 to about 80, about 40 to about 60, about 60 to about 100, about 60 to about 80, or about 80 to about 100 mg of a glidant. In further embodiments, the core tablet contains about 1 mg of the glidant. In yet other embodiments, the core tablet contains about 2 mg of the glidant.
  • In further aspects, the core tablet contains a lubricant. For example, the core tablet contains about 0.5 to about 100 mg of a lubricant. In some embodiments, the core tablet contains about 0.5, about 1, about 2, about 3, about 4, about 5, about 10, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, or about 100 mg of a lubricant. In other embodiments, the core tablet contains about 0.5 to about 80, about 0.5 to about 60, about 0.5 to about 40, about 0.5 to about 20, about 0.5 to about 10, about 0.5 to about 5, about 0.5 to about 1, about 1 to about 100, about 1 to about 80, about 1 to about 60, about 1 to about 40, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 2 to about 100, about 2 to about 80, about 2 to about 60, about 2 to about 40, about 2 to about 20, about 2 to about 10, about 2 to about 5, about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 100, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 20 to about 100, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 100, about 40 to about 80, about 40 to about 60, about 60 to about 100, about 60 to about 80, or about 80 to about 100 mg of a lubricant. In further embodiments, the core tablet contains about 0.5 mg of the lubricant. In yet other embodiments, the core tablet contains about 1 mg of the lubricant.
  • In further aspects, the core tablet contains a filler. For example, the core tablet contains about 1 to about 200 mg of a filler. In some embodiments, the core tablet contains about 1, about 2, about 3, about 4, about 5, about 10, about 20, about 30, about 40, about 50, about 60, about 70, about 80, about 90, about 100, about 110, about 120, about 130, about 140, about 150, about 160, about 170, about 180, about 190, or about 200 mg of a filler. In other embodiments, the core tablet contains about 1 to about 180, about 1 to about 160, about 1 to about 140, about 1 to about 120, 1 to about 100, about 1 to about 80, about 1 to about 60, about 1 to about 40, about 1 to about 20, about 1 to about 10, about 1 to about 5, about 2 to about 200, about 2 to about 180, about 2 to about 160, about 2 to about 140, about 2 to about 120, about 2 to about 100, about 2 to about 80, about 2 to about 60, about 2 to about 40, about 2 to about 20, about 2 to about 10, about 2 to about 5, about 5 to about 200 m, about 5 to about 180, about 5 to about 160, about 5 to about 140, about 5 to about 120, about 5 to about 100, about 5 to about 80, about 5 to about 60, about 5 to about 40, about 5 to about 20, about 5 to about 15, about 5 to about 10, about 10 to about 200, about 10 to about 180, about 10 to about 160, about 10 to about 140, about 10 to about 120, about 10 to about 100, about 10 to about 80, about 10 to about 60, about 10 to about 40, about 10 to about 20, about 20 to about 200, about 20 to about 180, about 20 to about 160, about 20 to about 140, about 20 to about 120, about 20 to about 100, about 20 to about 80, about 20 to about 60, about 20 to about 40, about 40 to about 200, about 40 to about 180, about 40 to about 160, about 40 to about 140, about 40 to about 120, about 40 to about 100, about 40 to about 80, about 40 to about 60, about 60 to about 200, about 60 to about 180, about 60 to about 160, about 60 to about 140, about 60 to about 120, about 60 to about 100, about 60 to about 200, about 60 to about 180, about 60 to about 160, about 60 to about 140, about 60 to about 120, about 60 to about 100, about 60 to about 80, about 80 to about 200, about 80 to about 180, about 80 to about 160, about 80 to about 140, about 80 to about 120, about 80 to about 100 mg, about 100 to about 200, about 100 to about 180, about 100 to about 160, about 100 to about 140, about 100 to about 120, about 120 to about 200, about 120 to about 180, about 120 to about 160, about 120 to about 140, about 140 to about 200, about 140 to about 180, about 140 to about 160, about 160 to about 200, about 160 to about 180, or about 180 to about 200 mg of a filler. In further embodiments, the core tablet contains about 88.5 mg of the filler. In yet other embodiments, the core tablet contains about 177 mg of the filler.
  • In some preferred embodiments, the oral tablet comprises a core tablet of about 100 mg and comprising about 5 mg aticaprant, about 5 mg disintegrant, about 88.5 mg filler, about 1 mg glidant, and about 0.5 mg lubricant.
  • In other preferred embodiments, oral tablet comprising a core tablet of about 200 mg, the core tablet comprising about 10 mg aticparant, about 10 mg disintegrant, about 177 mg filler, about 2 mg glidant, and about 1 mg lubricant.
  • As noted above, the core tablet may be coated with a film coat. In some embodiments, the oral tablet comprises about 3 mg of film coat. In other embodiments, the oral tablet comprises about 6 mg of film coat.
  • In some aspects, the film coated oral tablet comprises about 80 to about 99.9% by weight of the core tablet and about 0.1 to about 20% by weight, based on the weight of the film coated oral tablet, of the core tablet. In some embodiments, the film coated oral tablet comprises about 80, about 81, about 82, about 83, about 84, about 85, about 86, about 87, about 88, about 89, about 90, about 91, about 92, about 93, about 94, about 95, about 96, about 97, about 98, about 99, or 99.9% by weight, based on the weight of the film coated oral tablet. In other embodiments, the film coated oral tablet comprises about 80 to about 99, about 80 to about 96, about 80 to about 94, about 80 to about 92, about 80 to about 90, about 80 to about 88, about 80 to about 86, about 80 to about 84, about 80 to about 82, about 82 to about 99, about 82 to about 96, about 82 to about 94, about 82 to about 92, about 82 to about 90, about 82 to about 88, about 82 to about 86, about 82 to about 84, about 84 to about 99, about 84 to about 99, about 84 to about 96, about 84 to about 94, about 84 to about 92, about 84 to about 90, about 84 to about 88, about 84 to about 86, about 86 to about 99, about 86 to about 96, about 86 to about 94, about 86 to about 92, about 86 to about 90, about 86 to about 88, about 88 to about 99, about 88 to about 96, about 88 to about 94, about 88 to about 92, about 88 to about 90, about 90 to about 99, about 90 to about 96, about 90 to about 94, about 90 to about 92, about 92 to about 99, about 92 to about 96, about 92 to about 94, about 94 to about 99, about 94 to about 96, about 96 to about 99, or about 98 to about 99% by weight, based on the weight of the film coated oral tablet, of the core tablet. In further embodiments, the film coated oral tablet comprises about 97% core tablet by weight, based on the weight of the film coated oral tablet. In yet other embodiments, the film coated oral tablet comprises about 0.1 to about 20% by weight, based on the weight of the film coated oral tablet, of film coat. In still further embodiments, film coated oral tablet comprises about 0.1, about 0.5, about 1, about 2, about 3, about 4, about 5, about 6, about 7, about 8, about 9, about 10, about 11, about 12, about 13, about 14, about 15, about 16, about 17, about 18, about 19, or about 20% by weight, based on the weight of the film coated oral tablet, of the film coat. In other embodiments, the film coated oral tablet comprises about 0.1 to about 18, about 0.1 to about 16, about 0.1 to about 14, about 0.1 to about 12, about 0.1 to about 10, about 0.1 to about 8, about 0.1 to about 6, about 0.1 to about 4, about 0.1 to about 2, about 0.1 to about 1, about 0.5 to about 20, about 0.5 to about 18, about 0.5 to about 16, about 0.5 to about 14, about 0.5 to about 12, about 0.5 to about 10, about 0.5 to about 8, about 0.5 to about 6, about 0.5 to about 4, about 0.5 to about 2, about 1 to about 20, about 1 to about 18, about 1 to about 16, about 1 to about 14, about 1 to about 12, about 1 to about 10, about 1 to about 8, about 1 to about 6, about 1 to about 4, about 1 to about 2, about 2 to about 20, about 2 to about 18, about 2 to about 16, about 2 to about 14, about 2 to about 12, about 2 to about 10, about 2 to about 8, about 2 to about 8, about 2 to about 6, about 2 to about 4, about 4 to about 20, about 4 to about 18, about 4 to about 16, about 4 to about 12, about 4 to about 10, about 4 to about 8, about 4 to about 6, about 6 to about 20, about 6 to about 18, about 6 to about 16, about 6 to about 14, about 6 to about 12, about 6 to about 10, about 6 to about 8, about 8 to about 20, about 8 to about 18, about 8 to about 16, about 8 to about 14, about 8 to about 12, about 8 to about 10, about 10 to about 20, about 10 to about 18, about 10 to about 16, about 10 to about 14, about 10 to about 12, about 12 to about 20, about 12 to about 18, about 12 to about 16, about 12 to about 14, about 14 to about 20, about 14 to about 18, m about 14 to about 16, about 16 to about 20, about 16 to about 18, or about 18 to about 20% by weight, based on the weight of the film coated oral tablet, of the film coat. In further embodiments, the film coated oral tablet comprises about 3% by weight, based on the weight of the film coated oral tablet, of the film coat. In yet other embodiments, the film coated oral tablet comprises about 97% core tablet by weight and about 3% film coat by weight, based on the weight of the film coated oral tablet.
  • In some embodiments, the disclosure provides oral tablets comprising about 5 mg aticaprant, wherein the oral tablet comprises a core tablet of about 100 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 30 mg microcrystalline cellulose, about 30 mg lactose monohydrate, about 2.5 mg croscarmellose sodium, and about 0.5 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 28.5 mg silicified microcrystalline cellulose, about 2.5 mg croscarmellose sodium, about 0.5 mg silica, colloidal anhydrous, and about 0.5 mg magnesium stearate.
  • In other embodiments, the disclosure provides oral tablets comprising about 10 mg aticaprant, wherein the oral tablet comprises a core tablet of about 200 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 60 mg microcrystalline cellulose, about 60 mg lactose monohydrate, about 5 mg croscarmellose sodium, and about 1 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 57 mg silicified microcrystalline cellulose, about 5 mg croscarmellose sodium, about 1 mg silica, colloidal anhydrous, and about 1 mg magnesium stearate.
  • The solid compositions may also have a desirable dissolution profile that provide the desired release of aticaprant. In some embodiments, the solid composition contains about 2 mg and 20 mg of aticaprant and has a dissolution profile comprising a Q value of between about 60% and 90% at 45 minutes, under the dissolution operating conditions of (i) apparatus: Paddle (USP Type 2, Ph. Eur., JP), (ii) dissolution medium: 0.01 M hydrochloric acid, (iii) volume: 900 mL, (iv) temperature: 37±0.5° C., (v) rotation speed: 50 rpm, and (vi) analytical finish: UHPLC with UV detection at 247 nm. In some embodiments, the Q value is about 60, about 61, about 62, about 63, about 64, about 65, about 66, about 67, about 68, about 69, about 70, about 71, about 72, about 73, about 74, about 75, about 75, about 76, about 77, about 78, about 79, about 80, about 81, about 82, about 83, about 84, about 85, about 86, about 87, about 88, about 89, about 90, about 91, about 92, about 93, about 94, or about 95% at 45 minutes. In other embodiments, the Q value is about 60 to about 85, about 60 to about 80, about 60 to about 75, about 60 to about 70, about 70 to about 90, about 70 to about 85, about 70 to about 80, about 70 to about 75, about 75 to about 90, about 75 to about 85, about 75 to about 80, about 80 to about 90, about 80 to about 85, or about 85 to about 90% at 45 minutes. In further embodiments, the Q value is between about 70% and 80% at 45 minutes. In other aspects, the Q value is about 75% at 45 minutes.
  • Advantageously, aticaprant may be administered once daily, or the total daily dosage may be administered in divided doses of two, three or four times daily. In some embodiments, the composition containing aticaprant is administered once daily. In other embodiments, the oral tablet containing aticaprant is administered once daily. In further embodiments, the solid pharmaceutical composition containing anticaprant is administered once daily.
  • As described herein, in particular, the patient had an inadequate response to other antidepressant therapy prior to treatment with aticaprant. Thus, in a particular embodiment, the disclosure relates to aticaprant, for use as described herein, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with aticaprant. In a further particular embodiment, the disclosure also relates to the use of aticaprant in the manufacture of a medicament, as described herein, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with of aticaprant. In a further particular embodiment, the disclosure further relates to a package or pharmaceutical product as described herein, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with aticaprant. Such antidepressant therapy can be in particular selected from a selective serotonin reuptake inhibitor (SSRI), serotonin-norepinephrine reuptake inhibitor (SNRI), or a combination thereof.
  • As described herein, aticaprant may be used as adjunctive treatment, or in other words, in conjunction, as an add-on, or in combination with one or more antidepressants, for example, the patient may be already, or also, administered one or more antidepressants. Thus, in a further particular embodiment, the disclosure relates to aticaprant, for use as described herein, comprising administration of aticaprant, as adjunctive treatment with an effective amount of one or more antidepressants. In a further particular embodiment, the disclosure relates to aticaprant, for use as described herein, comprising administration of aticaprant, in conjunction with an effective amount of one or more antidepressants. In a further particular embodiment, the disclosure relates to aticaprant, for use as described herein, comprising administration of aticaprant, in combination with an effective amount of one or more antidepressants. In a further particular embodiment, the disclosure also relates to the use of aticaprant, in the manufacture of a medicament, as described herein, wherein the treatment comprises administration of an effective amount of aticaprant, as adjunctive treatment with an effective amount of one or more antidepressants. In a further particular embodiment, the disclosure also relates to the use of aticaprant, as described herein, wherein the treatment comprises administration of an effective amount of aticaprant, in conjunction with an effective amount of one or more antidepressants. In a further particular embodiment, the disclosure also relates to the use of aticaprant, as described herein, wherein the treatment comprises administration of an effective amount of aticaprant, in combination with an effective amount of one or more antidepressants. In a further particular embodiment, the disclosure further relates to a package or pharmaceutical product as described herein, wherein the instructions for treatment direct the administration of an effective amount of aticaprant, as adjunctive treatment with an effective amount of one or more antidepressants. In a further particular embodiment, the disclosure further relates to a package or pharmaceutical product as described herein, wherein the instructions for treatment direct the administration of an effective amount of aticaprant, in conjunction with an effective amount of one or more antidepressants. In a further particular embodiment, the disclosure further relates to a package or pharmaceutical as described herein, wherein the instructions for treatment direct administration of an effective amount of aticaprant, in combination with an effective amount of one or more antidepressants. Such one or more antidepressants can be selected from a selective serotonin reuptake inhibitor (SSRI), serotonin-norepinephrine reuptake inhibitor (SNRI), or a combination thereof.
  • As already described, the disclosure relates to aticaprant, for use as described herein. In a particular embodiment, aticaprant is S-aticaprant. In a further embodiment of the disclosure, aticaprant, in particular S-aticaprant, for use as described herein, is to be administered in an amount of about 2 to about 35 mg, more in particular, of about 10 mg. In a yet further embodiment, aticaprant, in particular S-aticaprant, for use as described herein, is administered orally. Furthermore, in a further particular embodiment, the disclosure relates to aticaprant, in particular S-aticaprant, for use as described herein, administered once daily. The disclosure also relates to the use of aticaprant, in the manufacture of a medicament, as described herein. In a particular embodiment, aticaprant is S-aticaprant. In a further embodiment of the use as described herein, about 2 to about 35 mg aticaprant, is to be administered, more in particular, about 10 mg. In a yet further embodiment of the use, aticaprant is to be administered orally. Furthermore, in a further particular embodiment of the use aticaprant in particular S-aticaprant, is to be administered once daily. In a further particular embodiment, the disclosure further relates to a package or pharmaceutical product as described herein, wherein aticaprant is in particular S-aticaprant. In a further embodiment of the package or pharmaceutical product as described herein, the instructions for treatment direct administration of about 2 to about 35 mg aticaprant, more in particular, about 10 mg. In a yet further embodiment of the package or pharmaceutical product as described herein, the instructions for treatment direct aticaprant, in particular S-aticaprant, is for oral administration. Furthermore, in a further particular embodiment of the package or pharmaceutical product, as described herein, the instructions for treatment direct aticaprant, in particular S-aticaprant, is for once daily administration.
  • Advantageously, administration of aticaprant, does not result in weight gain during treatment, including clinically relevant weight gain. Thus, in a further particular embodiment, the disclosure relates to aticaprant, for use as described herein, wherein the patient does not experience weight gain during the treatment with aticaprant. In a further particular embodiment, the disclosure relates to a use as defined herein, wherein the patient does not experience weight gain during the treatment with aticaprant. In a further particular embodiment, the disclosure further relates to a package or pharmaceutical product as described herein, wherein the patient does not experience weight gain during the treatment with aticaprant. The body weight of the patient can in particular be assessed at the time of the initial administration of aticaprant.
  • It was also unexpectedly observed that, based on assessment at the time of initial administration, the patient does not experience a decrease in sexual functioning during the treatment with aticaprant. Thus, in further particular embodiment, the disclosure relates to aticaprant, for use as described herein, wherein the patient does not experience a decrease in sexual functioning during the treatment with aticaprant. In a further particular embodiment, the disclosure relates to a use as described herein, wherein the patient does not experience a decrease in sexual functioning during the treatment with aticaprant. In a further particular embodiment, the disclosure relates to a package or pharmaceutical product as described herein, wherein the patient does not experience a decrease in sexual functioning during the treatment with aticaprant. Such term “sexual functioning” comprises sexual drive, sexual arousal, vaginal lubrication, erection, orgasm achievement, or orgasm satisfaction. Sexual satisfaction can be assessed by methods known to the skilled person, for example, by applying the Arizona Sexual Experience Scale (ASEX).
  • As already described, the patient has anhedonia. In certain aspects, the anhedonia is moderate. In other aspects, the anhedonia is severe. Anhedonia can be measured, through an anhedonia scale, for example, the Snaith Hamilton Pleasure Scale (SHAPS). Thus, in a particular embodiment, the disclosure relates to aticaprant, for use as described herein, wherein the anhedonia of the patient is reduced by at least 40%, as measured by the change from baseline in total score in an anhedonia scale following 6 weeks of the treatment with aticaprant, more in particular, the anhedonia of the patient is reduced within about 3 weeks to about 6 weeks as measured by the change from baseline in total score in an anhedonia scale. In a further particular embodiment, the anhedonia scale is the Snaith Hamilton Pleasure Scale (SHAPS). Thus, in a particular embodiment, the disclosure relates to the use as described herein, wherein the anhedonia of the patient is reduced by at least 40%, as measured by the change from baseline in total score in an anhedonia scale following 6 weeks of the treatment with aticaprant, more in particular, the anhedonia of the patient is reduced within about 3 weeks to about 6 weeks as measured by the change from baseline in total score in an anhedonia scale. In a further particular embodiment, the anhedonia scale is the Snaith Hamilton Pleasure Scale (SHAPS). In a further particular embodiment, the disclosure relates to the package or pharmaceutical product as described herein, wherein the anhedonia of the patient is reduced by at least 40%, as measured by the change from baseline in total score in an anhedonia scale following 6 weeks of the treatment with aticaprant, more in particular, the anhedonia of the patient is reduced within about 3 weeks to about 6 weeks as measured by the change from baseline in total score in an anhedonia scale. In a further particular embodiment, the anhedonia scale is the Snaith Hamilton Pleasure Scale (SHAPS).
    • Treatment Methods
  • In one aspect of the present invention, methods are provided for treating patients having a more severe type of depression, i.e., major depressive disorder, using the compounds, compositions, e.g., solid compositions, and tablets, e.g., oral tablets, described herein. The patient also may be experiencing anhedonia. Because MDD alone is difficult to treat, treatment patients having anhedonia are even more problematic since their ability to gauge pleasure is impaired. Thus, such patients often receive inadequate treatment due to ineffective medications, repeated and unnecessary medical appointments, lack of patient compliance, overall patient frustration, among others. Further, antidepressants are known to have a variety of side effects such as weight gain, metabolic side effects, extrapyramidal symptoms, akathisia, cognitive impairment, among others. Thus, patients may choose to refrain from or stop taking antidepressants to avoid or prevent any side-effects.
  • The methods described herein are effective in managing the patient's depression and anhedonia using aticaprant. Desirably, the methods successfully permit the patient to manage their depression while simultaneously reducing anhedonia. In particular embodiments, the patients treated according to the described methods have moderate to severe anhedonia. The term “anhedonia” as used herein refers to the lack of or decreased ability to experience pleasure in daily activities. The term anhedonia includes loss of pleasure in sensory experiences (i.e., touch, taste, smell), as well as social interactions. In some embodiments, anhedonia and depressed mood are diagnostic criteria for a major depressive episode as part of MDD. Anhedonia also describes deficits in one or more components of reward-related behavior, also known as the pleasure cycle, such as wanting, liking, and learning. The pleasure cycle can be divided into three phases: the appetitive phase (dominated by wanting), the consummatory phase (dominated by liking), and the satiety phase (dominated by learning). The appetitive phase is characterized by the initial energy expenditure to attain a reward; the consummatory phase is enjoyment of the reward; and the satiety phase is characterized by learning and feedback integration.
  • To assess a potential effect on anhedonia, an anhedonia scale may be used. For example, the Snaith-Hamilton Pleasure Scale (SHAPS) analysis is a validated scale for the measurement of anhedonia. The SHAPS is a subject completed scale in which subjects score whether or not they experience pleasure in performing a list of activities or experiences. The SHAPS is a self-reported 14-item instrument, developed for the assessment of hedonic capacity. Subjects score whether they experience pleasure in performing a list of activities or experiences. Subjects can rate the answers as 1-4 where 1 indicates “Definitely agree”, 2 indicates “Agree”, 3 indicates “Disagree” and 4 indicates “Definitely disagree”. The subject's item responses are summed to provide a total score ranging from 14 to 56. A higher total SHAPS score indicates higher levels of current anhedonia. Physician/clinical judgment can be used to assess anhedonia separately or in conjunction with an anhedonia scale.
  • In some embodiments, the patient has moderate anhedonia. In other embodiments, the patient has severe anhedonia. An assessment of moderate or severe anhedonia is typically determined physician/clinical judgment and/or by one or more tests that provide insight into whether a patient has anhedonia. For example, the severity of the anhedonia may be determined using the SHAPS method. In some embodiments, a patient with moderate or severe anhedonia is considered to have a high level of anhedonia. For example, a patient with a SHAPS score of 38 or greater is considered to have moderate to severe anhedonia that can be considered a high level of anhedonia. In some embodiments, a high level of anhedonia is reflected by a SHAPS score of at least about 40, about 42, about 44, about 46, about 48, about 50, about 52, about 54, about 56, about 58, or higher. A patient with mild or no anhedonia would be considered to have a low level of anhedonia that is assessed by physician/clinical judgment and/or one or more tests. For example, a patient with a SHAPS score of less than 38 is considered to have low anhedonia. In certain embodiments, a patient with mild anhedonia may have a SHAPS score of 20 to less than 38, for example, a SHAPS score of 20 to about 36, about 22 to about 36, about 24 to about 36, about 26 to about 36, about 26 to about 34, about 26 to about 32, about 26 to about 30, about 26 to about 28, about 28 to about 36, about 28 to about 36, about 30, to about 36, about 32 to about 36, about 34 to about 36, about 20 to about 34, about 22 to about 34, about 24 to about 34, about 26 to about 32, about 26 to about 30, about 26 to about 28, about 28 to about 36, about 28 to about 34, about 28 to about 32, about 28 to about 30, about 30 to about 36, about 30 to about 34, about 30 to about 32, about 32 to about 36, about 32 to about 34, or about 34 to about 36. Typically, a SHAPS score of less than 20 can be considered to correspond to normal hedonic functioning, and for purposes of this disclosure, would fall into the low category of anhedonia, e.g., a SHAPS score of less than 38.
  • In some embodiments, the patient's anhedonia is reduced from a high level of anhedonia to a low level of anhedonia. In yet other embodiments, the patient's anhedonia is reduced by at least about 40%, as measured by the change from baseline in total score in an anhedonia scale following treatment with aticaprant. In yet other embodiments, the patient's anhedonia is reduced by at least about 40%, about 50%, about 60%, about 70%, about 80%, about 90%, or about 95%, as measured by the change from baseline in total score in an anhedonia scale following treatment with aticaprant. In still further embodiments, In yet other embodiments, the patient's anhedonia is reduced by about 40 to about 90%, about 50 to about 90%, about 60 to about 90%, about 70 to about 90%, about 80 to about 90%, about 40 to about 80%, about 50 to about 80%, about 60 to about 80%, about 70 to about 80%, about 40 to about 70%, about 50 to about 70%, about 60 to about 70%, about 40 to about 60%, about 50 to about 60%, or about 50 to about 60%, as measured by the change from baseline in total score in an anhedonia scale following treatment with aticaprant. In other embodiments, the patient's anhedonia is ameliorated, i.e., reduced by 100%, as measured by the change from baseline in total score in an anhedonia scale following treatment with aticaprant.
  • Reduction of anhedonia after initiating treatment with aticaprant may be measured relative to the anhedonia of the patient as measured before treatment with aticaprant, i.e., a baseline anhedonia measurement. In doing so, the treating clinician is able to calculate the change of anhedonia from the baseline to the real time anhedonia measurement at any point after treatment with aticaprant. Thus, standard methods for measuring anhedonia may be used, such as an anhedonia scale, e.g., SHAPS.
  • Desirably, a baseline anhedonia measurement is obtained no more than about 1 week before initiating treatment with aticaprant. In some embodiments, a baseline anhedonia measurement is obtained about 7 days, about 6 days, about 5 days, about 4 days, about 3 days, about 2 days, or about 1 day before treatment with aticaprant. In further embodiments, a baseline anhedonia measurement is obtained about 24 hours, about 18 hours, about 12 hours, about 8 hours, about 4 hours, about 2 hours, about 1 hours, about 30 minutes, or about 15 minutes before initiating treatment with aticaprant.
  • The patient's change of anhedonia will depend on several factors including, without limitation, anhedonia severity, patient's sensitivity to aticaprant, other pharmaceutical agents being administered, among others. In some embodiments, the patient's anhedonia is reduced after about 3 weeks of treatment with aticaprant. In other embodiments, the patient's anhedonia is reduced after about 3 weeks of treatment with aticaprant. In further embodiments, the patient's anhedonia is reduced after about 3 weeks to about 6 weeks, and, in certain embodiments, through week 6, of treatment with aticaprant. In certain embodiments, the patient's anhedonia is reduced by at least about 40%, as measured by the change from baseline in total score in an anhedonia scale following about 6 weeks of the treatment with aticaprant. In further embodiments, the anhedonia of the patient is reduced within about 3 weeks, and in some embodiments within about 3 weeks to about 6 weeks, as measured by the change from baseline in total score in an anhedonia scale and/or by physician/clinical judgement.
  • The methods described herein were found to not only improve the patient's depression and anhedonia symptoms, but resulted in fewer antidepressant side effects. Doing so resulted in less absenteeism (i.e., more visits or interactions with physicians), greater cognitive functioning, improvements in health-related quality of life, more interest and engagement in everyday activities, improvement in family and inter-personal relationships, ability to function in the workplace, fewer hospitalizations, among others.
  • In some embodiments, the disclosure provides methods for treating MDD in a human patient by administering to the patient a pharmaceutical composition comprising between about 2 mg and 20 mg aticaprant, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with aticaprant. In some embodiments, administration of the pharmaceutical composition to the patient achieves a pharmacokinetic (PK) profile comprising one or more of the PK parameters noted above (dose-normalized to 10 mg) after administration of the composition to a human after at least a 10-hour fast.
  • As used herein, unless otherwise noted, the terms “subject” and “patient” refer to a human, who has been the object of treatment, observation or experiment. Preferably, the patient has experienced and/or exhibited at least one symptom of the disease or disorder to be treated and/or prevented. In some embodiments, the patient is an adult. As used herein, the term “adult” as used herein refers to a human that is about 18 years of age or older. In certain aspects, the patient is an elderly adult, i.e., greater than or equal to 65 years of age.
  • As used herein, unless otherwise noted, the terms “treating”, “treatment” and the like, shall include the management and care of a subject or patient (preferably mammal, more preferably human) for the purpose of combating a disease, condition, or disorder and includes the administration of a compound described herein to prevent the onset of the symptoms or complications, alleviate one or more of the symptoms or complications, or eliminate the disease, condition, or disorder.
  • As used herein, the term “depression” (also referred to as depressive disorder) includes major depressive disorder, persistent depressive disorder, seasonal affective disorder, postpartum depression, premenstrual dysphoric disorder, situational depression, anhedonia, melancholic, mid-life depression, late-life depression, bipolar depression, depression due to identifiable stressors, treatment resistant depression, or combinations thereof. In certain embodiments, the depression is major depressive disorder. In other embodiments, the major depressive disorder is with melancholic features or anxious distress. In further embodiments, the depression is treatment-resistant depression. In other embodiments, the depression is major depressive disorder with suicidal ideation.
  • As known in the art, a patient is considered to have major depressive disorder if exhibiting five or more symptoms during the same two week period that are a change from previous functioning; depressed mood and/or loss of interest/pleasure must be present; excluding symptoms clearly attributable to another medical condition. See, e.g., Table 4.
  • TABLE 4
    1. Depressed mood: Most of the day, nearly every day; may be
    subjective (e.g., feels sad, empty, hopeless) or observed by
    others (e.g., appears tearful); in children and adolescents,
    can be irritable mood
    2. Loss of interest/pleasure: Markedly diminished interest/pleasure in
    all (or almost all) activities most of the day, nearly every day;
    may be subjective or observed by others
    3. Weight loss or gain: Significant weight loss (without dieting) or
    gain (change of >5% body weight in a month), or decrease or
    increase in appetite nearly every day; in children, may be
    failure to gain weight as expected
    4. Insomnia or hypersomnia: Nearly every day
    5. Psychomotor agitation or retardation: Nearly every day and
    observable by others (not merely subjectively restless or slow)
    6. Fatigue: Or loss of energy, nearly every day
    7. Feeling worthless or excessive/inappropriate guilt: Nearly every
    day; guilt may be delusional; not merely self-reproach or guilt
    about being sick
    8. Decreased concentration: Nearly every day; may be indecisiveness;
    may be subjective or observed by others
    9. Thoughts of death/suicide” Recurrent thoughts of death (not
    just fear of dying), recurrent suicidal ideation without specific
    plan, or suicide attempt, or a specific plan for suicide
  • In some embodiments, to be diagnosed with MDD, the following criteria also are met:
  •
    1. Symptoms cause clinically significant distress or impairment
    in social, occupational, or other important areas of functioning
    2. Episode not attributable to physiological effects of a
    substance or another medical condition
    3. Episode not better explained by schizoaffective disorder,
    schizophrenia, schizophreniform disorder, delusional disorder,
    or other specified and unspecified schizophrenia spectrum and
    other psychotic disorders
    4. No history of manic or hypomanic episode
  • Major depressive disorder may be categorized as mild, moderate, or severe. In some embodiments, the MDD is mild. In other embodiments, the MDD is moderate. In further embodiments, the MDD is severe. As used herein, “mild MDD” applies to a patient having few, if any, symptoms in excess of those required to make the diagnosis, the intensity of the symptoms is distressing but manageable, and the symptoms result in minor impairment in social or occupational functioning. The mild MDD may be a single episode (ICD-10 F32.0) or a recurrent episode (ICD-10 F33.0). “Moderate MDD” applies to a patient having a number of symptoms, intensity of symptoms, and/or functional impairment are between those specified for “mild” and “severe.” The moderate MDD may be a single episode (ICD-10 F32.1) or a recurrent episode (ICD-10 F33.1). “Severe MDD” applies to a patient where the number of symptoms is substantially in excess of that required to make the diagnosis, the intensity of symptoms is seriously distressing and unmanageable, and the symptoms markedly interfere with social and occupational functioning, and urgent symptom control is necessary. In some embodiments, the severe MDD may be a single episode (ICD-10 F32.2) or a recurrent episode (ICD-10 F33.2). In other embodiments, MDD is classified according to the DSM-5 definition of Table 5.
  • TABLE 5
    DSM-5 Criteria for MDD
    1. Depressed Mood At least 1
    2. Loss of interest/pleasure (anhedonia)
    1. Weight loss or gain At least 5
    2. Sleep problems
    3. Psychomotor agitation or retardation
    4. Guilt or worthlessness
    5. Decreased concentration
    6. Suicidality
    7. Fatigue
    1. Symptoms cause significant distress or impairment Must have all 4
    2. Not attributable to medical condition
    3. Exclude schizophrenia disorders
    4. No hx of mania or hypomania
  • Several scales are known in the art that may be utilized to diagnose or monitor patients with MDD. Examples of these scales include, without limitation, the Montgomery-Åsberg Depression Rating Scale (MADRS), Clinical Global Impression—Severity (CGI-S) scale, Symptoms of Major Depressive Disorder Scale (SMDDS), Self-Assessment of Treatment Experience (SATE) scale, and Massachusetts General Hospital (MGH) Antidepressant Treatment Response Questionnaire (ATRQ), i.e., MGH-ATRQ.
  • In some embodiments, MADRS is utilized to diagnose and/or monitor the patient. MADRS is a 10-item rating scale that is used in antidepressant studies. It is clinician-administered and designed to be used in subjects with MDD to measure the overall severity of depressive symptoms. The MADRS scale is validated, reliable, and acceptable to regulatory health authorities as a primary scale to determine efficacy in major depression. In some embodiments, MADRS is administered using the Structured Interview Guide for the MADRS (SIGMA). The scale consists of 10 items, each of which is scored from 0 (item not present or normal) to 6 (severe or continuous presence of the symptoms), summed for a total possible score of 60. Higher scores represent a more severe condition. The MADRS evaluates apparent sadness, reported sadness, inner tension, sleep appetite, concentration, lassitude, inability to feel (interest level), pessimistic thoughts, and suicidal thoughts.
  • In other embodiments, CGI-S is utilized to diagnose and/or monitor the patient's depression. CGI-S is a scale that rates the severity of the subject's illness at the time of assessment, relative to the clinician's past experience with subjects who have the same diagnosis and improvement with treatment. CGI-S provides an overall clinician-determined summary measure of severity of subject's illness that considers all available information, including knowledge of subject's history, psychosocial circumstances, symptoms, behavior, and impact of symptoms on subject's ability to function. CGI-S evaluates severity of psychopathology on scale of 0 to 7. Subject is assessed on severity of mental illness at time of rating according to: 0=not assessed; 1=normal (not at all ill); 2=borderline mentally ill; 3=mildly ill; 4=moderately ill; 5=markedly ill; 6=severely ill; 7=among most extremely ill patients.
  • In further embodiments, SMDDS is utilized to diagnose and/or monitor the patient's depression. SMDDS is a subjective rating of the patient. The SMDDS is a 16-item PRO measure. Each item is rated by the subject according to a 5-point Likert scale. Subjects respond to each question using a rating scale between 0 (“Not at all” or “Never”) to 4 (“Extremely” or “Always”). The total score ranges from 0 to 60. The SMDDS uses a 7-day recall period and verbal rating scales. Higher score indicates more severe depressive symptomatology.
  • In yet other embodiments, SATE is utilized to diagnose and/or monitor the patient's depression. SATE is a one to three questionnaire administered when the subject is unable to complete other evaluations, i.e., away from the clinical setting such as at home. SATE is useful to evaluate improvement or deterioration of depressive symptoms of the subjects over a short period of time. For rating overall depression, subject selected one option out of Improved, not changed or got worse; for depression improvement, subject selected one option out of slightly improved, much improved, very much improved and for depression worsen subject selected slightly worse, much worse, very much worse. See, Table 6.
  • TABLE 6
    SATE Questionnaire
    Question 1: Since starting this study medication, overall would you say
    your depression is:
    Improved
    Got worse
    Not changed
    If the subject selects answer 1 (Improved), following question is asked:
    Question 2: How much did your depression improve?
    Slightly improved
    Much improved
    Very much improved
    If the subject selects answer 3 (Got worse), following question is asked:
    Question 3: How much did your depression worsen?
    Slightly worse
    Much worse
    Very much worse
  • The MGH-ATRQ is a self-rated scale used to determine treatment resistance in patient's having MDD. This questionnaire examines the antidepressant treatment history, using specific anchor points to define the adequacy of both dose and duration of each antidepressant trial, and the degree of symptomatic improvement. The MGH-ATRQ permits determining treatment resistance in depression and is known to those skilled in the art.
  • In certain embodiments, the patient had an inadequate response to other antidepressant therapy. “Inadequate response” as used herein refers to a patient experiencing a less than about 50% reduction in depressive symptom severity from the start of initiating treatment. Typically, the inadequate response is during a current/active episode of the depression. In some embodiments, an inadequate response refers to a patient experiencing about 26 to less than about 50% reduction in depressive symptom severity from the start of initiating treatment. In other embodiments, an inadequate response refers to a patient experiencing about 26 to about 49, about 26 to about 45, about 26 to about 40, about 26 to about 35, about 26 to about 30, about 30 to about 49, about 30 to about 45, about 30 to about 40, about 30 to about 35, about 35 to about 49, about 35 to about 45, about 35 to about 40, about 40 to about 49, or about 40 to about 45% reduction in depressive symptom severity from the start of initiating treatment. A patient's response may be measured by one or more scales described herein and/or by physician/clinical judgment. In some embodiments, an inadequate response is measured by MGH-ATRQ, MADRS, or SHAPS. In further embodiments, an inadequate response is measured by MGH-ATRQ.
  • To the extent a patient is said to have a partial response to treatment, this refers to some minor to moderate symptomatic improvement since the initiation of treatment, but some of the initial symptoms are still present and troubling to the patient and these persistent symptoms still affect behavior and function. For instance, the patient's motivation, productivity, and interest in his or her usual activities may still be impaired.
  • The term “other antidepressant therapy” as used herein refers to an antidepressant medication or non-pharmacological treatment that is used to treat patients having depression. In some aspects, the other antidepressant therapy is an antidepressant medication. In other aspects, the other antidepressant therapy is a non-pharmacological treatment. In further aspects, the other antidepressant therapy is an antidepressant medication other than aticaprant.
  • The antidepressant medication is any pharmaceutical agent which can be used to treat depression. Suitable examples include, without limitation, mono-amine oxidase inhibitors, tricyclics, tetracyclics, non-cyclics, triazolopyridines, selective serotonin reuptake inhibitors (SSRI), serotonin receptor antagonists, serotonin noradrenergic reuptake inhibitors (SNRI), noradrenergic and specific serotonergic agents, noradrenaline reuptake inhibitors, or antipsychotics (typical or atypical antipsychotics). Examples of mono-amine oxidase inhibitors include phenelzine, tranylcypromine, moclobemide, and the like. Examples of tricyclics include imipramine, amitriptyline, desipramine, nortriptyline, doxepin, protriptyline, trimipramine, clomipramine, amoxapine, and the like. Examples of tetracyclics includes maprotiline, and the like. Examples of non-cyclics include nomifensine, and the like. Examples of triazolopyridines include trazodone, and the like. Examples of SSRIs include fluoxetine, sertraline, paroxetine, citalopram, citalopram, escitalopram, fluvoxamine, and the like. Examples of serotonin receptor antagonists include nefazadone, and the like. Examples of SNRIs include venlafaxine, milnacipran, desvenlafaxine, duloxetine, levomilnacipran and the like. Examples of noradrenergic and specific serotonergic agents include mirtazapine, and the like. Examples of noradrenaline reuptake inhibitors include reboxetine, edivoxetine and the like. Examples of typical antipsychotics include phenothiazines (e.g., chlorpromazine, thioridazine, fluphenazine, perphenazine, trifluoperazine, levomepromazin), thioxanthenes (e.g., thiothixene, flupentixol), butyrophenones (e.g., haloperidol), dibenzoxazepines (e.g., loxapine), dihydroindolones (e.g., molindone), substituted benzamides (e.g., sulpride, amisulpride), and the like. Examples of atypical antipsychotics include paliperidone, clozapine, risperidone, olanzapine, quetiapine, zotepine, ziprasidone, iloperidone, perospirone, blonanserin, sertindole, ORG-5222, sonepiprazole, aripiprazole, nemonapride, SR-31742, CX-516, SC-111, NE-100, divalproate (mood stabilizer) and the like. In further embodiments, the antidepressant medication includes natural products such as Kava-Kava, St. John's Wort, and the like or dietary supplements such as s-adenosylmethionine, and the like. In yet other embodiments, the antidepressant medication includes neuropeptides such as thyrotropin-releasing hormone and the like or compounds targeting neuropeptide receptors such as neurokinin receptor antagonists and the like. In still further embodiments, the antidepressant medication is a hormone such as triiodothyronine, and the like. In other embodiments, the antidepressant medication is SSRI, SNRI, or a combination thereof. Preferably, the antidepressant is a SSRI that is escitalopram, sertraline, paroxetine, fluoxetine or citalopram. In other embodiments, the antidepressant medication is a SNRI that is venlafaxine, duloxetine, vortioxeine or desvenlafaxine.
  • The non-pharmacologic treatment for use herein may be selected by one skilled in the art. In some embodiments, the non-pharmacologic treatment is psychotherapy, transcranial magnetic stimulation, or the like.
  • Therapeutically effective amounts/dosage levels and dosage regimens for the other antidepressant therapy may be readily determined by one of ordinary skill in the art. For example, therapeutic dosage amounts and regimens for pharmaceutical agents approved for sale are publicly available, for example as listed on packaging labels, in standard dosage guidelines, in standard dosage references such as the Physician's Desk Reference (Medical Economics Company or online at http:///www.pdrel.com) or other sources.
  • In some embodiments, other antidepressant therapy may include one antidepressant medication. In other embodiments, other antidepressant therapy includes two or more antidepressant medications. In further embodiments, other antidepressant therapy includes two antidepressant medications. In yet other embodiments, other antidepressant therapy includes three antidepressant medications. The attending physician would be able to select suitable antidepressant therapies for use as described herein.
  • In certain embodiments, the patient was receiving treatment with other antidepressant therapy prior to receiving aticaprant. In some embodiments, the patient was receiving treatment with other antidepressant therapy that comprised a SSRI, SNRT, or a combination thereof. In other embodiments, the patient stopped treatment with other antidepressant therapy before initiating treatment with aticaprant.
  • Also encompassed by the methods described herein include adjunctive treatment with an effective amount of one or more antidepressants. As used herein, the term “adjunctive treatment” and “adjunctive therapy” shall mean treatment of a patient in need thereof by administering aticaprant in combination with one or more antidepressant(s), wherein aticaprant and the antidepressant(s) are administered by any suitable means, simultaneously, sequentially, separately, or in a single pharmaceutical formulation.
  • In some aspects, aticaprant is administered adjunctively with other antidepressant(s) currently being administered to the patient, including current antidepressant(s) to which the patient had an inadequate response, i.e., the antidepressant failed to treat the patient's depression. In other embodiments, aticaprant is administered adjunctively with an antidepressant(s) not previously administered to the patient, i.e., a new antidepressant. In still other embodiments, aticaprant is administered in a regimen with an antidepressant(s) previously administered to the patient.
  • Where aticaprant and other antidepressant(s) are administered in separate dosage forms, the number of dosages administered per day for each active compound may be the same or different and more typically different. The antidepressant may be dosed as prescribed by the attending physician and/or by its label and aticaprant is dosed as described herein. Typically, a patient is under concurrent treatment with both an antidepressant and aticaprant, where both are administered by their prescribed dosing regimens. The aticaprant and antidepressant(s) may be administered according to simultaneous or alternating regimens, at the same or different times during the course of the therapy, concurrently in divided or single forms.
  • Aticaprant and the antidepressant(s) may be administered via the same or different routes of administration. Examples of suitable methods of administration include, but are not limited to, oral, intravenous (iv), intranasal (in) intramuscular (im), subcutaneous (sc), transdermal, buccal, or rectal. In some embodiments, aticaprant is administered orally.
  • Treatment with aticaprant as described herein has several advantages over the treatments in the art. In some embodiments, the patient does not experience many of the side effects that are associated with other antidepressants, i.e., antidepressants other than aticaprant. In certain aspects, the patient does not experience weight gain during the treatment with aticaprant. As used herein, the term “weight gain” refers to an increase in the weight of patient, relative to the weight of the patient before taking aticaprant or the weight of the patient that is assessed at the time of the initial administration of aticaprant. In certain embodiments, the patient may actually see a decrease in overall weight, relative to the weight of the patient before taking aticaprant. In further embodiments, the patient's weight is stable, i.e., does not increase or decrease. In certain embodiments, the patient does not experience a clinically relevant weight gain which is characterized as a weight increase of ≥7%.
  • This is contrary to many other antidepressants where weight gain, including clinically relevant weight gain, is a common, but unfortunate, side-effect.
  • In further aspects, the patient does not experience a decrease in sexual functioning during the treatment with aticaprant. As used herein, the term “decrease in sexual functioning” refers to reducing or lessening of one or more components of the human sex drive, i.e., sexual functioning. In some embodiments, the sexual functioning comprises one or more of sexual drive, sexual arousal, vaginal lubrication, erection, orgasm achievement, or orgasm satisfaction. In other embodiments, the sexual functioning comprises sexual drive. In further embodiments, the sexual functioning comprises vaginal lubrication satisfaction. In further embodiments, the sexual functioning comprises orgasm achievement. In yet other embodiments, the sexual functioning comprises orgasm satisfaction. Desirably, the patient's sexual functioning is assessed at the time of initial administration of aticaprant. Thus, the patient's sexual functioning while taking aticaprant can be compared to the patient's sexual functioning before administration of aticaprant. Sexual functioning may be assessed by using standard scales and techniques such as the Arizona Sexual Experience Scale (ASEX). The ASEX is used to investigate whether aticaprant has a further positive or negative effect on sexual function. The ASEX is 5 item rating scale administered to patients that quantifies sexual drive, sexual arousal, vaginal lubrication or penile erection, ability to reach orgasm and satisfaction. Scores range from 5 to 30, and two different versions of the scale are available (males and females).
  • Other scales may be utilized to determine the effectiveness of the methods used herein to treat the patient. Examples include the Cognitive and Physical Functioning Questionnaire (CPFQ), Karolinska Sleepiness Scale (KSS), and Temporal Experience of Pleasure Scale (TEPS). The CPFQ is a brief self-report scale that provides additional information regarding the impact of adjunctive treatment on aspects of cognitive and executive function including attention, memory and mental acuity. Subjects with MDD are often reported to have difficulties with functioning in this area. The KSS is a subject-reported assessment used to rate sleepiness on a scale of 1 to 9, ranging from “extremely alert” (1) to “very sleepy, great effort to keep awake, fighting sleep” (9). The TEPS includes 18 items, 2 subscales designed to distinguish between anticipatory and consummatory pleasure.
  • The methods described herein include administering an effective amount of aticaprant to the patient. The term “effective amount” as used herein, means that amount of active compound or pharmaceutical agent that elicits the biological or medicinal response in a human that is being sought by a researcher, medical doctor or other clinician, which includes alleviation of one or more of the symptoms of the disease or disorder being treated. In some embodiments, aticaprant is utilized in an effective amount as determined by the attending physician. In other embodiments, other antidepressant(s) is utilized in an effective amount either separately or in combination with aticaprant.
    • Embodiments
  • The invention provides also the following non-limiting embodiments:
      • Embodiment 1 is a pharmaceutical composition comprising about 2 mg to about 20 mg aticaprant and a filler, wherein the composition comprises between about 0.1% to about 90% aticaprant by weight.
      • Embodiment 2 is the pharmaceutical composition of Embodiment 1, further comprising one or more of: a disintegrant, a glidant, a lubricant, a solvent, a coloring agent, and a binder.
      • Embodiment 3 is the pharmaceutical composition of Embodiment 1 or 2, wherein the composition comprises between about 10% to about 99.9% filler by weight.
      • Embodiment 4 is the pharmaceutical composition of any one of Embodiments 1-3, wherein the composition comprises a disintegrant.
      • Embodiment 5 is the pharmaceutical composition of Embodiment 4, wherein the composition comprises between about 0.5% to about 50% disintegrant by weight.
      • Embodiment 6 is the pharmaceutical composition of any one of Embodiments 1-5, wherein the composition comprises a glidant.
      • Embodiment 7 is the pharmaceutical composition of Embodiment 6, wherein the composition comprises between about 0.1% to about 10% glidant by weight.
      • Embodiment 8 is the pharmaceutical composition of any one of Embodiments 1-7, wherein the composition comprises a lubricant.
      • Embodiment 9 is the pharmaceutical composition of Embodiment 8, wherein the composition comprises between about 0.05% to about 5% lubricant by weight.
      • Embodiment 10 is the pharmaceutical composition of any one of Embodiments 1-9, wherein the composition comprises one or more of: an aticaprant to filler ratio between 0.005 and 9 by weight; an aticaprant to disintegrant ratio between 0.1 and 10 by weight; an aticaprant to glidant ratio between 0.5 and 50 by weight; and an aticaprant to lubricant ratio between 1 and 100 by weight.
      • Embodiment 11 is the pharmaceutical composition of any one of Embodiments 1-10, wherein the composition comprises about 5% aticaprant by weight, about 88.5% filler by weight, about 5% disintegrant by weight, about 1% glidant by weight, and about 0.5% lubricant by weight.
      • Embodiment 12 is the pharmaceutical composition of any one of Embodiments 1-11, wherein the composition is an oral tablet.
      • Embodiment 13 is the pharmaceutical composition of Embodiment 12, wherein the oral tablet is a film coated oral tablet comprising (a) a core tablet and (b) a film coat.
      • Embodiment 14 is the pharmaceutical composition of Embodiment 13, wherein the ratio of the film coat to core tablet is between about 0.03 to 10 by weight.
      • Embodiment 15 is the pharmaceutical composition of Embodiment 13 or 14, wherein the film coat comprises a coating powder.
      • Embodiment 16 is the pharmaceutical composition of any one of Embodiments 13-15, wherein the core tablet comprises an intragranular and an extragranular phase.
      • Embodiment 17 is the pharmaceutical composition of Embodiment 16, wherein the ratio of intragranular to extragranular phase in the core tablet is between about 1.5 and 3.
      • Embodiment 18 is the pharmaceutical composition of Embodiment 16, wherein the intragranular phase comprises aticaprant, a filler, a disintegrant, and a glidant.
      • Embodiment 19 is the pharmaceutical composition of Embodiment 18, wherein the intragranular phase comprises one or more of: an aticaprant to filler ratio of between about 0.008 and 0.8 by weight; an aticaprant to disintegrant ratio of between about 0.2 and 20 by weight; and an aticaprant to glidant ratio of between about 1 and 100 by weight.
      • Embodiment 20 is the pharmaceutical composition of Embodiment 16 or 17, wherein the extragranular phase comprises a filler, a disintegrant, a glidant, and a lubricant.
      • Embodiment 21 is the pharmaceutical composition of Embodiment 20, wherein the extragranular phase comprises one or more of: a filler to disintegrant ratio of between about 1 and 100 by weight; a filler to glidant ratio of between about 5 and 500 by weight; and a filler to lubricant ratio of between about 5 and 500 by weight.
      • Embodiment 22 is the pharmaceutical composition of any one of Embodiments 13-21, wherein the film coated oral tablet comprises about 97% core tablet by weight and about 3% film coat by weight and wherein the core tablet comprises about 5% aticaprant by weight, about 88.5% filler by weight, about 5% disintegrant by weight, about 1% glidant by weight, and about 0.5% lubricant by weight.
      • Embodiment 23 is the pharmaceutical composition of any one of Embodiments 1-22, wherein the composition is an oral tablet comprising a core tablet of about 100 mg, the core tablet comprising about 5 mg aticaprant, about 5 mg disintegrant, about 88.5 mg filler, about 1 mg glidant, and about 0.5 mg lubricant.
      • Embodiment 24 is the pharmaceutical composition of Embodiment 23, further comprising about 3 mg of film coat.
      • Embodiment 25 is the pharmaceutical composition of any one of Embodiments 1-24, wherein the composition is an oral tablet comprising a core tablet of about 200 mg, the core tablet comprising about 10 mg Aticparant, about 10 mg disintegrant, about 177 mg filler, about 2 mg glidant, and about 1 mg lubricant.
      • Embodiment 26 is the pharmaceutical composition of Embodiment 25, further comprising about 6 mg of film coat.
      • Embodiment 27 is the pharmaceutical composition of any of Embodiments 1-26, wherein the filler is selected from: microcrystalline cellulose, lactose monohydrate, and silicified microcrystalline cellulose.
      • Embodiment 28 is the pharmaceutical composition of any of Embodiments 2-27, wherein the disintegrant is croscarmellose sodium.
      • Embodiment 29 is the pharmaceutical composition of any of Embodiments 2-28, wherein the glidant is silica, colloidal anhydrous.
      • Embodiment 30 is the pharmaceutical composition of any of Embodiments 2-29, the lubricant is magnesium stearate.
      • Embodiment 31 is the pharmaceutical composition of any of Embodiments 15-30, wherein the coating powder is Opadry II Orange.
      • Embodiment 32 is an oral tablet comprising about 5 mg aticaprant, wherein the oral tablet comprises a core tablet of about 100 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 30 mg microcrystalline cellulose, about 30 mg lactose monohydrate, about 2.5 mg croscarmellose sodium, and about 0.5 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 28.5 mg silicified microcrystalline cellulose, about 2.5 mg croscarmellose sodium, about 0.5 mg silica, colloidal anhydrous, and about 0.5 mg magnesium stearate.
      • Embodiment 33 is the oral tablet of Embodiment 32, further comprising about 3 mg film coat.
      • Embodiment 34 is the oral tablet of Embodiment 33, wherein the film coat comprises Opadry II Orange.
      • Embodiment 35 is an oral tablet comprising about 10 mg aticaprant, wherein the oral tablet comprises a core tablet of about 200 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 60 mg microcrystalline cellulose, about 60 mg lactose monohydrate, about 5 mg croscarmellose sodium, and about 1 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 57 mg silicified microcrystalline cellulose, about 5 mg croscarmellose sodium, about 1 mg silica, colloidal anhydrous, and about 1 mg magnesium stearate.
      • Embodiment 36 is the oral tablet of Embodiment 35, further comprising 3 mg film coat.
      • Embodiment 37 is the oral tablet of Embodiment 36, wherein the film coat comprises Opadry II Orange.
      • Embodiment 38 is a pharmaceutical composition comprising between about 2 mg and 20 mg aticaprant, wherein the composition has a pharmacokinetic (PK) profile comprising one or more of the following parameters after administration of the composition to a human after at least a 10-hour fast (dose-normalized to 10 mg):
        • a. a mean Cmax between about 30 and 40 ng/mL;
        • b. a mean AUCinfinity between about 300 and 430 h*ng/mL;
        • c. a mean AUClast between about 280 and 430 h*ng/mL;
        • d. a median tmax between about 1 to 4 hours.
      • Embodiment 39 is the pharmaceutical composition of Embodiment 38, wherein the mean Cmax is between about 30 and 35 ng/mL.
      • Embodiment 40 is the pharmaceutical composition of Embodiment 38 or 39, wherein the mean AUCinfinity is between about 300 and 320 h*ng/mL.
      • Embodiment 41 is the pharmaceutical composition of any one of Embodiments 38-40, wherein the mean AUClast is between about 280 and 310 h*ng/mL.
      • Embodiment 42 is the pharmaceutical composition of any one of Embodiments 38-41, wherein the median tmax is about 1.5 hours.
      • Embodiment 43 is the pharmaceutical composition of any one of Embodiments 38-42, wherein the composition is an oral tablet.
      • Embodiment 44 is the pharmaceutical composition of any one of Embodiments 38-43, wherein the composition further comprises one or more of: a filler, a disintegrant, a glidant, a lubricant, a binder, and a coloring agent.
      • Embodiment 45 is the pharmaceutical composition of any one of Embodiments 38-44, wherein the composition comprises between about 0.1% and 90% aticaprant by weight.
      • Embodiment 46 is the pharmaceutical composition of any one of Embodiments 38-45, wherein the composition comprises about 5 mg aticaprant or about 10 mg aticaprant.
      • Embodiment 47 is the pharmaceutical composition of any one of Embodiments 38-46, wherein the composition comprises one or more of: an aticaprant to filler ratio between 0.005 and 9 by weight; an aticaprant to disintegrant ratio between 0.1 and 10 by weight; an aticaprant to glidant ratio between 0.5 and 50 by weight; and an aticaprant to lubricant ratio between 1 and 100 by weight.
      • Embodiment 48 is the pharmaceutical composition of any one of Embodiments 38-47, wherein the composition wherein the composition comprises about 5% aticaprant by weight, about 88.5% filler by weight, about 5% disintegrant by weight, about 1% glidant by weight, and about 0.5% lubricant by weight.
      • Embodiment 49 is a method for treating major depressive disorder (MDD) in a human patient, the method comprising administering to the patient a pharmaceutical composition comprising between about 2 mg and 20 mg aticaprant, wherein the patient had an inadequate response to other antidepressant therapy prior to treatment with aticaprant, and wherein the administration of the pharmaceutical composition to the patient achieves a pharmacokinetic (PK) profile comprising one or more of the following PK parameters (dose-normalized to 10 mg) after administration of the composition to a human after at least a 10-hour fast:
        • e. a mean Cmax between about 30 and 40 ng/mL;
        • f. a mean AUCinfinity between about 300 and 430 h*ng/mL;
      • g. a mean AUClast between about 280 and 430 h*ng/mL;
      • h. a median tmax between about 1 to 4 hours.
      • Embodiment 50 is the method of Embodiment 49, wherein the mean Cmax is between about 30 and 35 ng/mL.
      • Embodiment 51 is the method of Embodiment 49 or 50, wherein the mean AUCinfinity is between about 300 and 320 h*ng/mL.
      • Embodiment 52 is the method of any one of Embodiments 49-51, wherein the mean AUClast is between about 280 and 310 h*ng/mL.
      • Embodiment 53 is the method of any one of Embodiments 49-52, wherein the median tmax is about 1.5 hours.
      • Embodiment 54 is the method of any one of Embodiments 49-53, wherein the composition is an oral tablet.
      • Embodiment 55 is the method of any one of Embodiments 49-54, wherein the composition further comprises one or more of: a filler, a disintegrant, a glidant, a lubricant, a binder, and a coloring agent.
      • Embodiment 56 is the method of any one of Embodiments 49-55, wherein the composition comprises between about 0.1% and 90% aticaprant by weight.
      • Embodiment 57 is the method of any one of Embodiments 49-56, wherein the composition comprises between about 10% and 99.9% filler by weight.
      • Embodiment 58 is the method of any one of Embodiments 49-57, wherein the composition comprises one or more of: an aticaprant to filler ratio between 0.005 and 9 by weight; an aticaprant to disintegrant ratio between 0.1 and 10 by weight; an aticaprant to glidant ratio between 0.5 and 50 by weight; and an aticaprant to lubricant ratio between 1 and 100 by weight.
      • Embodiment 59 is the method of any one of Embodiments 49-58, wherein the composition wherein the composition comprises about 5% aticaprant by weight, about 88.5% filler by weight, about 5% disintegrant by weight, about 1% glidant by weight, and about 0.5% lubricant by weight.
      • Embodiment 60 is the method of any one of Embodiments 49-59, wherein the patient has anhedonia.
      • Embodiment 61 is the method of any one of Embodiments 49-60, wherein the pharmaceutical composition comprises about 5 mg aticaprant.
      • Embodiment 62 is the method of any one of Embodiments 49-60, wherein the pharmaceutical composition comprises about 10 mg aticaprant.
      • Embodiment 63 is the method of any one of Embodiments 49-60, wherein the other antidepressant therapy comprised one or more antidepressants.
      • Embodiment 64 is the method of Embodiment 63, wherein the one or more antidepressants comprised a SSRI, SNRI, or a combination thereof.
      • Embodiment 65 is the method of any one of Embodiments 49-64, wherein the aticaprant is S-aticaprant.
      • Embodiment 66 is the method of any one of Embodiments 49-65, further comprising treatment with an effective amount of one or more antidepressants.
      • Embodiment 67 is the method of Embodiment 66, wherein the one or more antidepressants is a SSRI, SNRI, or combination thereof.
      • Embodiment 68 is the method of any one of Embodiments 49-67, wherein the pharmaceutical composition comprising aticaprant is administered once daily.
      • Embodiment 69 is a solid pharmaceutical composition comprising between about 2 mg and 20 mg aticaprant, wherein the composition has a dissolution profile comprising a Q value of between about 60% and 90% at 45 minutes, under the following dissolution operating conditions:
        • Apparatus: Paddle (USP Type 2, Ph. Eur., JP)
        • Dissolution medium: 0.01 M hydrochloric acid
        • Volume: 900 mL
        • Temperature: 37+/−0.5 degrees Celsius
        • Rotation Speed: 50 rpm
        • Analytical Finish: UHPLC with UV detection at 247 nm.
      • Embodiment 70 is the solid pharmaceutical composition of Embodiment 69, wherein the composition comprises about 5 mg or about 10 mg aticaprant.
      • Embodiment 71 is the solid pharmaceutical composition of Embodiment 69 or 70, wherein the Q value is between about 70% and 80% at 45 minutes.
      • Embodiment 72 is the solid pharmaceutical composition of Embodiment 71, wherein the Q value is about 75% at 45 minutes.
      • Embodiment 73 is the solid pharmaceutical composition of any one of Embodiments 69-72, wherein the composition is an oral tablet.
      • Embodiment 74 is the solid pharmaceutical composition of any one of Embodiments 69-73, wherein the composition further comprises one or more of: a filler, a disintegrant, a glidant, a lubricant, a binder, and a coloring agent.
      • Embodiment 75 is the solid pharmaceutical composition of any one of Embodiments 69-74, wherein the composition comprises between about 0.1% and 90% aticaprant by weight.
      • Embodiment 76 is the solid pharmaceutical composition of any one of Embodiments 69-75, wherein the composition comprises between about 10% and 99.9% filler by weight.
      • Embodiment 77 is the solid pharmaceutical composition of any one of Embodiments 69-76, wherein the composition comprises one or more of: an aticaprant to filler ratio between 0.005 and 9 by weight; an aticaprant to disintegrant ratio between 0.1 and 10 by weight; an aticaprant to glidant ratio between 0.5 and 50 by weight; and an aticaprant to lubricant ratio between 1 and 100 by weight.
      • Embodiment 78 is the solid pharmaceutical composition of any one of Embodiments 69-77, wherein the composition wherein the composition comprises about 5% aticaprant by weight, about 88.5% filler by weight, about 5% disintegrant by weight, about 1% glidant by weight, and about 0.5% lubricant by weight.
      • Embodiment 79 is a method of treating major depressive disorder (MDD) in a human patient comprising administering to the patient the pharmaceutical composition of any one of
      • Embodiments 1-32 or 38-48, the oral tablet of any of Embodiments 33-37, or the solid pharmaceutical composition of any of Embodiments 69-78.
      • Embodiment 80 is a method of Embodiment 79, wherein the patient has anhedonia.
      • Embodiment 81 is the method of any one of Embodiments 79-80, wherein the pharmaceutical composition, the oral tablet, or the solid pharmaceutical composition comprises about 5 mg aticaprant.
      • Embodiment 82 is the method of any one of Embodiments 79-81, wherein the pharmaceutical composition, the oral tablet, or the solid pharmaceutical composition comprises about 10 mg aticaprant.
      • Embodiment 83 is the method of any one of Embodiments 79-82, wherein the patient had an inadequate response to other antidepressant therapy prior to the treatment with aticaprant.
      • Embodiment 84 is the method of Embodiment 83 wherein the other antidepressant therapy comprised one or more antidepressants.
      • Embodiment 85 is the method of Embodiment 84, wherein the one or more antidepressants comprised a SSRI, SNRI, or a combination thereof.
      • Embodiment 86 is the method of any one of Embodiments 79-85, wherein the aticaprant is S-aticaprant.
      • Embodiment 87 is the method of any one of Embodiments 79-86, further comprising treatment with an effective amount of one or more antidepressants.
      • Embodiment 88 is the method of Embodiment 87, wherein the one or more antidepressants is a SSRI, SNRI, or combination thereof.
      • Embodiment 89 is the method of any one of Embodiments 79-88, wherein the pharmaceutical composition, the oral tablet, or the solid pharmaceutical composition comprising aticaprant is administered once daily.
      • Embodiment 90 is a method of treating major depressive disorder in a human patient, comprising administering a pharmaceutical composition comprising aticaprant and one or more pharmaceutically acceptable excipients to the human patient, wherein the patient had a previous inadequate response to other antidepressant therapy and wherein the pharmaceutical composition is administered orally once daily with or without food.
      • Embodiment 91 is the method of Embodiment 90, wherein the pharmaceutical composition is an oral tablet.
      • Embodiment 92 is the method of Embodiment 90 or 91, wherein the pharmaceutical composition comprises about 5 mg to 10 mg aticaprant, about 5 mg aticaprant, or about 10 mg aticaprant.
      • Embodiment 93 is the method of any one of Embodiments 90-92 wherein the other antidepressant therapy comprised one or more antidepressants.
      • Embodiment 94 is the method of Embodiment 93, wherein the one or more antidepressants comprised a SSRI, SNRI, or a combination thereof.
      • Embodiment 95 is the method of any one of Embodiments 90-94, wherein the aticaprant is S-aticaprant or the aticaprant is crystalline aticaprant.
      • Embodiment 96 is the method of any one of Embodiments 90-95, further comprising treatment with an effective amount of one or more antidepressants.
      • Embodiment 97 is the method of Embodiment 96, wherein the one or more antidepressants is a SSRI, SNRI, or combination thereof.
      • Embodiment 98 is the method of any one of Embodiments 90-97, wherein the patient has anhedonia, optionally moderate to severe anhedonia.
      • Embodiment 99 is the method of any one of Embodiments 90-98, wherein the pharmaceutical composition comprises one or more of: a filler, a disintegrant, a glidant, a lubricant, a binder, and a coloring agent.
      • Embodiment is 100 is the method of Embodiment 99, wherein the filler is selected from: microcrystalline cellulose, lactose monohydrate, and silicified microcrystalline cellulose; the disintegrant is croscarmellose sodium; the glidant is silica, colloidal anhydrous; and the lubricant is magnesium stearate.
      • Embodiment 101 is the method of any one of Embodiments 90-100, wherein the pharmaceutical composition comprises between about 0.1% and 90% aticaprant by weight.
      • Embodiment 102 is the method of any one of Embodiments 90-101, wherein the pharmaceutical composition comprises between about 10% and 99.9% filler by weight.
      • Embodiment 103 is the method of any one of Embodiments 90-102, wherein the pharmaceutical composition is a film coated oral tablet, comprising (i) a film coat and (ii) a core tablet, wherein the core tablet comprises about 5% aticaprant by weight, about 88.5% filler by weight, about 5% disintegrant by weight, about 1% glidant by weight, and about 0.5% lubricant by weight.
      • Embodiment 104 is the method of wherein the film coated oral tablet comprises about 97% core tablet by weight and about 3% film coat by weight.
      • Embodiment 105 is the method of any one of Embodiments 90-104, wherein the pharmaceutical composition is an oral tablet comprising about 10 mg aticaprant, wherein the oral tablet comprises a core tablet of about 200 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 60 mg microcrystalline cellulose, about 60 mg lactose monohydrate, about 5 mg croscarmellose sodium, and about 1 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 57 mg silicified microcrystalline cellulose, about 5 mg croscarmellose sodium, about 1 mg silica, colloidal anhydrous, and about 1 mg magnesium stearate.
  • The following Examples are set forth to aid in the understanding of the invention, and are not intended and should not be construed to limit in any way the invention set forth in the claims which follow thereafter.
  • Abbreviations
    ABV Alcohol-by-Volume
    AE Adverse Event
    ALT Alanine Aminotransferase
    Anti-HEV Anti-hepatitis E Virus (Immunoglobulin M)
    (IgM)
    ASEX Arizona Sexual Experiences Scale
    AST Aspartate Transaminase
    ATRQ Antidepressant Treatment History Questionnaire
    AV Atrioventricular
    BMI Body Mass Index
    CGI-S Clinical Global Impression - Severity
    CI Confidence Interval
    CPFQ Cognitive and Physical Functioning Questionnaire
    CSF Cerebrospinal Fluid
    C-SSRS Columbia Suicide Severity Rating Scale
    CYP cytochrome P450
    DSC Differential Scanning Calorimetry
    DSM Diagnostic and Statistical Manual of Mental
    Disorders
    ECG Electrocardiogram
    eITT Enriched Intent-To-Treat (population)
    FAS Full Safety Analysis Set
    fITT Full Intent-To-Treat (population)
    FSH Follicle Stimulating Hormone
    G17 Gastrin-17
    GI Gastrointestinal
    HAM-A | Hamilton Depression Rating Scale
    HDRS-17
    HCV Hepatitis C Virus
    HbsAg Hepatitis b Surface Antigen
    β-hCG β-human Chorionic Gonadotropin
    HAM-A6 6 Item Subscale from HAM-A
    HIV Human Immunodeficiency Virus
    HPA Hypothalamus Pituitary Adrenal
    Hp IgG Helicobacter IgG antibodies
    ICH International Conference on Harmonisation
    KOR Kappa Opioid Receptor
    KSS Karolinska Sleepiness Scale
    LBBB Left Bundle Branch Block
    LC-MS/MS Liquid Chromatography/Mass Spectrometry/Mass
    Spectrometry
    LOQ Limit of Quantification
    LS Least Squares
    LSD Lysergic Acid Diethylamide
    MADRS Montgomery Asberg Depression Rating Scale
    MDD Major Depressive Disorder
    mDSC Modulated Differential Scanning Calorimetry
    MedDRA Medical Dictionary for Regulatory Activities
    MINI Mini International Neuropsychiatric Interview
    MMRM Mixed-effects Model for Repeated Measures
    MOR Mu Opioid Receptor
    NSAID Nonsteroidal Anti-Inflammatory Drug
    PCP Phencyclidine
    PGI Pepsinogen I
    PGII Pepsinogen II
    PK Pharmacokinetic
    PPI Proton Pump Inhibitor
    PRO Patient Reported Outcome
    QD Once Daily
    RH Relative Humidity
    RT Toom Temperature
    SATE Self-Assessment of Treatment Experience
    SD Standard Deviation
    SHAPS Snaith-Hamilton Pleasure Scale
    SIGH-A Structured Interview Guide for the Hamilton
    Anxiety scale
    SIGMA The Structured Interview Guide for the MADRS
    SMDDS Symptoms of Major Depressive Disorder Scale
    SNRI Serotonin-Norepinephrine Reuptake Inhibitor
    SSRI Selective Serotonin Reuptake Inhibitor
    TEAE Treatment-Emergent Adverse Event
    THF Tetrahydrofuran
    TSH Thyroid-Stimulating Hormone
    ULN Upper Limit of Normal
    USP United States Pharmacopeia
    XRPD X-ray Powder Diffraction
    • Example 1: Instrument and Methodology Details
  • A. X-Ray Powder Diffraction (XRPD)
  • Bruker AXS D8 Advance
  • XRPD diffractograms were collected on a Bruker D8 diffractometer using Cu Kα radiation (40 kV, 40 mA) and a θ-2θ goniometer fitted with a Ge monochromator. The incident beam passes through a 2.0 mm divergence slit followed by a 0.2 mm anti-scatter slit and knife edge. The diffracted beam passes through an 8.0 mm receiving slit with 2.5° Soller slits followed by the Lynxeye Detector. The software used for data collection and analysis was Diffrac Plus XRD Commander and Diffrac Plus EVA respectively.
  • Samples were run under ambient conditions as flat plate specimens using powder as received. The sample was prepared on a polished, zero-background (510) silicon wafer by gently pressing onto the flat surface or packed into a cut cavity. The sample was rotated in its own plane.
  • The details of the standard Pharmorphix data collection method are:
      • Angular range: 2 to 42° 2θ
      • Step size: 0.05° 2θ
      • Collection time: 0.5 s/step (total collection time: 6.40 min)
  • When required other methods for data collection are used with details as shown in Table 7.
  • TABLE 7
    Additional D8 XRPD methods
    4 Minute Method
    Angular Range
    2 to 31° 2θ
    Step Size 0.06° 2θ
    Time per Step 0.5 s/step
  • PANalytical Empyrean
  • XRPD diffractograms were collected on a PANalytical Empyrean diffractometer using Cu Kα radiation (45 kV, 40 mA) in transmission geometry. A 0.5° slit, 4 mm mask and 0.04 rad Soller slits with a focusing mirror were used on the incident beam. A PIXcel3D detector, placed on the diffracted beam, was fitted with a receiving slit and 0.04 rad Soller slits. The software used for data collection was X'Pert Data Collector using X'Pert Operator Interface. The data were analyzed and presented using Diffrac Plus EVA or HighScore Plus.
  • Samples were prepared and analyzed in either a metal or Millipore 96 well-plate in transmission mode. X-ray transparent film was used between the metalsheets on the metal well-plate and powders (approximately 1-2 mg) were used as received. The Millipore plate was used to isolate and analyze solids from suspensions by adding a small amount of suspension directly to the plate before filtration under a light vacuum.
  • The scan mode for the metal plate used the gonio scan axis, whereas a 2θ scan was utilized for the Millipore plate.
  • The details of the standard screening data collection method are:
      • Angular range: 2.5 to 32.0° 2θ
      • Step size: 0.0130° 2θ
      • Collection time: 12.75 s/step (total collection time of 2.07 min)
  • The software used for data collection was X'Pert Data Collector and the data analyzed and presented using Diffrac Plus EVA.
  • B. Differential Scanning calorimetry (DSC)
  • TA Instruments Q2000
  • DSC data were collected on a TA Instruments Q2000 equipped with a 50 position auto-sampler. Typically, 0.5-3 mg of each sample, in a pin-holed aluminum pan, was heated at 10° C./min from 25° C. to 275° C. A purge of dry nitrogen at 50 mL/min was maintained over the sample.
  • Modulated temperature DSC was carried out using an underlying heating rate of 2° C./min and temperature modulation parameters of ±0.636° C. (amplitude) every 60 seconds.
  • The instrument control software was Advantage for Q Series and Thermal Advantage and the data were analyzed using Universal Analysis or TRIOS.
  • TA Instruments Discovery DSC
  • DSC data were collected on a TA Instruments Discovery DSC equipped with a 50 position auto-sampler. Typically, 0.5-3 mg of each sample, in a pin-holed aluminum pan, was heated at 10° C./min from 25° C. to 275° C. A purge of dry nitrogen at 50 mL/min was maintained over the sample.
  • The instrument control software was TRIOS and the data were analyzed using TRIOS or Universal Analysis.
  • C. Chemical Purity Determination by HPLC
  • Purity analysis was performed on an Agilent HP1100/Infinity II 1260 series system equipped with a diode array detector and using OpenLAB software. The full method details are provided in Table 8.
  • TABLE 8
    HPLC method for chemical purity determinations
    Parameter Value
    Type of method Reverse phase with gradient elution
    Sample Preparation 0.2 mg/ml in acetonitrile:water 1:1
    Column Supelco Ascentis Express C18 2.7 μm
    100 × 4.6 mm
    Column Temperature (° C.) 25
    Injection (μL) 5
    Detection: Wavelength, 255, 90
    Bandwidth (nm)
    Flow Rate (ml/min) 2
    Phase A 0.1% TFA in water
    Phase B 0.085% TFA in acetonitrile
    Time (min) % Phase A % Phase B
    Timetable
    0 95 5
    6 5 95
    6.2 95 5
    8 95 5
    • Example 2—Preparation of the Aticaprant THF Solvate
  • Figure US20230277500A1-20230907-C00004
  • Aqueous sodium hydroxide was added to compound 1 in 2-methyltetrahydrofuran. After phase separation, compound 2, i.e., the free base of compound 1, in 2-MeTHF was solvent switched to tetrahydrofuran (THF). Reductive amination of compound 3 using compound 2 was carried out by adding sodium triacetoxyborohydride and THF. Upon reaction completion, the reaction mixture was washed with saturated sodium bicarbonate and sodium chloride. The organic phase containing crude compound 4 was concentrated and ethanol and water were added. The product was crystallized using THF, ethanol, and water to produce compound 4 as a solid.
  • Charge 7.3 L/kg water into a reactor. Charge 6.6 L/kg 2-MeTHF into the reactor. Charge 1.15 mol/mol of compound 1 into the reactor. Dose 2.3 mol/mol 50% aq. NaOH into the reactor over a minimum 20 minutes at 22° C. while stirring. Rinse with 1.0 L/kg water into the reactor. Stir for minimum 30 minutes at 22° C. Settle for minimum 30 minutes. Separate and discard the lower aqueous layer. Concentrate under vacuum to minimal volume at maximum 45° C. Charge portions of THF to the reactor and distill back to minimal volume to complete the solvent switch. Adjust the reactor to 20° C. Charge 5.0 L/kg THF into the reactor. Charge 1.00 mole compound 3 into the reactor. Charge 10.0 L/kg THF into the reactor. Adjust R1 to 32° C. and stir for minimum 1 hour. Adjust the reactor to 15° C. Charge 1.50 mole/mole NaBH(OAc)3 in portions into the reactor at 15° C. Stir for minimum 1 hour at 15° C. Dose 5.0 L/kg water at 15° C. to the reactor. Dose 3.05 mole/mole 50% aq. NaOH at 15° C. to the reactor and stir for minimum 2 hours. Rinse with 0.5 L/kg water. Settle for minimum 30 minutes. Separate and discard the lower aqueous layer. Charge 6.2 L/kg 20% aq. NaCl at 15° C. to the reactor and stir for minimum 30 minutes. Settle for minimum 30 minutes. Separate and discard the lower aqueous layer. Concentrate under vacuum to 8.0 L/kg at maximum 45° C. Adjust the reactor to 25° C. Charge 8.0 L/kg EtOH (2% MeOH) and 8.0 L/kg water at 25° C. to the reactor. Dose 2.0 L/kg water at 25° C. over minimum 2.5 hours. Charge 0.03 kg/kg of crude compound 4 seeds to the reactor at 25° C. Stir for minimum 2 hours at 25° C. Charge 6.0 L/kg water at 25° C. to the reactor over minimum 7.5 hours. Cool to 2.5° C. over minimum 7 hours. Stir for minimum 6 hours at 2.5° C. Isolate the product and wash with THF/EtOH/water 1:1:2 (volume ratio). Dry the product at 25° C.
    • Example 3—Preparation of Pure Aticaprant
  • Figure US20230277500A1-20230907-C00005
  • Charge 1.0 mol of crude compound 4 into a dissolution reactor. Add 1.91 L/mol of 2-MeTHF. Add 2.39 L/mole n heptane. Stir the contents of the reactor. Adjust temperature to 42° C. and stir for minimum 10 minutes until full dissolution. Filter the solution over a polish filter into a crystallization reactor to remove insoluble matter that might be present. Rinse the polish filter. Stir for minimum 10 minutes at 40° C. Cool to 20° C. over minimum 1 hour. Stir for minimum 10 minutes at 20° C. Dose 1.23 L/mol n-heptane over a minimum 30 minutes at 20° C. Stir for a minimum 10 minutes at 20° C. Seed with 0.02 mole/mole JNJ 67953964 AAA at 20° C. Stir for a minimum 8 hours at 20° C. Dose 3.68 L/mol of n-heptane over a minimum 12 hours at 20° C. Stir for a minimum 2 hours at 20° C. Cool to 10° C. over a minimum 3 hours. Stir for a minimum 4 hours at 10° C. Isolate compound 5. Wash the wet cake with 2-MeTHF/n-heptane (25/75 w/w %). Dry compound 5 at 50° C.
  • Characterization was performed on compound 5 and the results are shown in Table 9.
  • TABLE 9
    Characterization data for Form III
    XRPD Crystalline
    HPLC Purity 99.3%
    DSC Endo. 121.0° C., 75 J/g.
    Degradation not observed
    TGA No weight loss observed before degradation.
    Degradation onset ~250° C.
    GVS 0.4% max uptake at 90% RH
    No hysteresis observed
    XRPD unchanged after GVS
  • Form III of aticaprant was found to be crystalline by XRPD. 1H NMR showed that the material was consistent with the proposed structure, with the presence of residual ethyl acetate. Ion chromatography showed that there were no cations/anions present, and HPLC showed 99.8% purity. The DSC (heating from 20 to 131° C. at 10° C./min) showed a peak temperature at 121° C. See, FIG. 3 .
    • Example 4—Tablets Containing Aticaprant
  • Tablets containing aticaprant were prepared according to the scheme in FIG. 24 containing the components in Table 10.
  • TABLE 10
    Qualitative and Quantitative Composition of the Aticaprant Tablet
    Quantity Quantity
    Component (mg/tablet) (mg/tablet)
    Intragranular Phase:
    Core Tablet:
    Intragranular Phase:
    Aticaprant (unmilled) or aticaprant 5.00 10.00
    microfinea (milled)
    Microcrystalline cellulose 30.00 60.00
    Lactose monohydrateb 30.00 60.00
    Croscarmellose sodium 2.50 5.00
    Silica, colloidal anhydrous 0.50 1.00
    Extragranular Phase:
    Silicified microcrystalline cellulose 28.50 57.00
    Croscarmellose sodium 2.50 5.00
    Silica, colloidal anhydrous 0.50 1.00
    Magnesium Stearatec 0.05 1.00
    Core Tablet Weight: 100.00 200.00
    Film Coat:
    Purified waterd 12.00d 24.00d
    Opadry II orange 3.00 6.00
    Total Weight: 103.00 206.00
    a“aticaprant microfine” is milled aticaprant (physically proceed in milling equipment).
    bFrom animal origin.
    cFrom vegetable source.
    dRemoved during processing.
  • Tablets were prepared according to the following:
      • 1. Mix the following, screened components in a blend using a suitable blender:
      • a. Aticaprant or aticaprant microfine
      • b. Microcrystalline cellulose
      • c. Silica, colloidal anhydrous
      • d. Lactose monohydrate
      • 2. Screen the blend using a suitable screen.
      • 3. Add the following screened components to the blend. Mix further using a suitable blender:
      • a. Microcrystalline cellulose
      • b. Lactose monohydrate
      • 4. Screen the blend using a suitable screen.
      • 5. Add the following screened components to the blend. Mix further using a suitable blender
      • a. Microcrystalline cellulose
      • b. Lactose monohydrate
      • 6. Screen the blend using a suitable screen.
      • 7. Add the following screened components to the blend. Mix further using a suitable blender:
      • Microcrystalline cellulose
      • Lactose monohydrate
      • Croscarmellose sodium
      • 8. Make a dry granulate by using a suitable compaction technique.
      • 9. Add the following screened components to the dry granulate and mix using a suitable blender:
      • a. Silicified microcrystalline cellulose
      • b. Croscarmellose sodium
      • c. Silica, colloidal anhydrous
      • 10. Add the following screened component to the blend and mix using a suitable blender
      • a. Magnesium stearate
      • 11. Compress the blend into core tablets using a suitable tablet press.
      • 12. Suspend the coating powder in purified water using a suitable vessel.
      • 13. Spray the coating suspension on the core tablets using a suitable coater.
      • 14. Collect the film-coated tablets and package them in a suitable container.
    Example 5—Testing of Tablets Containing Aticaprant
  • The tablets of Example 3 are tested to determine dissolution properties and chemical stability. See, Table 11 for dissolution conditions and Tables 12-13 for results.
  • TABLE 11
    Dissolution Operating Conditions
    Parameter Conditions
    Apparatus Paddle (USP Type 2, Ph. Eur., JP).
    Dissolution Medium 0.01M hydrochloric acid
    Volume
    900 mL
    Temperature 37 ± 0.5° C.
    Rotation Speed
    50 rpm
    Analytical Finish UHPLC with UV detection at 247 nm
  • TABLE 12
    Criteria
    Characteristic Acceptance Result
    Specificity No interference with the peak of active or No inter-
    % dissolution of 100% placebo ≤2% ference
    Accuracy Recovery at the 20% concentration level of 100%
    lowest dosage strength
    20% ≤ X ≤ 50% = 75-125%
    Recovery at the 100% concentration level 102%
    of lowest dosage strength ≥50% = 95-105%
    Recovery at the 100% concentration level 101%
    of highest dosage strength ≥50% = 95-105%
    Recovery at the 120% concentration level 101%
    of lowest dosage strength ≥50% = 95-105%
    Precision - % RSD of 5 injections of the same  0.3%
    System reference solution ≤2.0%
    Repeatability
    Linearity % RSD of response factors ≤4%  0.8%
    Correlation coefficient (R) ≥0.995 1.00
    Range Linearity, accuracy, and precision criteria Pass
    are fulfilled for the 20-120% range
    Filtration Difference between % dissolution of  1%
    recovery filtered and unfiltered solution  0%
    (Whatman must be ≤2% for each of the 3 tested  1%
    Spartan RC individual filters
    0.45 μm
    30 mm)
    Solution Concentration of active is within the range
    Stability 97-103% of the initial value
    Stock solutions stored in clear volumetric 101%
    flasks at ambient conditions, 8 days
    Reference solutions stored in clear 100%
    volumetric flasks in the refrigerator, 8
    days/hours
    Reference solutions stored in clear 101%
    volumetric flasks at ambient conditions, 8
    days
    Sample solutions stored in clear 100%
    unpierced pre-slit vials in the refrigerator,
    7 days/hours
    Sample solutions stored in clear 101%
    unpierced pre-slit vials at ambient
    conditions, 7 days
    System % RSD ≤2.0% Pass
    Suitability Recovery reference 1 = 97.0-103.0% Pass
    Recovery reference 2 = 98.0-102.0% Pass
  • TABLE 13
    Dissolution (%) of Aticaprant Tablets
    Tablet
    1 Tablet 2 Tablet 3 Tablet 4 Tablet 5 Tablet 6
    98 97 100 98 98 95
  • The chemical stability of the tablets is evaluated over a 28-day period using a Risk Based Predictive Stability (RiBPS) study. The stability protocols for the studies are provided in Tables 14-15.
  • TABLE 14
    Storage Conditions and Testing Frequency for the Accelerated Stability Study
    40° C./ 50° C./ 60° C./ 60° C./ 60° C./ 70° C./ 70° C./ 70° C./ 80° C./
    Storage 75% 30% 10% 50% 75% 30% 50% 75% 10%
    Time RH RH RH RH RH RH RH RH RH
    3 days A A A A A A
    7 days A A A A A A A A
    14 days A A A A A A A
    21 days A A A A A A
    28 days Ab A A A A
    aduplicates; btriplicates; —: Not Tested; A = Assay and chromatographic purity
  • TABLE 15
    Storage Conditions and Testing Frequency for the Accelerated Stability
    Study
    50° C./ 50° C./ 60° C./ 60° C./ 70° C./ 70° C./ 80° C./ 80° C./
    Storage 10% 30% 10% 50% 30% 50% 10% 50%
    Time
    5° C. RH RH RH RH RH RH RH RH
    3 days A A A A A
    7 days A A A A A A A A
    14 days A A A A A A
    21 days Ab A A A A A
    aduplicates; btriplicates; —: Not Tested; A = Assay and chromatographic purity
  • The ICH stability protocol for is presented in Table 16.
  • TABLE 16
    Storage Conditions and Testing Frequency for Stability Study
    Accelerated/Stress Conditions
    ICH
    Long Term Storage Conditions Lightb
    Storage 25° C./ 30° C./ 40° C./ Protected
    Time 60% 75% 75% ICH Lightb (Primary
    (months) 5° C. RH RH RH 50° C. Unprotected pack)
    Initial A A (A)
     3 A (A) A A A
     6 (A) A A
     9 (A) A
    12 (A) A A
    18 (A) A
    24 (A) A A
    36 (A) A A
    bLight ICH: CIE85-ID65, integrated near UV energy not less than 200 W*h/m2, overall illumination not less than 1200 klux*h.
    Tests performed: A = Appearance, assay, chromatographic purity, and dissolution; —: Not tested; Tests given in brackets are kept in reserve and are activated if stability information becomes relevant or if problems arise at the active time points.
  • During the RiBPS study, 3 main degradation products (RRT 0.399, RRT 0.466, and RRT 0.874) showed an increasing trend over the storage period. Levels of degradation ranged from 0.06% to 0.98% for RRT 0.399, from <0.05% to 0.39% for RRT 0.466, and from <0.05 to 0.99% for RRT 0.874.
  • The results of the RiBPS study showed that degradant RRT 0.466 is the shelf-life limiting attribute for the drug product.
  • The results demonstrated that for the drug product stored in open dish the probability to pass 12 months is 99% for the specification limit of 0.30% when stored at 25° C./60% RH and 30° C./75% RH.
    • Example 6
  • This was a multi-center, placebo-controlled, randomized, double-blind study in subjects with MDD who have had an inadequate response to SSRI/SNRT treatment. Aticaprant was evaluated as an adjunctive therapy; therefore, eligible subjects were maintained on their SSRI/SNRI treatment without change throughout the study. At least 50% of recruited subjects had to be anhedonic (as measured by SHAPS total score ≥20).
  • A. Objectives
  • The primary objective was to evaluate the efficacy of aticaprant compared to placebo when administered as adjunctive treatment in subjects with MDD partially responsive to SSRI/SNRI treatment in terms of reduction of symptoms of depression, as assessed by the change from baseline on the MADRS in non-responders during the placebo lead-in period.
  • The secondary objectives are:
      • i. To evaluate the efficacy of aticaprant compared to placebo when administered as adjunctive treatment in subjects with MDD partially responsive to SSRI/SNRT treatment in terms of reduction of symptoms of depression, as assessed by the change from baseline on the MADRS in both responders and non-responders during the placebo lead-in period.
      • ii. To investigate the overall safety and tolerability of treatment with adjunctive aticaprant in subjects with MDD when used in combination with a SSRI or SNRI.
      • iii. To investigate the effect of aticaprant versus placebo on depression related anhedonia as assessed by the SHAPS.
      • iv. To investigate the effect of aticaprant on symptoms of depression using the Clinical Global Impression-Severity (CGI-S), the patient reported Symptoms of Major Depressive Disorder Scale (SMDDS) and the self-assessment of treatment experience (SATE).
      • v. To investigate the effect of aticaprant on symptoms of anxiety using the HAM-A and on core symptoms of anxiety using the HAM-A6 subscale.
      • vi. To assess the plasma PK of aticaprant in subjects with MDD and explore its relationship with efficacy and safety parameters.
  • Secondary exploratory objectives include:
      • i. To explore the effect of aticaprant on aspects of cognitive and executive function using the CPFQ.
      • ii. To explore mood-related biomarkers (including but not limited to growth factors, HPA axis markers, immune system activation, metabolic markers) and genetic/epigenetic variation that may be related to clinical response, nonresponse, or safety and tolerability parameters of aticaprant.
  • B. Study Design
  • For each subject, the study consisted of two phases: a screening phase of up to 5 weeks and a double-blind treatment phase lasting 11 weeks. See, FIG. 4 .
  • Subjects with MDD who have had treatment initiated with a permitted SSRI/SNRI and have had an inadequate or only partial response to this treatment were screened. Assessments include the MINI, Antidepressant Treatment History Questionnaire (TRQ), and MADRS.
  • The treatment phase consisted of 3 periods. A placebo lead-in period of concealed duration, after which subjects entered the double-blind treatment period when they were randomly assigned to 10 mg aticaprant (two 5 mg capsules) or continue placebo for 6 weeks. Each capsule contained aticaprant (5 mg), microcrystalline cellulose (94.95 mg), and magnesium stearate (0.05 mg) in a hard gelatin capsule. Subjects who completed the treatment period, entered the withdrawal period and were treated with placebo for the remaining time of the treatment phase. The total duration for each subject was approximately 16 weeks. There were 11 scheduled visits, including screening. An overall flow diagram is shown in FIG. 4 .
  • Subjects were screened within 35 to 2 days prior to Day 1 to ascertain their eligibility per the inclusion and exclusion criteria. The symptoms of depression were assessed using the structured interview guide for the MADRS.
  • Double-Blind Treatment Phase
  • The duration of the double-blind treatment phase was 11 weeks divided into 3 periods. The subject received medication after completion of the visit on Day 1. The first dose was taken at home on Day 2. All medication was taken in fasting condition. At Visits 3, 4 and 5, the subjects were re-randomized to blind subjects the duration of the placebo lead-in period. During the double-blind phase, the subjects visited the center for out-patient visits every 1 to 2 weeks. See, Table 17.
  • TABLE 17
    Time and Events Schedule
    Phase Screening aDouble-blind treatment phase
    Visit number 1 2 3 4 5 6 7 8 9 10 b11 or EW
    Week (end of) −5 to 0 0 1 2 3 4 6 7 8 9 11
    Day −35 to −2 1 8 15 22 29 43 50 57 64 78
    Safety assessments
    Physical and X X X X
    neurological
    examination
    ASEX X X X X X X
    KSS X X X X X X
    Suicidality by C-SSRS X X X X X X X X X X X
    Dosing
    Randomization X X X X
    Supply new medication X X X X X X X X X
    Oral dose medicationd Day 2 until and including Day 78e
    Meal after dosing Xl Xl Xl Xl Xl Xl Xl Xl Xl Xl
    Clinical Assessments
    Structured Interview Xj X X X X X X X X X X
    Guide MADRS
    Structured Interview X X X X X X X X X X
    Guide SIGH-A
    CGI-S X X X X X X X X X X
    SMDDS X X X X X
    CPFQ X X X X X
    SHAPS X X X X X X X X X X X
    SATEk once weekly while at home
    Ongoing subject review
    Assessment of subject X up to 3 occasion when at home
    engagementk
    Adverse events Continuous
    Concomitant medication Continuous
    EW = early withdrawal;
    aVisits should be conducted ± 3 days of the scheduled day (based on Visit 2, not based on previous visit).
    bIf a subject discontinues treatment before the end of the double-blind treatment phase, EW visit should be completed.
    dAt home: In fasting condition. At clinic visit days: Use blisters dispensed at the previous visit. In fasting condition after completion of predose assessments.
    eWhen Visit 11 is planned up to 3 days later, continue medication.
    jDuring the first screening visit and by telephone up to 4 days before Visit 2, if 2 weeks or more elapse between the MADRS rating at screening and Visit 2.
    kUsing Q1.6-app on subjects' smartphone.
    lBreakfast, lunch or dinner after drug intake at site.
  • Lead-in period: Subjects who successfully complete the baseline examination visit at the clinical site/unit, were treated with placebo for the entire duration of the lead-in period.
  • Treatment period: At the end of the lead-in period both placebo lead-in responders and placebo lead-in non-responders were randomized to receive either placebo or 10 mg aticaprant in a 1:1 ratio for 6 weeks. Subjects remained blinded to exact timing of the randomization, response criterion and drug treatment assignment for each subject.
  • Withdrawal period: Subjects who completed the double-blind treatment period prior to the end of Week 11 entered the withdrawal period where they were treated with placebo for the remaining time of the treatment phase.
  • C. Dosage and Administration
  • Aticaprant was supplied as 5-mg capsules. Placebo was supplied as matching capsules. All subjects took 2 capsules QD. The capsules were taken daily from Day 2 to Day 78 in fasting condition with some water (fasting for at least 4 hours before dosing). Medication was taken before breakfast. If the subject has forgotten to take the medication before breakfast, this was done before the next following meal, at the latest at dinner of the same day. If the subject remembered later than dinner, the dose of that day was omitted, and the subject took the dose before breakfast on the next day.
  • When Visit 11 was planned up to 3 days later, the subject continued medication until Visit 11.
  • The capsules were swallowed whole and not chewed, divided, dissolved or crushed. After having taken the medication, subjects did not to eat or drink for at least 30 minutes.
  • The first dose was taken in fasting condition on Day 2 of the double-blind phase. The dose of the medication was:
      • 10 mg aticaprant: 2 capsules of 5 mg aticaprant
      • Placebo: 2 placebo capsules.
  • Medication dose was adjusted as needed to 5 mg QD based on the results of a blinded review of the safety data. When a dose reduction has been decided on, this only applied to new subjects and the dose of medication was:
      • 5 mg aticaprant: 1 capsule of 5 mg aticaprant
      • Placebo: 1 placebo capsule.
  • As used herein, the Enriched ITT Analysis Set (eITT) is defined as all enrolled lead-in placebo non-responders who were randomized into a treatment period, received at least one dose of study medication in the treatment period and have at least one post-baseline MADRS assessment during the treatment period. Similarly, the Full ITT Analysis Set (fITT) is defined as all enrolled subjects who were randomized into a treatment period, received at least one dose of study medication in the treatment period and have at least one post-treatment baseline assessment of MADRS during the treatment period.
  • D. Clinical Assessments
      • (i) Depression: Montgomery-Åsberg Depression Rating Scale (MADRS), Clinical Global Impression—Severity (CGI-S), Symptoms of Major Depressive Disorder Scale (SMDDS), and Self-assessment of treatment experience (SATE)
      • (ii) Anhedonia: Snaith-Hamilton Pleasure Scale (SHAPS)
      • (iii) Anxiety: Structured Interview Guide for the Hamilton Anxiety scale (SIGH-A) and HAM-A6
      • (iv) Effects on Cognition: The Cognitive and Physical Functioning Questionnaire (CPFQ)
      • (v) Safety assessments
  • Standard safety assessments including physical and neurological examination, vital signs, 12-lead ECG, clinical chemistry, hematology, and urinalysis was performed. Based on observations of GI complaints in previous studies, a panel including PGI, PGII, G17 and Hp IgG was added to the clinical laboratory test panel to test for stomach mucosa status.
      • (vi) Suicidal ideation: C-SSRS
      • (vii) Exploratory: CPFQ
      • (viii) Central sedating effects: Karolinska Sleepiness Scale
      • (ix) Sexual dysfunction: ASEX
  • E. Patient Population
  • Of 184 subjects, 169 were randomized into the treatment period and included in the safety population, while 166 subjects were considered for the full ITT population. Out of the 166 subjects in the full ITT population, 121 (73%) were lead-in placebo non-responders (enriched ITT population) and the remaining 45 (27%) were lead-in placebo responders. Of the 121 subjects in the enriched population, 112 (92.6%) were white and 84 (69.4%) were female. The mean age was 41.6 years, ranging from 19 to 64 years. All subjects had anhedonia (defined as SHAPS total score ≥20) at treatment baseline. A high anhedonia level (defined as SHAPS total score ≥38) was observed in 43.8% of the subjects. In general, the treatment groups were similar with respect to the baseline characteristics. Subject demographics for the eITT and safety analysis are provided in Tables 18 and 19.
  • TABLE 18
    Summary of Demographics and Baseline
    Characteristics; Full Safety Analysis
    aticaprant
    Placebo 10 mg Total
    (N = 84) (N = 85) (N = 169)
    Age (Years)
    N 84 85 169
    Mean (SD) 42.1 (12.54) 43.0 (12.81) 42.6 (12.65)
    Median 43.5 43.0 43.0
    Range (19; 64) (21; 64) (19; 64)
    Gender
    N 84 85 169
    Female 62 (73.8%) 60 (70.6%) 122 (72.2%)
    Male 22 (26.2%) 25 (29.4%) 47 (27.8%)
    Race
    N 84 85 169
    American Indian 1 (1.2%) 0 1 (0.6%)
    or Alaska Native
    Asian 2 (2.4%) 2 (2.4%) 4 (2.4%)
    Black or 2 (2.4%) 5 (5.9%) 7 (4.1%)
    African American
    White 79 (94.0%) 78 (91.8%) 157 (92.9%)
    Ethnicity
    N 84 85 169
    Hispanic or 10 (11.9%) 13 (15.3%) 23 (13.6%)
    Latino
    Not Hispanic 74 (88.1%) 72 (84.7%) 146 (86.4%)
    or Latino
    Country
    N 84 85 169
    Germany 4 (4.8%) 5 (5.9%) 9 (5.3%)
    Moldova 15 (17.9%) 14 (16.5%) 29 (17.2%)
    Russia 25 (29.8%) 21 (24.7%) 46 (27.2%)
    Ukraine 9 (10.7%) 7 (8.2%) 16 (9.5%)
    United Kingdom 10 (11.9%) 15 (17.6%) 25 (14.8%)
    United States 21 (25.0%) 23 (27.1%) 44 (26.0%)
    Baseline Height (cm)
    N 84 85 169
    Mean (SD) 167.4 (7.91) 168.2 (8.64) 167.8 (8.27)
    Median 167.5 167.6 167.6
    Range (150; 183) (152; 195) (150; 195)
    Baseline Weight (kg)
    N 84 85 169
    Mean (SD) 76.2 (14.73) 78.7 (15.23) 77.4 (14.99)
    Median 75.3 78.9 77.1
    Range  (47; 116)  (42; 119)  (42; 119)
    Baseline BMI (kg/m2)
    N 84 85 169
    Mean (SD) 27.2 (4.92) 27.7 (4.56) 27.5 (4.73)
    Median 26.6 28.1 27.6
    Range (19; 35) (18; 35) (18; 35)
    Presence of Anhedonia at Baseline
    N 84 85 169
    No 0 1 (1.2%) 1 (0.6%)
    Yes 84 (100.0%) 84 (98.8%) 168 (99.4%)
    Lead-in response status
    N 84 85 169
    No 62 (73.8%) 62 (72.9%) 124 (73.4%)
    Yes 22 (26.2%) 23 (27.1%) 45 (26.6%)
  • TABLE 19
    Summary of Demographics and Baseline Characteristics; eITT
    aticaprant
    Placebo 10 mg Total
    (N = 61) (N = 60) (N = 121)
    Age (Years)
    N 61 60 121
    Mean (SD) 41.6 (12.34) 41.6 (12.78) 41.6 (12.51)
    Median 43.0 40.5 42.0
    Range (19; 64) (21; 64) (19; 64)
    Gender
    N 61 60 121
    Female 42 (68.9%) 42 (70.0%) 84 (69.4%)
    Male 19 (31.1%) 18 (30.0%) 37 (30.6%)
    Race
    N 61 60 12
    Indian or 1 (1.6%) 0 1 (0.8%)
    Alaska Native
    Asian 2 (3.3%) 1 (1.7%) 3 (2.5%)
    Black or 2 (3.3%) 3 (5.0%) 5 (4.1%)
    African
    American
    White 56 (91.8%) 56 (93.3%) 112 (92.6%)
    Ethnicity
    N 61 60 121
    Hispanic or 3 (4.9%) 7 (11.7%) 10 (8.3%)
    Latino
    Not Hispanic 58 (95.1%) 53 (88.3%) 111 (91.7%)
    or Latino
    Country
    N 61 60 121
    Germany 4 (6.6%) 4 (6.7%) 8 (6.6%)
    Moldova 15 (24.6%) 14 (23.3%) 29 (24.0%)
    Russia 19 (31.1%) 18 (30.0%) 37 (30.6%)
    Ukraine 7 (11.5%) 5 (8.3%) 12 (9.9%)
    United 6 (9.8%) 10 (16.7%) 16 (13.2%)
    Kingdom
    United 10 (16.4%) 9 (15.0%) 19 (15.7%)
    States
    Baseline Height (cm)
    N 61 60 121
    Mean (SD) 168.1 (8.19) 167.3 (8.10) 167.7 (8.13)
    Median 168.0 166.3 167.0
    Range (151; 183) (152; 186) (151; 186)
    Baseline Weight (kg)
    N 61 60 121
    Mean (SD) 74.7 (14.19) 76.8 (15.12) 75.7 (14.63)
    Median 74.2 77.1 75.6
    Range  (47; 116)  (42; 119)  (42; 119)
    Baseline BMI (kg/m2)
    N 61 60 121
    Mean (SD) 26.4 (4.67) 27.3 (4.36) 26.9 (4.52)
    Median 25.7 27.8 26.7
    Range (19; 35) (18; 35) (18; 35)
    Presence of Anhedonia at Baseline
    N 61 60 121
    No 0 0 0
    Yes 61 (100.0%) 60 (100.0%) 121 (100.0%)
    Lead-in response status
    N 61 60 121
    No 61 (100.0%) 60 (100.0%) 121 (100.0%)
    Yes 0 0 0
  • E. Evaluations of Efficacy
  • At the end of the lead-in period, response status of the subjects was assessed according to the double-blind response criteria based on reduction in MADRS relative to lead-in baseline. Both lead-in placebo responders and lead-in placebo non-responders were randomly assigned in a 1:1 ratio to either aticaprant or placebo in the treatment period. The randomization was stratified by lead-in response status (non-responders: <30% reduction from baseline in MADRS total score at the end of the lead-in period vs responders: ≥30% reduction from baseline at the end of the lead-in period) and presence/absence of anhedonia (presence defined as SHAPS total score ≥20).
  • Treatment duration: The study consisted of two periods: a screening phase of up to 5 weeks and a double-blind treatment phase of 11 weeks. The double-blind treatment phase of the trial consisted of 3 periods. The first period was a placebo lead-in of 3 weeks, after which subjects entered the treatment period when they were randomly assigned to aticaprant or continuation on placebo for 6 weeks. Subjects who successfully completed the treatment period were treated with placebo during a 2-week withdrawal period, i.e., Period 3. The total duration for each subject was approximately 16 weeks.
  • Primary analysis set for efficacy: The efficacy analysis is based on the eITT set defined as all enrolled lead-in placebo non-responders who were randomized into the treatment period, received at least one dose of medication, and have at least one post-baseline MADRS assessment during the treatment period. The primary analysis set is used for all efficacy endpoints.
  • Secondary analysis set for efficacy: A secondary analysis set is the fITT set defined as all enrolled subjects who were randomized into the treatment period, received at least one dose of medication, and have at least one post-baseline MADRS assessment during the treatment period. The secondary analysis set is used for all efficacy endpoints to examine the effect in the general population, which may be useful for designing subsequent studies in the development program.
  • Analysis set for safety: The safety analysis is based on the full safety analysis set, defined as all enrolled subjects who received at least one dose of medication in the treatment period.
  • The efficacy endpoints were presented for both the eITT and the fITT.
  • Level of significance: The analysis of primary efficacy endpoint was performed at a significance level of 0.20 (one-sided). The analysis of secondary efficacy endpoints was performed at a significance level of 0.20 (two-sided). No adjustment for multiple comparisons was performed.
  • F. Results
  • (i) Primary Endpoint: Change from Treatment Baseline in MADRS Total Score at Treatment Week 6 in Non-Responders during Placebo Lead-in Period
  • Enriched ITT Analysis Set
  • The mean (SD) MADRS total score at treatment baseline was 29.0 (4.61), ranging from 19 to 41. See, FIG. 5 . The mean change from treatment baseline (SD) in MADRS total score at treatment week 6 was −10.2 (8.44) for aticaprant and −8.2 (8.53) for placebo. The observed effect size was 0.23. See, Tables 20-22 and FIG. 8 .
  • TABLE 20
    Summary of Baseline Psychiatry Rating Scales at the Start of the Lead-in
    and Treatment Periods; eITT Analysis Set
    MADRS SHAPS
    Total Score Total Score
    Mean Median Mean Median
    N (SD) (Range) N (SD) (Range)
    Lead-in Baseline
    Placebo
     61 33.4 (4.25) 34.0 (26; 42)  61 38.0 (6.28) 38.0 (22; 55)
    Aticaprant  60 32.5 (4.18) 32.0 (25; 45)  60 38.3 (5.66) 38.0 (21; 53)
    Total 121 32.9 (4.22) 33.0 (25; 45) 121 38.1 (5.96) 38.0 (21; 55)
    Treatment Baseline
    Placebo
     61 29.2 (5.47) 29.0 (19; 41)  61 36.8 (5.75) 37.0 (23; 50)
    Aticaprant  60 28.7 (3.58) 28.5 (21; 36)  60 36.4 (5.16) 36.5 (20; 49)
    Total 121 29.0 (4.61) 29.0 (19; 41) 121 36.6 (5.45) 37.0 (20; 50)
  • TABLE 21
    MADRS Total Score: Mean Changes to Placebo
    During the Treatment Period; eITT Analysis Set
    Mean 90% CI
    Analysis Mean Change to for Mean
    Visit Change from Placebo Change to Effect
    Treatment N Baseline (SD) (SD pooled) Placebo Size
    Treatment Week
    1
    Placebo 61 −2.2 (3.73)
    Aticaprant 60 −3.3 (5.21) −1.1 (4.52) [−2.4, 0.3] −0.24
    Treatment Week 3
    Placebo 59 −4.3 (5.99)
    Aticaprant 59 −5.7 (6.38) −1.4 (6.18) [−3.3, 0.5] −0.22
    Treatment Week 4
    Placebo 60 −6.4 (6.66)
    Aticaprant 57 −7.3 (7.35) −0.9 (7.00) [−3.1, 1.2] −0.14
    Treatment Week 5
    Placebo 60 −7.4 (7.15)
    Aticaprant 55 −8.4 (7.36) −1.1 (7.25) [−3.3, 1.2] −0.14
    Treatment Week 6
    Placebo 59 −8.2 (8.53)
    Aticaprant 59 −10.2 (8.44)  −2.0 (8.49) [−4.6, 0.6] −0.23
    Negative change from baseline indicates improvement. Negative change to Placebo indicates favorable aticaprant effect. Negative effect size favors aticaprant; positive effect size favors Placebo.
  • TABLE 22
    MADRS Total Score: MMRM Results - Estimated LS Means and
    Comparison versus Placebo; eITT Analysis Set
    LSMean
    Difference 60%
    Analysis (SE)\ Confidence
    Visit Mean Mean LSMean Treatment Interval on p-
    Treatment N (SD) (SD) (SE) Placebo Difference valueª
    Treatment Week 1
    Placebo 61 26.9 −2.2 −2.0
    (6.77) (3.73) (0.92)
    aticaprant 60 25.4 −3.3 −3.2 −1.2 (1.24) [−2.28, 0.1604
    (5.93) (5.21) (0.93) −0.19]
    Treatment Week 3
    Placebo 59 24.8 −4.3 −4.2
    (8.25) (5.99) (0.92)
    aticaprant 59 23.1 −5.7 −5.6 −1.5 (1.25) [−2.55, 0.1159
    (6.58) (6.38) (0.93) −0.44]
    Treatment Week 4
    Placebo 60 22.7 −6.4 −6.2
    (9.10) (6.66) (0.92)
    aticaprant 57 21.5 −7.3 −7.3 −1.1 (1.25) [−2.19, 0.1811
    (7.49) (7.35) (0.93) −0.09]
    Treatment Week 5
    Placebo 60 21.7 −7.4 −7.2
    (9.54) (7.15) (0.92)
    aticaprant 55 20.5 −8.4 −8.7 −1.5 (1.25) [−2.60, 0.1103
    (7.44) (7.36) (0.94) −0.48]
    Treatment Week 6
    Placebo 59 20.9 −8.2 −8.0
    (10.54) (8.53) (0.92)
    aticaprant 59 18.6 −10.2 −10.1 −2.1 (1.25) [−3.20, 0.0443
    (8.14) (8.44) (0.93) −1.09|
    aOne-sided test for no difference between treatments from a MMRM model with subject as random effect; country, treatment, time and time-by-treatment interaction as factors; and baseline MADRS total score as continuous covariate. An AR(1) variance-covariance matrix was employed
  • Based on the results of a MMRM model with subject as random effect;
      • country, treatment, time and time-by-treatment interaction as factors; and baseline MADRS total score as continuous covariate a significant positive efficacy signal was detected for aticaprant versus placebo at the one-sided 0.20 significance level. The estimated LS mean difference at treatment week 6 between aticaprant and placebo was −2.1 with 80% 1-sided CI upper limit of −1.09. The corresponding p-value was 0.044. The treatment effect was larger in the fITT than in the eITT population: −3.1 with 80% 1-sided CI upper limit of −2.2 (p=0.002). The effect size was 0.36 and 0.23, respectively. See, FIGS. 2 and 3 .
  • Full ITT Analysis Set
  • The mean (SD) baseline MADRS total score at treatment baseline was 25.3 (7.86), ranging from 0 to 41. See, FIGS. 7A and 7B. The mean changes from treatment baseline in MADRS total score at Treatment Week 6 for fITT were smaller than for eITT: −9.7 (8.02) for aticaprant and −6.6 (8.57) for placebo. The observed effect size was 0.36. These results illustrate a statistical superiority over placebo with a durability of effect with the greatest difference seen at week 6. See, Table 23.
  • TABLE 23
    Summary of Baseline Psychiatry Rating Scales at the Start of the Lead-in
    and Treatment Periods; fITT Analysis Set
    MADRS SHAPS
    Total Score Total Score
    Mean Median Mean Median
    N (SD) (Range) N (SD) (Range)
    Lead-in Baseline
    Placebo
    83 32.8 (4.25) 33.0 (26; 42) 83 37.8 (6.01) 38.0 (22; 55)
    Aticaprant 83 32.4 (4.27) 32.0 (21; 45) 83 37.3 (6.23) 38.0 (14; 53)
    Total 166 32.6 (4.25) 32.0 (21; 45) 166 37.6 (6.11) 38.0 (14; 55)
    Treatment Baseline
    Placebo
    83 25.7 (7.73) 26.0 (10; 41) 83 36.3 (5.44) 36.0 (23; 50)
    Aticaprant 83 24.8 (8.02) 27.0 (0; 36) 83 35.0 (5.85) 36.0 (14; 49)
    Total 166 25.3 (7.86) 26.5 (0; 41) 166 35.6 (5.67) 36.0 (14; 50)
  • Significant effect for aticaprant versus placebo in fITT population was also detected. The estimated LS mean difference at treatment week 6 between aticaprant and placebo was −3.1 with 80% 1-sided CI upper limit of −2.21. The corresponding p-value was 0.002. See, Tables 24-25 and FIG. 6 .
  • TABLE 24
    MADRS Total Score: MMRM Results - Estimated LS Means and
    Comparison versus Placebo; fITT Analysis Set
    Change from Baseline
    LSMean
    Difference 60%
    Analysis (SE)\ Confidence
    Visit Mean Mean LSMean Treatment Interval on p-
    Treatment N (SD) (SD) (SE) Placebo Difference valuea
    Treatment Week 1
    Placebo 83 24.0 −1.8 −1.7
    (8.12) (4.00) (0.78)
    aticaprant 83 21.7 −3.1 −3.2 −1.6 (1.03) [−2.44, 0.0653
    (8.78) (4.81) (0.77) −0.70]
    Treatment Week 3
    Placebo 81 22.2 −3.4 −3.4
    (9.28) (6.50) (0.78)
    aticaprant 80 20.0 −5.1 −5.2 −1.9 (1.04) [−2.74, 0.0368
    (8.53) (6.74) (0.78) −0.99]
    Treatment Week 4
    Placebo 82 20.8 −4.9 −4.8
    (9.24) (7.02) (0.78)
    aticaprant 78 17.9 −7.2 −7.3 −2.5 (1.04) [−3.34, 0.0093
    (9.32) (7.02) (0.78) −1.59]
    Treatment Week 5
    Placebo 82 19.2 −6.4 −6.3
    (9.89) (7.16) (0.78)
    aticaprant 76 16.7 −8.3 −8.7 −2.4 (1.05) [−3.24, 0.0125
    (9.47) (7.48) (0.78) −1.47]
    Treatment Week 6
    Placebo 81 19.0 −6.6 −6.5
    (10.35) (8.57) (0.78)
    aticaprant 77 15.9 −9.7 −9.6 −3.1 (1.05) [−3.97, 0.0017
    (9.09) (8.02) (0.79) −2.21]
    aOne-sided test for no difference between treatments from a MMRM model with subject as random effect; country, treatment, time and time-by-treatment interaction as factors; and baseline MADRS total score as continuous covariate. An AR(1) variance-covariance matrix was employed
  • TABLE 25
    MADRS (Montgomery-Åsberg Depression Rating Scale) Total Score: Mean
    Changes to Placebo During the Treatment Period; fITT Analysis Set
    90%
    Mean CI for
    Change to Mean
    Analysis Visit Placebo Change to Effect
    Treatment N (SD pooled) Placebo Size
    Treatment Week
    1
    Placebo 83
    Aticaprant 83 −1.3 (4.43) [−2.4, −0.2] −0.29
    Treatment Week 3
    Placebo 81
    Aticaprant 80 −1.7 (6.62) [−3.4, 0.0]  −0.26
    Treatment Week 4
    Placebo 82
    Aticaprant 78 −2.3 (7.02) [−4.1, −0.4] −0.32
    Treatment Week 5
    Placebo 82
    Aticaprant 76 −1.9 (7.31) [−3.9, −0.0] −0.26
    Treatment Week 6
    Placebo 81
    Aticaprant change from 77 −3.0 (8.31) [−5.2, −0.8] −0.36
    Negative change from baseline indicates improvement. Negative change to Placebo indicates favorable aticaprant effect. Negative effect size favors aticaprant; positive effect size favors Placebo.
  • COVID-19 Impact on Primary Efficacy Assessment
  • Supplementary analysis was conducted using the same MMRM model as described for the primary analysis on all the data collected prior to 15 Mar. 2020 (estimated date of the COVID-19 lockdowns in most of the countries participating in the trial). Seventeen percent of the subjects in fITT and 19% in eITT population had at least one of the MADRS assessment excluded from the model due to COVID-19 impact. Results of the analysis corroborated the findings of the primary efficacy analysis in both: eITT and fITT populations. LSMeans difference estimate was −3.0 (80% 1-sided CI upper limit of −1.88) for eITT and −3.4 (80% 1-sided CI upper limit of −2.51) for fITT.
  • (ii) Secondary Endpoints
  • MADRS Remission Rates over Treatment Period
  • At Treatment Week 6 the percentage of subjects with MADRS remission (MADRS total score ≤10) in the eITT population was 16.9% for aticaprant and 16.9% for placebo. Treatment week 6 remission rates in fITT population were 31.2% for aticaprant and 22.2% for placebo. For both populations (eITT and fITT), no significant treatment differences were detected at treatment week 6 using Chi-square test (2-sided p=0.999 and p=0.203, respectively). See, FIGS. 11 and 12 .
  • MADRS Response Rates (at Least 30% Improvement) Over Treatment Period
  • The percentage of subjects with ≥30% improvement in MADRS total score at treatment week 6 in the eITT population was 57.6% for aticaprant and 45.8% for placebo. Treatment week 6 response rates in fITT population were 61.8% for aticaprant and for 44.4% placebo. For both populations, treatment differences at Treatment Week 6 were significant at 20% 2-sided significance level (Chi-square test: p=0.197 for eITT and p=0.029 for fITT).
  • MADRS Response Rates (at Least 50% Improvement) Over Treatment Period
  • The percentage of subjects with ≥50% improvement in MADRS total score at treatment week 6 in the eITT population was 35.6% for aticaprant and 22.0% for placebo. Treatment week 6 response rates in fITT population were 38.2% for aticaprant and 23.5% for placebo. For both populations, treatment differences at treatment week 6 were significant at 20% 2-sided significance level (Chi-square test: p=0.104 for eITT and p=0.046 for fITT). See, Table 26 and FIGS. 13-16 .
  • TABLE 26
    Change from Treatment Baseline in MADRS
    Total Score at Treatment Week 6 in Both Responders
    and Non-Responders during Placebo Lead-in Period
    aticaprant
    10
    End point values Placebo milligrams (mg)
    Number of subjects analyzed 81 77
    Units: score on a scale
    Measure Type: Least −6.5 ± 0.78 −9.6 ± 0.79
    Squares Mean
    (Standard Error)
    P-value =0.0017
    Parameter type Least Squares Mean Difference
    Point estimate −3.1
    Confidence interval
    level
    80%
    sides 1-Sided
    lower limit
    upper limit −2.21
    Variability estimate Standard Error of the mean
    Dispersion value 1.05
  • Changes in SHAPS Total Score from Treatment Baseline to Treatment Week 6
  • Enriched ITT Analysis Set
  • In eITT population, in a subgroup of subjects with high anhedonia level (baseline SHAPS total score ≥38), larger differences between aticaprant placebo at Treatment Week 6 were observed than in subjects with low anhedonia level (20≤baseline SHAPS total score <38). The effect size was 0.38 and 0.11, respectively.
  • The mean (SD) SHAPS total score at treatment baseline was 36.6 (5.45), ranging from 20 to 50. The mean change from treatment baseline (SD) in SHAPS total score at treatment week 6 was −4.6 (6.23) for aticaprant and −4.2 (5.04) for placebo. The observed effect size was 0.07. See, Table 27 and FIGS. 17 and 37 .
  • TABLE 27
    SHAPS Total Score: Mean Changes to Placebo
    During the Treatment Period; eITT Analysis Set
    Mean 90%
    Change Mean CI for
    Analysis from Change to Mean
    Visit Baseline Placebo Change to Effect
    Treatment N (SD) (SD pooled) Placebo Size
    Treatment Week
    1
    Placebo 61 −1.3 (3.17)
    aticaprant 60 −1.9 (4.30) −0.6 (3.77) [−1.7, 0.6] −0.15
    Treatment Week 3
    Placebo 59 −2.2 (4.65)
    aticaprant 59 −3.4 (5.25) −1.2 (4.96) [−2.8, 0.3] −0.25
    Treatment Week 4
    Placebo 60 -3.3 (4.47)
    aticaprant 57 −4.5 (5.89) −1.2 (5.21) [−2.8, 0.4] −0.23
    Treatment Week 5
    Placebo 60 −3.9 (4.88)
    aticaprant 56 −4.3 (6.07) −0.4 (5.49) [−2.1, 1.3] −0.08
    Treatment Week 6
    Placebo 59 −4.2 (5.04)
    aticaprant 59 −4.6 (6.23) −0.4 (5.66) [−2.1, 1.3] −0.07
    Negative change from baseline indicates improvement. Negative change to Placebo indicates favorable aticaprant effect. Negative effect size favors aticaprant; positive effect size favors Placebo.
  • Changes in SHAPS total score were analyzed with the same MMRM model used for MADRS total score. The estimated LS Mean difference with 80% 2-sided CI at treatment week 6 between aticaprant and placebo was −0.7 [−1.81, 0.41]. See, FIG. 7 and Tables 28 and 29 and FIG. 18 . The corresponding p-value was 0.419.
  • TABLE 28
    SHAPS Total Score: MMRM Results - Estimated LS Means and Comparison
    versus Placebo; eITT Analysis Set
    Change from Baseline
    LSMean
    Difference 60%
    Analysis (SE)\ Confidence
    Visit Mean Mean LSMean Treatment Interval on p-
    Treatment N (SD) (SD) (SE) Placebo Difference valuea
    Treatment Week 1
    Placebo 61 35.5 −1.3 −0.9
    (6.00) (3.17) (0.63)
    aticaprant 60 34.5 −1.9 −1.7 −0.8 (0.86) [−1.90, 0.31] 0.3542
    (5.63) 5 (4.30) (0.64)
    Treatment Week 3
    Placebo 59 34.9 −2.2 −1.8
    (6.09) (4.65) (0.64)
    aticaprant 59 33.0 −3.4 −3.2 −1.4 (0.86) [−2.53, −0.31] 0.1005
    (6.39) (5.25) (0.64)
    Treatment Week 4
    Placebo 60 33.7 −3.3 −2.9
    (5.89) (4.47) (0.63)
    aticaprant 57 32.0 −4.5 −4.3 −1.4 (0.86) [−2.48, −0.26] 0.1131
    (6.24) (5.89) (0.64)
    Treatment Week 5
    Placebo 60 33.1 −3.9 −3.5
    (5.88) (4.88) (0.64)
    aticaprant 56 32.4 −4.3 −4.0 −0.5 (0.87) [−1.65, 0.57] 0.5332
    (6.61) (6.07) (0.64)
    Treatment Week 6
    Placebo 59 32.9 −4.2 −3.7
    (6.04) (5.04) (0.64)
    aticaprant 59 31.9 −4.6 −4.4 −0.7 (0.87) [−1.81, 0.41] 0.4188
    (6.60) (6.23) (0.64)
    atwo-sided test for no difference between treatments from a MMRM model with subject as random effect; country, treatment, time and time-by-treatment interaction as factors; and baseline SHAPS total score as continuous covariate. An AR(1) variance-covariance matrix was employed.
  • TABLE 29
    SHAPS Total Score: MMRM Results - Estimated LS Means and Comparison
    versus Placebo; fITT Analysis Set
    Change from Baseline
    LSMean
    Difference 60%
    (SE)\ Confidence
    Analysis Visit Mean Mean LSMean Treatment Interval on p-
    Treatment N (SD) (SD) (SE) Placebo Difference valueª
    Treatment Week 1
    Placebo 83 34.8 −1.5 −1.0
    (5.86) (3.57) (0.54)
    aticaprant 83 32.9 −2.0 −1.9 −1.0 (0.72) [−1.88, 0.1888
    (6.09) (4.05) (0.54) −0.02]
    Treatment Week 3
    Placebo 81 34.3 −2.2 −1.7
    (6.36) (5.11) (0.54)
    aticaprant 80 31.9 −3.2 −3.1 −1.4 (0.73) [−2.32, 0.0580
    (6.54) (5.07) (0.54) −0.45]
    Treatment Week 4
    Placebo 82 33.4 −3.0 −2.5
    (5.70) (4.41) (0.54)
    aticaprant 78 30.8 −4.2 −4.1 −1.6 (0.73) [−2.51, 0.0321
    (6.37) (5.70) (0.55) −0.63]
    Treatment Week 5
    Placebo 82 32.6 −3.8 −3.3
    (5.63) (4.76) (0.55)
    aticaprant 77 30.9 −4.3 −4.1 −0.8 (0.73) [−1.71, 0.2912
    (6.76) (5.70) (0.55) 0.17]
    Treatment Week 6
    Placebo 81 32.2 −4.2 −3.7
    (5.81) (4.98) (0.55)
    aticaprant two-sided test 77 30.5 −4.7 −4.5 −0.8 (0.73) [−1.79, 0.2503
    (6.98) (5.91) (0.55) 0.10]
    atwo-sided test for no difference between treatments from a MMRM model with subject as random effect; country, treatment, time and time-by-treatment interaction as factors; and baseline SHAPS total score as continuous covariate. An AR(1) variance-covariance matrix was employed
  • The estimated LS mean differences with 80% 2-sided CI at treatment week 6 between aticaprant and placebo was −0.8 [−1.79, 0.10]. The corresponding p-value was 0.250. See, FIGS. 7 and 8 .
  • Full ITT Analysis Set
  • Similar trend was observed in fITT population and differences were larger in magnitude than those observed in eITT population. The effect size was 0.51 and 0.29, respectively. The mean (SD) baseline SHAPS total score at treatment baseline was 35.6 (5.67), ranging from 14 to 50. The mean changes from treatment baseline in SHAPS total score at treatment week 6 for fITT population were similar to changes in eITT: −4.7 (5.91) for aticaprant and −4.2 (4.98) for placebo. The observed effect size was 0.08. See, Table 30.
  • TABLE 30
    SHAPS Total Score: Mean Changes to Placebo
    During the Treatment Period; fITT Analysis Set
    Mean Mean 90% CI
    Analysis Change from Change to for Mean
    Visit Baseline Placebo Change to Effect
    Treatment N (SD) (SD pooled) Placebo Size
    Treatment Week
    1
    Placebo 83 −1.5 (3.57)
    aticaprant 83 −2.0 (4.05) −0.6 (3.82) [−1.5, 0.4] −0.15
    Treatment Week 3
    Placebo 81 −2.2 (5.11)
    aticaprant 80 −3.2 (5.07) −1.0 (5.09) [−2.4, 0.3] −0.20
    Treatment Week 4
    Placebo 82 −3.0 (4.41)
    aticaprant 78 −4.2 (5.70) −1.2 (5.08) [−2.5, 0.1] −0.23
    Treatment Week 5
    Placebo 82 −3.8 (4.76)
    aticaprant 77 −4.3 (5.70) −0.5 (5.24) [−1.8, 0.9] −0.09
    Treatment Week 6
    Placebo 81 −4.2 (4.98)
    aticaprant 77 −4.7 (5.91) −0.5 (5.45) [−1.9, 1.0] −0.08
    Negative change from baseline indicates improvement. Negative change to Placebo indicates favorable aticaprant effect. Negative effect size favors aticaprant; positive effect size favors Placebo.
  • Changes in MADRS Total Score from Treatment Baseline to Treatment Week 6 by Anhedonia Level at Baseline
  • Enriched ITT Analysis Set
  • In subgroup of subjects with high anhedonia level (SHAPS total score ≥38) at treatment baseline, n=53, larger differences between aticaprant and placebo at treatment Week 6 were observed than in subjects with low anhedonia level (20≤baseline SHAPS total score <38), n=65:−3.4 with 90% 2-sided CI of [−7.5, 0.7] and −0.9 with 90% 2-sided CI of [−4.2, 2.5], respectively (Table 31). The observed effect size was 0.38 and 0.11, respectively.
  • TABLE 31
    MADRS (Montgomery-Åsberg Depression Rating Scale) Total
    Score: Mean Changes to Placebo During the Treatment Period by
    Anhedonia Level at Treatment Baseline; eITT Analysis Set
    Level
    Mean 90% CI
    Mean Change Change to for Mean
    Analysis Visit from Baseline Placebo Change to Effect
    Treatment N (SD) (SD pooled) Placebo size
    Low anhedonia
    Treatment Week
    1
    Placebo 34 −1.8 (3.43)
    aticaprant 34 −2.3 (5.03) −0.5 (4.30) [−2.2, 1.2] −0.12
    Treatment Week 3
    Placebo 32 −4.8 (5.70)
    aticaprant 33 −4.9 (5.99) −0.1 (5.85) [−2.5, 2.4] −0.01
    Treatment Week 4
    Placebo 33 −6.5 (6.16)
    aticaprant 32 −6.4 (7.40) 0.0 (6.80) [−2.8, 2.9] 0.01
    Treatment Week 5
    Placebo 33 −7.6 (6.80)
    aticaprant 29 −7.2 (6.46) 0.3 (6.65) [−2.5, 3.2] 0.05
    Treatment Week 6
    Placebo 32 −8.3 (8.25)
    aticaprant 33 −9.2 (8.01) −0.9 (8.13) [−4.2, 2.5] −0.11
    High anhedonia
    Treatment Week
    1
    Placebo 27 −2.7 (4.08)
    aticaprant 26 −4.6 (5.25) −1.8 (4.69) [−4.0, 0.3] −0.39
    Treatment Week 3
    Placebo 27 −3.6 (6.35)
    aticaprant 26 −6.7 (6.83) −3.0 (6.59) [−6.1, 0.0] −0.46
    Treatment Week 4
    Placebo 27 −6.3 (7.34)
    aticaprant 25 −8.5 (7.26) −2.2 (7.30) [−5.6, 1.2] −0.30
    Treatment Week 5
    Placebo 27 −7.1 (7.67)
    aticaprant 26 −9.7 (8.18) −2.6 (7.93) [−6.3, 1.0] −0.33
    Treatment Week 6
    Placebo 27 −8.1 (9.01)
    aticaprant 26 −11.5 (8.95)  −3.4 (8.98) [−7.5, 0.7] −0.38
    Low Anhedonia level (SHAPS Total Score at Treatment Baseline >= 20 and < 38), High Anhedonia level (SHAPS Total Score at Treatment Baseline >= 38). The MADRS Total Score ranges from 0 to 60, with higher scores indicating greater severity of depression.
  • Full ITT Analysis Set
  • A similar trend was observed in fITT population. The differences were larger in magnitude compared to eITT population: −4.6 with 90% 2-sided CI of [−8.4, −0.8] for subjects with high anhedonia level (n=63) and −2.3 with 90% 2-sided CI of [−5.0, 0.4] for subjects with low anhedonia level (n=94). See, Table 32. The observed effect size was 0.51 and 0.29, respectively.
  • TABLE 32
    MADRS (Montgomery-Åsberg Depression Rating Scale) Total Score:
    Mean Changes to Placebo During the Treatment Period
    by Anhedonia Level at Treatment Baseline; fITT Analysis Set
    Mean 90% CI
    Analysis Mean Change Change to for Mean
    Visit from Baseline Placebo Change to Effect
    Treatment N (SD) (SD pooled) Placebo size
    Low anhedonia
    Treatment Week
    1
    Placebo 49 −1.3 (4.17)
    aticaprant 52 −2.4 (4.59) −1.0 (4.39) [−2.5, 0.4] −0.24
    Treatment Week 3
    Placebo 47 −3.6 (6.04)
    aticaprant 49 −4.1 (6.67) −0.5 (6.37) [−2.7, 1.7] −0.08
    Treatment Week 4
    Placebo 48 −4.9 (6.53)
    aticaprant 48 −6.4 (6.77) −1.5 (6.65) [−3.8, 0.8] −0.23
    Treatment Week 5
    Placebo 48 −6.6 (6.82)
    aticaprant 45 −7.3 (6.90) −0.7 (6.86) [−3.1, 1.7] −0.10
    Treatment Week 6
    Placebo 47 −6.5 (8.11)
    aticaprant 47 −8.8 (7.48) −2.3 (7.80) [−5.0, 0.4] −0.29
    High anhedonia
    Treatment Week
    1
    Placebo 34 −2.4 (3.71)
    aticaprant 30 −4.4 (5.04) −2.0 (4.38) [−3.8, −0.1] −0.45
    Treatment Week 3
    Placebo 34 −3.1 (7.17)
    aticaprant 30 −6.9 (6.66) −3.8 (6.94) [−6.7, −0.9] −0.54
    Treatment Week 4
    Placebo 34 −4.8 (7.75)
    aticaprant 29 −8.6 (7.32) −3.8 (7.56) [−7.0, −0.6] −0.50
    Treatment Week 5
    Placebo 34 −6.2 (7.72)
    aticaprant 30 −10.2 (8.04) −4.0 (7.87) [−7.3, −0.7] −0.51
    Treatment Week 6
    Placebo 34 −6.8 (9.30)
    aticaprant 29 −11.3 (8.69)  −4.6 (9.03) [−8.4, −0.8] −0.51
    Low Anhedonia level (SHAPS Total Score at Treatment Baseline >= 20 and < 38), High Anhedonia level (SHAPS Total Score at Treatment Baseline >= 38). The MADRS Total Score ranges from 0 to 60, with higher scores indicating greater severity of depression.
  • This data illustrates that segmentation into high vs low anhedonia had a benefit for treating MDD: higher treatment effect for aticaprant. Further, the placebo response was lower in patients with high anhedonia, as compared to low anhedonia.
  • Change from Treatment Baseline in CGI-S Total Score at Treatment
  • TABLE 33
    Change from Treatment Baseline in CGI-S Total Score at Treatment
    aticaprant 10
    End point values Placebo milligrams (mg)
    Number of subjects analyzed 59 59
    Units: Scores on a scale
    Measure Type: Arithmetic Mean (SD) −0.76 ± 0.858 −0.92 ± 1.039
  • Change from Treatment Baseline in SMDDS Total Score at Treatment Week 6
  • TABLE 34
    Change from Treatment Baseline in SMDDS Total Score at Treatment Week
    aticaprant 10
    End point values Placebo milligrams (mg)
    Number of subjects analyzed 59 59
    Units: Scores on a scale
    Measure Type: Arithmetic Mean (SD) −8.49 ± 9.567 −8.03 ± 9.957
  • Number of Subjects with SATE Score at Treatment Week 6
  • TABLE 35
    Number of Subjects with SATE Score at Treatment Week 6
    aticaprant 10
    milligrams
    End point values Placebo (mg)
    Number of subjects analyzed 61 60
    Units: subjects
    Overall Depression (Got worse) (n = 40, 30) 1 0
    Overall Depression (Not changed) (n = 40, 30) 12 9
    Overall Depression (Improved) (n = 40, 30) 27 21
    Depression Worsened (Slightly worse) (n = 1, 0) 1 0
    Depression Worsened (Much worse) (n = 1, 0) 0 0
    Depression Worsened (Very much worse) 0 0
    (n = 1, 0)
    Depression Slightly improved (n = 27, 21) 13 15
    Depression Much improved (n = 27, 21) 11 6
    Depression Very Much Improved (n = 27, 21) 3 0
  • Change from Treatment Baseline in HAM-A6 Total Score at Treatment Week 6
  • TABLE 36
    Change from Treatment Baseline in HAM-A6
    Total Score at Treatment Week 6
    aticaprant 10
    End point values Placebo milligrams (mg)
    Number of subjects analyzed 59 59
    Units: scores on a scale
    Measure Type: Arithmetic Mean (SD) −2.19 ± 2.837 −2.73 ± 2.651
  • These data show a greater improvement in HAMA6 score in aticaprant treated patients vs. placebo.
  • Change from Treatment Baseline in Structured Interview Guide for the SIGH-A Score at Treatment Week 6
  • TABLE 37
    Change from Treatment Baseline in Structured Interview
    Guide for the SIGH-A score at Treatment Week 6
    aticaprant 10
    End point values Placebo milligrams (mg)
    Number of subjects analyzed 59 59
    Units: scores on a scale
    Measure Type: Arithmetic Mean (SD) −5.37 ± 6.549 −5.85 ± 5.369
  • Maximum Plasma Concentration (Cmax) of Aticaprant
  • Cmax is defined as maximum plasma concentration of aticaprant. The eITT population included all enrolled lead-in placebo non-responders who were randomized into a treatment period, received at least 1 dose of study medication, and had at least 1 post-baseline MADRS assessment during the treatment period. Here ‘N’ (number of subjects analyzed) includes the number of subjects evaluable for this endpoint. Here ‘n’ (number analyzed) included all subjects evaluable for specified time point categories.
  • TABLE 38
    Cmax of Aticaprant (10 mg)
    Number of subjects analyzed 58
    Units: nanograms per milliliter (ng/ml)
    Measure Type: Arithmetic Mean (SD)
    Week 1 (n = 56) 32.7 ± 10.9
    Week 3 (n = 56) 33.5 ± 11.1
    Week 6 (n = 56) 34.3 ± 11.1
    No statistical analyses of this end point.
  • (iii) Safety Endpoints
  • Overall, in full safety analysis set 40/85 (47.1%) of subjects in the aticaprant group and 30/84 (35.7%) of subjects in the placebo group experienced at least one TEAE during the treatment period. See, Table 39.
  • TABLE 39
    Overall Summary of Treatment-Emergent Adverse Events
    During the Treatment Period; Full Safety Analysis Set
    Placebo aticaprant 10 Overall
    (N = 84) mg (N = 85) (N = 169)
    n (%) n (%) n (%)
    Subjects with 1 or more TEAE 30 (35.7) 40 (47.1) 70 (41.4)
    Total subjects affected by 9 (10.7%) 23 (27.1%)
    non-serious adverse events
    Subjects with drug-related 13 (15.5) 20 (23.5) 33 (19.5)
    TEAE a
    Subjects with TEAE 0 0 0
    leading to death
    Subjects with 1 or more 1 (1.2) 0 1 (0.6)
    serious TEAE
    Subjects with TEAE leading 1 (1.2) 1 (1.2) 2 (1.2)
    to discontinuation of agent
    a Drug relationships of possible, probable, and very likely are included in this category. Subjects are presented by the treatment received during the Treatment period.
  • The most common TEAEs during the treatment period were headache (experienced by 10/85 subjects—11.8% in the aticaprant group and by 6/84 subjects—7.1% in the placebo group) and diarrhea (experienced by 7/85 subjects—8.2% in the aticaprant group and by 2/84 subjects—2.4% in the placebo group). See, Table 40.
  • TABLE 40
    Treatment-Emergent Adverse Events by Body
    System or Organ Class and Dictionary-Derived
    Term in >= 5% of Subjects in Either Treatment Group
    During the Treatment Period; Full Safety Analysis Set
    aticaprant
    Placebo
    10 mg Overall
    Body System (N = 84) (N = 85) (N = 169)
    Preferred Term n (%) n (%) n (%)
    Total no. Subjects with 30 (36) 40 (47) 70 (41)
    Adverse Events
    Infections And Infestations  9 (11) 13 (15) 22 (13)
    Nasopharyngitis 2 (2) 5 (6) 7 (4)
    Nervous System Disorders  9 (11) 13 (15) 22 (13)
    Headache 6 (7) 10 (12) 16 (10)
    Gastrointestinal Disorders  9 (11) 12 (14) 21 (12)
    Diarrhea 2 (2) 7 (8) 9 (5)
    Skin And Subcutaneous Tissue 3 (4) 6 (7) 9 (5)
    Disorders
    Pruritus
    0 5 (6) 5 (3)
    Percentages calculated with the number of subjects in each group as denominator. Reported dictionary version: MedDRA 22.1. Subjects are presented by the treatment received during the Treatment period.
  • There were 2 subjects in total who discontinued during the treatment period due to treatment-emergent adverse events: 1 subject in the aticaprant 10 group due to diarrhea, nausea, vomiting and headache, and another subject in placebo group due to acute calculous cholecystitis.
  • Overall, 17/169 subjects experienced TEAEs of special interest during the treatment period: 13/85 (15.3%) in the aticaprant group and 4/84 (4.8%) in the placebo group. The most common treatment-emergent adverse events during the treatment phase were headache and diarrhea. The most common TEAE of special interest during the treatment period were diarrhea and pruritus (experienced by 5/85 subjects—5.9% in the aticaprant group and by 0/84 subjects in the placebo group). Further 1 patient in the placebo group (1.19%) experienced acute cholecystitis, as compared to 0 patients receiving aticaprant. See, Table 41.
  • TABLE 41
    Treatment-Emergent Adverse Events of Special Interest
    During the Treatment Period; Full Safety Analysis Set
    aticaprant
    Placebo
    10 mg Overall
    Body System (N = 84) (N = 85) (N = 169)
    Preferred Term n (%) n (%) n (%)
    Total no. Subjects with Adverse 4 (4.8) 13 (15.3) 17 (10.1)
    Events of Special Interest
    Gastrointestinal Disorders 4 (4.8)  9 (10.6) 13 (7.7) 
    deaths causally related to
    treatment/all
    Diarrhea 2 (2.4) 7 (8.2) 9 (5.3)
    Abdominal Pain Upper 2 (2.4) 0 2 (1.2)
    Dyspepsia 1 (1.2) 1 (1.2) 2 (1.2)
    Abdominal Pain 0 1 (1.2) 1 (0.6)
    Skin And Subcutaneous Tissue 0 5 (5.9) 5 (3.0)
    Disorders
    Pruritus
    0 5 (5.9) 5 (3.0)
    Percentages calculated with the number of subjects in each group as denominator. Reported dictionary version: MedDRA 22.1. Subjects are presented by the treatment received during the Treatment period.
  • Two serious adverse events occurred. One subject in the placebo group experienced acute calculous cholecystitis during the treatment period and other subject suicidal ideation during the lead-in period. Both subjects discontinued due to these AEs.
  • No deaths were reported.
  • (iv) Anhedonia Analysis
  • Patients in the larger fITT group maintained baseline level of depression and anhedonia severity consistent with the eITT group. See, Tables 42-44.
  • TABLE 42
    Frequency of Subjects with Anhedonia at
    Treatment Baseline; fITT Analysis Set
    No Anhedonia Anhedonia
    (SHAPS Total (SHAPS Total
    N Score <20) Score >=20)
    Baseline/Day 22
    Placebo 83 0 83 (100%)
    aticaprant 83 1 (1.2%)  82 (98.8%)
    Total 166 1 (0.6%) 165 (99.4%) 
    Anhedonia classification is based on calculated SHAPS total score at Visit Day 22
  • The results illustrate that treatment effect is larger in patients with more anhedonia at baseline. See, FIG. 19 .
  • TABLE 43
    Frequency of Subjects with Different Level of Anhedonia at
    Treatment Baseline and Treatment Week 6; eITT Analysis Set
    Low Level of High Level of
    No Anhedonia Anhedonia Anhedonia
    (SHAPS Total (20<= SHAPS (SHAPS Total
    N Score <20) Total Score <38) Score >=38)
    Treatment Baseline
    Placebo
    61 0 34 (55.74%) 27 (44.26%)
    aticaprant 60 0 34 (56.67%) 26 (43.33%)
    Total 121 0 68 (56.2%)  53 (43.8%)
    Treatment Week 6
    Placebo 59 0 46 (77.97%) 13 (22.03%)
    aticaprant 59 3 (5.08%) 48 (81.36%) 8 (13.56%)
    Total 118 3 (2.54%) 94 (79.66%) 21 (17.8%)
    Anhedonia classification is based on re-calculated SHAPS total score at analysis visits Treatment Baseline and Treatment Week 6.
  • TABLE 44
    Frequency of Subjects with Different Level of Anhedonia at
    Treatment Baseline and Treatment Week 6; fITT Analysis Set
    Low Level of High Level of
    No Anhedonia Anhedonia Anhedonia
    (SHAPS Total (20>= SHAPS (SHAPS Total
    N Score <20) Total Score <38) Score >=38)
    Treatment Baseline
    Placebo
    83 0 49 (59.04%) 34 (40.96%)
    aticaprant 83 1 (1.2%) 52 (62.65%) 30 (36.14%)
    Total 166 1 (0.6%) 101 (60.84%)  64 (38.55%)
    Treatment Week 6
    Placebo 81 0 66 (81.48%) 15 (18.52%)
    aticaprant 77 7 (9.09%) 62 (80.52%)  8 (10.39%)
    Total 158 7 (4.43%) 128 (81.01%)  23 (14.56%)
    Anhedonia classification is based on re-calculated SHAPS total score at analysis visits Treatment Baseline and Treatment Week 6.
  • The results illustrate that the treatment effect is larger in patients with more anhedonia at baseline. See, FIGS. 20 -A and 20-B. In FIG. 20 -A, i.e., the high anhedonia group, the placebo+oral antidepressant group shows less placebo response as compared to the low anhedonia group in FIGS. 7-8 . Similarly the treatment effect of the aticaprant+oral antidepressant group is higher in the high anhedonia group as compared to the low anhedonia group. Overall the effect size is larger at every single time point (from week 1 onwards) in the high anhedonia group. The LSMD in the high anhedonia group is more than double that of the low anhedonia group at week 6. Further, when looking at the symptom level, greater improvement in items related to anhedonia and dysphoria in subgroup with high anhedonia vs low anhedonia. See, FIG. 21 .
  • (v) Weight Change
  • At the lead-in baseline timepoint, the mean weight for subjects in the placebo group was 76.17 kg compared to 78.66 in the aticaprant group. After 6 weeks in the double-blind treatment phase, the mean weight in the placebo group was 75.75 kg compared to 78.57 kg in the aticaprant group. This indicates that the weight in both groups remained relatively stable over the 6-week double blind treatment period. This is unexpected because other adjunctive treatments for MDD result in a mean weight increase. See, Thase M, et al. J Clin Psych. 2015: 76(9), 1224-1231; Thase, J Clin Psych. 2015, 76(9):1232-1240; El Khalili, Int J Neuropsychopharmacol. 2010, 13, 917-932; Marcus, J. Clin. Psychopharmacol. 2008, 28:156-165; Berman, J. Clin. Psychiatry 2007; 68:843-853; Berman, American College of Neuropsychopharmacology, 2008, Annual Meeting Abstracts (Scottsdale, Ariz., Dec. 7-11, 2008). Nashville, Tenn., ACNP, 2008; Earley, American College of Neuropsychopharmacology, 2007, Annual Meeting Abstracts (Boca Raton, Fla., Dec. 9-13, 2007). Nashville, Tenn., ACNP, 2007). See, Table 45.
  • TABLE 45
    Mean weight by treatment group (kg)
    Placebo Aticaprant
    weight n = 84 n = 85
    Screening, mean (SE) 76.39 (1.61) 78.42 (1.65)
    Lead-in Baseline, mean (SE) 76.17 (1.61) 78.66 (1.65)
    Withdrawal Baseline, mean (SE) 75.75 (1.62) 78.57 (1.71)
    Absolute Change (Withdrawal - Lead-in) −0.42    −0.09   
    Relative % Change −0.55% −0.11%
  • (vi) Completion Rate
  • Patients who passed the screening phase entered a lead in phase followed by a double-blind phase. Patients who responded to placebo during the lead in phase were labelled as non-responders. Patients who did not respond to placebo were labelled as non-responders. The double-blind treatment phase then continued for an additional 6 weeks, after which patients entered a withdrawal period.
  • Of the 121 subjects in the enriched population (60 in aticaprant and 61 in placebo group), 117 (96.7%) completed the study. The overall completion rate for the full ITT analysis set is 95%. This contrasts with completion rates of approximately 85% for studies of adjunctive aripiprazole (Pae, CNS Drugs, 2011; 25, 109-127) and 45-62% for adjunctive quetiapine (El Khalili cited above). In total 4 subjects (3.3%) discontinued the study: 2 subjects in placebo and 2 subjects in aticaprant treatment group. See, Tables 46 and 47.
  • TABLE 46
    Completion/Early Withdrawal Information; eITT Analysis Set
    aticaprant
    Placebo
    10 mg Total
    (N = 61) (N = 60) (N = 121)
    Subject Completed Treatment/Trial
    Completed 59 (96.7%) 58 (96.7%) 117 (96.7%) 
    Withdrawn 2 (3.3%) 2 (3.3%) 4 (3.3%)
    Reason For Withdrawal/Termination
    Lack of Efficacy 0 1 (1.7%) 1 (0.8%)
    Non-compliance with drug 0 1 (1.7%) 1 (0.8%)
    Withdrawal by subject 1 (1.6%) 0 1 (0.8%)
    Other 1 (1.6%) 0 1 (0.8%)
    Percentages calculated with the number of subjects in each group as denominator.
  • TABLE 47
    Completion/Early Withdrawal Information;
    Full Safety Analysis Set
    aticaprant
    Placebo
    10 mg Total
    (N = 84) (N = 85) (N = 169)
    Subject Completed Treatment/Trial
    Completed 81 (96.4%) 79 (92.9%) 160 (94.7%) 
    Withdrawn 3 (3.6%) 6 (7.1%) 9 (5.3%)
    Reason For Withdrawal/Termination
    Adverse event 1 (1.2%) 1 (1.2%) 2 (1.2%)
    Lack of Efficacy 0 2 (2.4%) 2 (1.2%)
    Non-compliance with drug 0 1 (1.2%) 1 (0.6%)
    Protocol deviation 0 1 (1.2%) 1 (0.6%)
    Withdrawal by subject 1 (1.2%) 0 1 (0.6%)
    Other 1 (1.2%) 1 (1.2%) 2 (1.2%)
    Percentages calculated with the number of subjects in each group as denominator.
  • (vii) Sexual Functioning
  • Impairments in sexual functioning is a common side effect of antidepressant treatment and can be very upsetting to patients and their sexual partners. Major depression itself is associated with increased sexual dysfunction, and many of the pharmacological treatments are known to worsen sexual functioning even further. In a large survey of nearly 5000 patients in France, it was estimated that in untreated patients with MDD, the prevalence of sexual dysfunction was 65%. The prevalence of sexual dysfunction increased to 71% for patients treated with antidepressant therapy.
  • Sexual pleasure is an important component of hedonic tone. The brain reward circuitry is controlled by several areas: nucleus accumbens, ventral tegmental area and the amygdala. It is hypothesized that treatment with kappa opioid receptors may restore the normal homeostatic balance in patients with overactivation. Treatment with aticaprant could potentially improve symptoms of anhedonia. Other symptoms associated with the reward circuitry includes: sexual pleasure, lack of interest and lack of enjoyment.
  • Patients had their sexual functioning measured using a standard, well accepted rating scale: ASEX. See, Table 48.
  • TABLE 48
    ASEX scores by treatment group
    Placebo Aticaprant
    n = 84 n = 85
    Baseline 22.04 21.26
    Endpoint 21.36 19.79
    Absolute Change −0.68 −1.47
    Relative % Change −3.09% −6.91%
  • The mean change from treatment baseline (SD) in ASEX total score to week 6 was −1.5 (4.02) points for aticaprant compared to −0.7 (2.98) points for placebo. A lower score on the ASEX indicates improvement. The score reduction at week 6 was greater in the aticaprant group compared to placebo. This is unexpected because adjunctive treatments with other agents are expected to worsen sexual functioning, i.e., increase in ASEX score over time. See, FIG. 22 .
  • Patients receiving aticaprant had notable improvements in sexual functioning. An examination of individual item level changes was also conducted and revealed that the greatest changes were seen in items related to consummatory pleasure: orgasm satisfying, reach orgasm and vaginal lubrication/erection. Most of the improvements seen in items 3, 4 and 5 of FIG. 23 .
  • (viii) Onset of Effect
  • The onset of effect for aticaprant can be estimated from the study. FIG. 10 -B depicts the least squares mean change from baseline. A significant treatment effect favoring aticaprant was seen as early as week 3. At this point, aticaprant showed a statistically superior effect compared to placebo.
    • Example 7—Single Dose Aticaprant as Adjunctive Antidepressant Therapy
  • Study Design: A 6-week, multicenter, double-blind, randomized, placebo-controlled study to assess the efficacy, safety, and tolerability of aticaprant in adult and elderly subjects (18 to 74 years) who have MDD with prominent anhedonia (MDD ANH+), and who have had an inadequate response to a SSRI or a serotonin and SNRI in the current depressive episode. See, FIG. 34 .
  • For all subjects, this study will consist of 3 phases: an eligibility screening phase (up to 4 weeks prior to first dose administration), a double-blind treatment phase of 6 weeks, and a follow-up of 1-2 weeks. Subjects who have completed the double-blind phase may participate in an open-label long-term safety study.
  • Sample Size and Randomization: Approximately 544 subjects with MDD with prominent anhedonia (MDD ANH+) and without prominent anhedonia (MDD ANH−) will be randomized in a 1:1 ratio to adjunctive placebo or aticaprant to achieve a minimum of 314 adult subjects meeting predefined criteria for MDD ANH+ eligible to be included in the primary analysis. Randomization will be stratified by study site, age group (adults [<65 years], elderly [≥65 years]), baseline anhedonia, and baseline MADRS total score. All subjects will continue their baseline antidepressant (SSRI/SNRT) during the entire study.
  • Doses and Administration All eligible subjects will receive aticaprant or placebo in addition to their baseline SSRI/SNRT which will be continued during the entire study. Study medication will be taken daily.
  • Inclusion Criteria:
    1. Age of 18 to 74 years (inclusive).
    2. Be medically stable on the basis of physical examination (including a brief
    neurological examination), medical history, vital signs (including blood pressure),
    and 12-lead ECG performed at screening and baseline. If there are any abnormalities
    that are not specified in the inclusion and exclusion criteria, their significance must
    be determined.
    3. Be medically stable on the basis of clinical laboratory tests performed at screening.
    If the results of the serum chemistry panel, hematology, or urinalysis are outside the
    normal reference ranges, retesting of an abnormal lab values that may lead to
    exclusion will be allowed once during the screening phase.
    4. Meet DSM-5 diagnostic criteria for recurrent or single episode MDD, without
    psychotic features (DSM-5 296.22, 296.23, 296.32, or 296.33), based upon clinical
    assessment and SCID-CT. Subjects 65 years of age or older must have had the first
    onset of depression prior to 55 years of age. The length of the current depressive
    episode must be ≤18 months.
    5. Have had an inadequate response to at least 1 but no more than 2 antidepressants
    (SSRI/SNRI), administered at an adequate dose and duration in the current episode
    of depression. An inadequate response is defined as 26% to <50% reduction in
    depressive symptom severity and overall good tolerability, as assessed by the MGH-
    ATRQ. An adequate trial is defined as an antidepressant treatment for at least 6
    weeks (and no greater than 12 months in the current episode) at or above the stable
    therapeutic dose specified in the MGH-ATRQ, must include the subject's current
    antidepressant treatment. If the subject has received 2 SSRI/SNRI treatments of
    sufficient dose and duration in the current episode, and has shown ≤25%
    improvement to both, then the subject would not qualify based on exclusion
    criterion (first exclusion criterion).
    6. Current major depressive episode, depression symptom severity, presence of
    anhedonia and antidepressant treatment response in the current depressive episode
    must be confirmed. Is receiving and tolerating well any one of the following SSRI
    or SNRI for depressive symptoms, in any formulation and available in the
    participating country: citalopram, duloxetine, escitalopram, fluvoxamine,
    fluoxetine, milnacipran, levomilnacipran, paroxetine, sertraline, venlafaxine,
    desvenlafaxine at a stable dose (at therapeutic dose level) for at least 6 weeks, and
    for no greater than 12 months in the current episode, at screening. The above
    SSRI/SNRI needs to be approved for the treatment of MDD. Subjects using
    fluvoxamine as baseline SSRI and have normal renal and hepatic function are
    admitted.
    7. HDRS-17 total score ≥22 at start of the screening and must not demonstrate a
    clinically significant improvement (which is defined as an improvement of >20%
    on their HDRS-17 total score) from the start to end of screening (from the first to
    the last independent HDRS-17 rating).
    8. Symptoms of anhedonia based on clinical assessment and confirmed by a positive
    response for anhedonia (MDE symptoms Item 2) on the SCID-CT at screening and
    baseline (Day 1 prior to randomization).
    9. BMI between 18 and 40 kg/m2 (inclusive).
    10. Outpatient at screening.
    11. A woman of childbearing potential must have a negative highly sensitive serum (β-
    hCG) pregnancy test at screening and a negative urine pregnancy test predose on
    Day 1 of the double-blind phase prior to randomization.
    12. Contraceptive use by men or women should be consistent with local regulations
    regarding the use of contraceptive methods for subjects in clinical studies.
    13. A woman must be either:
    Postmenopausal
    Permanently sterile
    Of childbearing potential and practicing a highly effective method of
    contraception (failure rate of <1% per year when used consistently and
    correctly).
    14. A woman must not to donate eggs (ova, oocytes) or freeze for future use for the
    purposes of assisted reproduction during the study and for a period of at least 1
    month after receiving the last dose of study medication.
    15. During the study and for a minimum of 1 spermatogenesis cycle (defined as
    approximately 3 months) after receiving the last dose of study medication, a man:
    who is sexually active with a woman of childbearing potential must use a
    barrier method of contraception (e.g., condom with spermicidal
    foam/gel/film/cream/suppository) and his female partner must use a highly
    effective method of contraception.
    who is sexually active with a woman who is pregnant must use a condom.
    must not to donate sperm.
  • Exclusion Criteria:
    1. History of treatment-resistant MDD, defined as a lack of response to 2 or more
    adequate antidepressant treatments in the current episode, as indicated by no or
    minimal improvement (≤25% improvement) when treated with an antidepressant of
    adequate dose (per MGH-ATRQ) and duration (at least 6 weeks).
    2. Current or prior DSM-5 diagnosis of a psychotic disorder or MDD with psychotic
    features, bipolar or related disorders (confirmed by the SCID-CT), intellectual
    disability (DSM-5 diagnostic codes 317, 318.0, 318.1, 318.2, 315.8, and 319),
    autism spectrum disorder, borderline personality disorder, antisocial personality
    disorder, histrionic personality disorder, narcissistic personality disorders or
    somatoform disorders.
    3. Current active DSM-5 diagnosis of obsessive-compulsive disorder, post-traumatic
    stress disorder, anorexia nervosa, or bulimia nervosa.
    4. Primary DSM-5 diagnosis of panic disorder, generalized anxiety disorder, social
    anxiety disorder, or specific phobia which has been the primary focus of psychiatric
    treatment within the past 2 years. These are allowed as secondary diagnoses if MDD
    is the primary focus of treatment.
    5. History or evidence of clinically meaningful noncompliance with current
    antidepressant therapy.
    6. History of moderate to severe substance use disorder including alcohol use disorder
    according to DSM-5 criteria within 6 months before screening or positive test results
    for alcohol and/or drugs of abuse (e.g., opiates [including methadone], cocaine,
    amphetamines, methamphetamines, cannabinoids, CBD, barbiturates, MDMA) at
    screening or at baseline. One retest during screening is allowed. Tobacco and
    caffeine use are not exclusionary.
    7. Has within the last 5 years received any prior antidepressant treatment with
    ketamine/esketamine, electroconvulsive therapy, vagal nerve stimulation, or a deep
    brain stimulation device. Subjects who previously had taken up to 2 doses of
    ketamine/esketamine and did not continue (e.g., did not benefit from the treatment
    or experienced tolerability issues) can be considered for enrollment.
    8. Homicidal ideation/intent or has suicidal ideation with some intent to act within 3
    months prior to the start of the screening phase, per clinical judgment or based on
    the C-SSRS, corresponding to a response of “Yes” on Item 4 (active suicidal
    ideation with some intent to act, without specific plan) or Item 5 (active suicidal
    ideation with specific plan and intent) for suicidal ideation on the C-SSRS, or a
    history of suicidal behavior within the past year prior to the start of the screening
    phase. Subjects reporting suicidal ideation with intent to act or suicidal behavior
    prior to the start of the double-blind treatment phase should be excluded.
    9. Cognitive impairment that would render the informed consent invalid or limit the
    ability of the subject to comply with the study requirements. Subject has
    neurodegenerative disorder (e.g., Alzheimer's disease, vascular dementia,
    Parkinson's disease with clinical evidence of cognitive impairment) or evidence of
    MCI. Subjects of age ≥65 years: has a MMSE <25 or <23 for those subjects with
    less than high school equivalent education.
    10. Current or history of seizures (uncomplicated childhood febrile seizures with no
    sequelae are not exclusionary).
    11. Clinically significant ECG abnormalities at screening or Day 1 prior to
    randomization that may jeopardize the subjects' safety or the integrity of the study
    defined as:
    During screening and/or Day 1, a QT interval corrected according to Fridericia's
    formula (QTcF): ≥450 msec (males); ≥470 msec (females).
    Evidence of second- and third-degree atrioventricular block.
    Features of new ischemia.
    Other clinically important arrhythmia or cardiac abnormalities.
    12. History of, or symptoms and signs suggestive of, liver cirrhosis (e.g., esophageal
    varices, ascites, and increased prothrombin time) OR ALT or AST values >3 × the
    ULN or total bilirubin >1.5 × the ULN in the screening phase. Repeat of screening
    test for abnormal ALT and AST is permitted during the screening period there is an
    alternative explanation for the out of range value.
    13. For elevations in bilirubin if the elevation in bilirubin is consistent with Gilbert's
    disease, the subject may participate.
    14. Positive test result for drugs of abuse (e.g., barbiturates, methadone, opiates,
    cocaine, PCP, MDMA, and amphetamine/methamphetamine) at the start of the
    screening phase or Day 1 of the double-blind treatment phase prior to
    randomization.
    15. Subjects who have a positive test result at screening due to prescribed
    psychostimulants taken for any indication must discontinue the medication at least
    2 weeks before Day 1 of the double-blind treatment phase (prior to randomization).
    The result of the Day 1 (prior to randomization) test for drugs of abuse must be
    negative for the subject to be randomized. Subjects who have a positive test result
    at screening due to prescribed/over-the-counter opiates or barbiturates may be
    permitted to continue in the screening phase if the medication is discontinued at
    least 1 week or 5 half-lives, whichever is longer, before Day 1 of the double-blind
    treatment phase (prior to randomization). The result of the Day 1 (prior to
    randomization) test for drugs of abuse must be negative for the subject to be
    randomized.
    Intermittent use of cannabinoids prior to the start of the screening phase is
    not exclusionary as long as the subject does not meet the criteria for
    substance use disorder.
    A positive test for cannabinoids at the start of the screening phase is not
    exclusionary; however, a positive test result for cannabinoids predose on
    Day 1 of the double-blind treatment phase is exclusionary.
    16. Taking a total daily dose of benzodiazepines greater than the equivalent of 6 mg/day
    of lorazepam at the start of the screening phase.
    17. Recent (last 3 months) history of, or current signs and symptoms of:
    Severe renal insufficiency (creatinine clearance <30 mL/min)
    Clinically significant or unstable cardiovascular, respiratory, gastrointestinal,
    neurologic, hematologic, rheumatologic, immunologic or endocrine disorders.
    Uncontrolled Type 1 or Type 2 diabetes mellitus. Subjects with Type 1 or Type 2
    diabetes mellitus who are controlled (hemoglobin Alc ≤8.0% and glucose ≤150
    mg/dL at screening) may be eligible to participate if otherwise medically healthy,
    and if on a stable regimen of glucose-lowering medications for at least 2 months
    prior to screening).
    18. Current signs/symptoms of hypothyroidism or hyperthyroidism. For subjects with a
    history of thyroid disease and for subjects who, regardless of thyroid history have
    the TSH value out of range, a FT4 test will be conducted. If the FT4 value is
    abnormal and considered to be clinically significant the subject is not eligible.
    19. Subjects with a pre-existing history of thyroid disease/disorder who are treated with
    thyroid hormones need to be on a stable dosage for 3 months prior to the start of the
    screening phase. Subjects taking thyroid supplementation for antidepressant
    purposes are not allowed. Has Cushing's Disease, Addison's Disease, primary
    amenorrhea, or other evidence of significant medical disorders of the hypothalamic-
    pituitary-adrenal axis.
    20. Significant medical illness, particularly unstable medical problem.
    21. Ongoing psychological treatments (e.g., Cognitive Behavior Therapy, Interpersonal
    Psychotherapy, Psychodynamic Psychotherapy etc.), initiated within 6 weeks prior
    to start of screening. A subject who has been receiving ongoing psychological
    treatment for a period of greater than 6 weeks is eligible, if psychological treatment
    to be of stable duration and frequency.
    22. Significant medical illness, particularly unstable medical problem.
    23. Clinically-relevant GI complaints per clinical judgment (unless symptoms of Axis I
    disorder) at screening or baseline or history of documented gastric disease
    (including but not limited to documented peptic ulcer disease, gastritis [including
    atrophic gastritis], upper GI bleeding, Barret's esophagus, Crohn disease, ulcerative
    colitis, GI precancerous conditions or any other clinically-relevant GI disease
    irritable bowel syndrome).
    24. Requires chronic use of a PPIs. A history of chronic NSAID or aspirin use. (Low
    dose aspirin e.g., in cardiovascular disease prevention is allowed).
    25. History of malignancy within 5 years before the start of the screening phase
    (exceptions are squamous and basal cell carcinomas of the skin and carcinoma in
    situ of the cervix, or malignancy that is considered cured with minimal risk of
    recurrence)
    26. Known allergies, hypersensitivity, intolerance, or contraindications to aticaprant
    and/or its excipients.
    27. Taken any prohibited therapies that would not permit dosing on Day 1.
    28. Received an investigational drug (including investigational vaccines) or used an
    invasive investigational medical device within 60 days before the start of the
    screening phase, or has participated in 2 or more MDD or other psychiatric condition
    clinical interventional studies (with different investigational medication) in the
    previous 1 year before the start of the screening phase, or is currently enrolled in an
    investigational interventional study.
    29. A woman who is pregnant, breastfeeding, or planning to become pregnant while
    enrolled or within 6 weeks after the last dose of the study medication.
    30. Plans to father a child while enrolled or within 90 days after the last dose of study
    intervention.
    31. Diagnosis of acquired immunodeficiency syndrome. Human immunodeficiency
    virus testing is not required.
    32. Any condition or situation/circumstance for which participation would not be in the
    best interest of the subject (e.g., compromise the well-being) or that could prevent,
    limit, or confound the protocol specified assessments.
  • A. Efficacy Objectives and Endpoints
  • The assessment of primary and secondary (key and other) endpoints will be conducted on the FAS which includes adult (not elderly) subjects with MDD ANH+ who took at least 1 dose of study medication.
  • Primary: To evaluate the efficacy of aticaprant compared with placebo as adjunctive therapy to an antidepressant (SSRI or SNRI) in improving depressive symptoms in adult subjects with MDD ANH+ and inadequate response to the current antidepressant, as assessed by the change from baseline in the MADRS total score from Day 1 (pre-randomization) to end of the 6-week double-blind treatment phase (Day 43):
      • Change from baseline to Day 43 in the MADRS total score.
  • Key Secondary: To assess efficacy of aticaprant compared with placebo in adult subjects with MDD ANH+ as adjunctive therapy to an antidepressant on patient-reported assessment of anhedonia outcomes:
      • Change from baseline to Day 43 in the Dimensional Anhedonia Rating Scale (DARS) total score.
  • Other Secondary: To assess the efficacy of aticaprant compared with placebo in adult subjects with MDD ANH+ as adjunctive therapy on the following:
      • Proportion of responders at Day 43 (≥50% reduction in MADRS total score).
      • Proportion of subjects with remission of depressive symptoms, defined as a MADRS total score ≤12 at Day 43.
      • Change from baseline to Day 43 in MADRS 6
      • Change from baseline to Day 43 in PHQ-9 total score.
      • Change from baseline to Day 43 in SHAPS total score.
      • Change from baseline to Day 43 in symptoms of anxiety using the GAD-7.
  • Exploratory: To assess the efficacy of aticaprant compared with placebo in adult subjects with MDD ANH+, and all MDD subjects (adult and elderly subjects with MDD ANH+ and MDD ANH−) as adjunctive therapy on the following:
      • Change from baseline over time in the MADRS total score.
      • Change from baseline over time in MADRS anhedonia items factor score.
      • Change from baseline over time in patient-reported outcomes of anhedonia (SHAPS, DARS).
      • Change from baseline over time in PHQ-9 total score.
      • Change from baseline to Day 43 in health-related quality of life and health status, as assessed by the EQ-5D-5L questionnaire.
      • Change from baseline to Day 43 in the SDS total score.
      • Change from baseline over time in the CGI-S score.
      • Change from baseline over time in symptoms of anxiety using the GAD-7.
      • Change from baseline over time in depressive symptoms using the PGI-S.
      • Change from baseline to Day 43 in patient-reported sexual functioning using the ASEX.
  • To assess the efficacy of aticaprant compared with placebo in adult subjects with MDD ANH− as adjunctive therapy on the following:
      • Change from baseline over time in MADRS total score.
      • Change from baseline over time in DARS total score.
  • Safety Objectives (All): The following safety endpoints will be assessed separately for the adult and elderly subjects; the safety analysis set for each age group will include all randomized subjects who have received at least one dose of study medication:
      • AEs including AESI. An AE can be any unfavorable and unintended sign (including an abnormal finding), symptom, or disease temporally associated with the use of a medicinal (investigational or non-investigational) product, whether or not related to that medicinal (investigational or non-investigational) product. TEAEs were AEs with onset during the treatment phase that has worsened since baseline. The full safety analysis set included all enrolled subjects who received at least 1 dose of study medication in the treatment period.
      • Vital signs
      • ECG, Laboratory Values
      • Weight/BMI
      • Suicidality assessment using the C-SSRS
      • Withdrawal symptoms assessment using the PWC-20
  • B. Concomitant Therapies and Prohibited Therapies
  • Background therapy: All subjects will continue their baseline antidepressant (SSRI/SNRT) during the entire study. The following antidepressants are permitted: citalopram, duloxetine, escitalopram, fluvoxamine, fluoxetine, milnacipran, levomilnacipran, paroxetine, sertraline, venlafaxine, and desvenlafaxine. Subjects will only continue one of these allowed antidepressants at an adequate and tolerated dose (i.e., monotherapy) during the study. No changes in antidepressant or dose are permitted from screening until the end of the study.
  • Prohibited therapies: Subjects must not use the following medications or food supplements prior to or during the study, as indicated, except to treat an AE or breakthrough symptoms, preferably after the EOT visit:
      • MAOIs within 4 weeks before screening until the first follow-up visit.
      • Antipsychotic drugs from at least 14 days before Day 1 until the first follow-up visit.
      • Hypnotic drugs or food supplements (from at least 7 days prior to Day 1 until the first follow-up visit), including but not limited to benzodiazepines, non-benzodiazepine hypnotics (e.g., zolpidem, zopiclone, zaleplon, eszopiclone, suvorexant and ramelteon), sedating antihistamines including over-the-counter hypnotics (e.g., diphenhydramine, doxylamine, and hydroxyzine), and melatonin/agomelatine.
      • Subjects who were taking benzodiazepines and/or permitted non-benzodiazepine sleep medications during the screening phase can continue these medications (at dosages equal to or less than the equivalent of 6 mg/day of lorazepam) during the double-blind treatment phase. No dose increases beyond the equivalent of 6 mg/day of lorazepam, or new benzodiazepine medications are permitted during the double-blind treatment phase.
      • Non-SSRI/SNRI antidepressants (e.g., doxepin, trazodone, mirtazapine, bupropion, tricyclic antidepressants, agomelatine, and SAMe) from at least 7 days before Day 1 until the first follow-up visit.
      • Any form of new psychotherapy or change in current psychotherapy is prohibited during the screening and double-blind phase.
      • Opiates and mood stabilizers (e.g., lithium and anticonvulsants) from at least 7 days prior to Day 1 until the first follow-up visit.
      • Stimulants (e.g., dexamphetamine, methylphenidate, dexmethylphenidate), oral systemic steroids, and appetite suppressants (ephedrine), and isoxsuprine from at least 7 days before Day 1 until EOT.
      • Magnetic and electrical stimulation therapies: electroconvulsive therapy, vagal nerve stimulation, deep brain stimulations, TMS of any type, or DCS or electrical stimulation, from screening to End-of-Study visit. TMS or DCS or electrical stimulation use prior to screening is not exclusionary.
      • T3, thyroid hormone or other thyroid function supplementation prescribed for depression.
      • These medications are allowed when given to control pre-existing thyroid disease/disorder.
      • Ketamine or esketamine within 5 years prior to and during the study (up to 2 doses are allowed in lifetime prior to screening).
      • Psychedelics (e.g., psilocybin).
      • Memantine.
      • Other investigational drugs within 30 days prior to and during the study.
    Example 8—a Randomized, Double-Blind, Multicenter, Placebo-Controlled Study to Evaluate the Efficacy, Safety, and Tolerability of Fixed Doses of Aticaprant 5 mg and 10 mg as Adjunctive Therapy in Adult and Elderly Subjects with MDD with Prominent Anhedonia and Inadequate Response to Current Antidepressant Therapy
  • Study Design: An 8-week, multicenter, double-blind, randomized, placebo-controlled study to assess the efficacy, safety, and tolerability of aticaprant in adult and elderly subjects (18 to 74 years) who have MDD with prominent anhedonia and who have had an inadequate response to a SSRI or a SNRI in the current depressive episode. See, FIG. 35 .
  • For all subjects, this study will consist of 3 phases:
      • an eligibility screening phase (up to 4 weeks prior to first dose administration),
      • a double-blind treatment phase of 8 weeks,
      • and a follow-up phase of 1-2 weeks.
  • Approximately 624 subjects (randomized in a 2:1:1 ratio to placebo, aticaprant 5 mg, and aticaprant 10 mg) will be enrolled in the study. This enrolment is targeted to achieve a minimum of 556 adult subjects with MDD with prominent anhedonia and approximately 68 elderly subjects (≥65 years) with MDD with prominent anhedonia.
  • Subjects who have completed the double-blind treatment phase may participate in an open-label long-term safety study.
  • Sample Size and Randomization: Approximately 624 adult (<65 years) and elderly (≥65 years) subjects with MDD with prominent anhedonia will be randomized in a 2:1:1 ratio to adjunctive placebo, 5-mg aticaprant, or 10-mg aticaprant to achieve a minimum of 556 adult subjects meeting predefined criteria for MDD with prominent anhedonia eligible to be included in the primary efficacy analysis set. Randomization will be stratified by study site, age group (adult, elderly) and baseline MADRS total score. All subjects will continue their baseline antidepressant (SSRI/SNRI) during the entire study.
  • Doses and Administration: All eligible subjects will receive aticaprant 5 mg, aticaprant 10 mg or placebo in addition to their baseline SSRI/SNRI which will be continued during the entire study. Study medication will be taken daily.
  • Inclusion Criteria:
    1. Age of 18 to 74 years (inclusive).
    2. Medically stable on the basis of physical examination (including a brief
    neurological examination), medical history, vital signs (including blood
    pressure), and 12-lead ECG performed at screening and baseline.
    3. Medically stable on the basis of clinical laboratory tests performed at screening.
    If the results of the serum chemistry panel, hematology, or urinalysis are outside
    the normal reference ranges, retesting of an abnormal lab values that may lead
    to exclusion will be allowed once during the screening phase.
    4. Meet DSM-5 diagnostic criteria for recurrent or single episode MDD, without
    psychotic features (DSM-5 296.22, 296.23, 296.32, or 296.33), based upon
    clinical assessment and confirmed by the SCID-CT. Subjects 65 years of age or
    older must have had the first onset of depression prior to 55 years of age. The
    length of the current depressive episode must be ≤18 months.
    5. Symptoms of anhedonia based on clinical assessment and confirmed by a
    positive response for anhedonia (MDE symptoms Item 2) on the SCID-CT at
    screening and baseline (Day 1 prior to randomization).
    6. SHAPS total score of ≥38 at screening and baseline (Day 1 prior to
    randomization) corresponding to prominent (high level) of anhedonia.
    7. Inadequate response to at least 1 but no more than 2 antidepressants
    (SSRI/SNRI), administered at an adequate dose and duration in the current
    episode of depression. An inadequate response is defined as 26% to <50%
    reduction in depressive symptom severity and overall good tolerability, as
    assessed by the MGH-ATRQ. An adequate trial is defined as an antidepressant
    treatment for at least 6 weeks (and no greater than 12 months in the current
    episode) at or above the stable therapeutic dose specified in the MGH-ATRQ,
    must include the subject's current antidepressant treatment. If the subject has
    received 2 SSRI/SNRI treatments of sufficient dose and duration in the current
    episode, and has shown ≤25% improvement to both, then the subject would not
    qualify based on exclusion criterion (first exclusion criterion).
    8. The current major depressive episode, depression symptom severity, presence
    of anhedonia and antidepressant treatment response in the current depressive
    episode, must be confirmed. Is receiving and tolerating well any one of the
    following SSRI or SNRI for depressive symptoms, in any formulation and
    available in the participating country citalopram, duloxetine, escitalopram,
    fluvoxamine, fluoxetine, milnacipran, levomilnacipran, paroxetine, sertraline,
    venlafaxine, desvenlafaxine at a stable dose (at therapeutic dose level) for at least
    6 weeks, and for no greater than 12 months in the current episode, at screening.
    The SSRI/SNRI needs to be approved for the treatment of MDD.
    9. HDRS-17 total score ≥22 at start of the screening and must not demonstrate a
    clinically significant improvement (which is defined as an improvement of >20%
    on their HDRS-17 total score) from the start to end of screening (from the
    first to the last independent HDRS-17 rating).
    10. BMI between 18 and 40 kg/m2 (inclusive).
    11. Outpatient at screening.
    12. A woman of childbearing potential must have a negative highly sensitive serum
    (β human chorionic gonadotropin [β-hCG]) pregnancy test at screening and a
    negative urine pregnancy test predose on Day 1 of the double-blind phase prior
    to randomization.
    13. Contraceptive use by men or women should be consistent with local regulations
    regarding the use of contraceptive methods for subjects in clinical studies.
    14. A woman must be either:
    Postmenopausal: A postmenopausal state is defined as no menses for 12
    months without an alternative medical cause. A high FSH level in the
    postmenopausal range based on the reference range of the central
    laboratory may be used to confirm a postmenopausal state in women not
    using hormonal contraception or hormonal replacement therapy,
    however in the absence of 12 months of amenorrhea, a single FSH
    measurement is insufficient.
    Permanently sterile
    Of childbearing potential and practicing a highly effective method of
    contraception (failure rate of <1% per year when used consistently and
    correctly).
    Remains on a highly effective method and for at least 1 month after the
    last dose of study medication.
    A woman must not donate eggs (ova, oocytes) or freeze for future use for
    the purposes of assisted reproduction during the study and for a period of
    at least 1 month after receiving the last dose of study medication.
    During the study and for a minimum of 1 spermatogenesis cycle (defined
    as approximately 3 months) after receiving the last dose of study
    medication, a man (a) who is sexually active with a woman of
    childbearing potential must use a barrier method of contraception and his
    female partner must use a highly effective method of contraception; (b)
    who is sexually active with a woman who is pregnant must use a condom;
    (c) must not donate sperm.
  • Exclusion Criteria:
    1. History of treatment-resistant MDD, defined as a lack of response to 2 or more
    adequate antidepressant treatments in the current episode, as indicated by no or
    minimal improvement (≤25% improvement) when treated with an antidepressant of
    adequate dose (per MGH-ATRQ) and duration (at least 6 weeks).
    2. Current or prior DSM-5 diagnosis of a psychotic disorder or MDD with psychotic
    features, bipolar or related disorders (confirmed by the SCID-CT), intellectual
    disability (DSM-5 diagnostic codes 317, 318.0, 318.1, 318.2, 315.8, and 319),
    autism spectrum disorder, borderline personality disorder, antisocial personality
    disorder, histrionic personality disorder, narcissistic personality disorders or
    somatoform disorders.
    3. Current active DSM-5 diagnosis of obsessive-compulsive disorder, post-traumatic
    stress disorder, anorexia nervosa, or bulimia nervosa.
    4. Primary DSM-5 diagnosis of panic disorder, generalized anxiety disorder, social
    anxiety disorder, or specific phobia which has been the primary focus of psychiatric
    treatment within the past 2 years. These are allowed as secondary diagnoses if MDD
    is the primary focus of treatment.
    5. History or evidence of clinically
    meaningful noncompliance with current
    antidepressant therapy.
    6. History of moderate to severe substance use disorder including alcohol use disorder
    according to DSM-5 criteria within 6 months before screening or positive test results
    for alcohol and/or drugs of abuse (e.g., opiates [including methadone], cocaine,
    amphetamines, methamphetamines, cannabinoids, CBD, barbiturates, MDMA) at
    screening or at baseline. One retest during screening is allowed. Tobacco and
    caffeine use are not exclusionary.
    7. Has within the last 5 years received any prior antidepressant treatment with
    ketamine/esketamine, electroconvulsive therapy, vagal nerve stimulation, or a deep
    brain stimulation device. Subjects who previously had taken up to 2 doses of
    ketamine/esketamine and did not continue (e.g., did not benefit from the treatment
    or experienced tolerability issues) can be considered for enrollment.
    8. Homicidal ideation/intent or has suicidal ideation with some intent to act within 3
    months prior to the start of the screening phase, per clinical judgment or based on
    the C-SSRS, corresponding to a response of “Yes” on Item 4 (active suicidal ideation
    with some intent to act, without specific plan) or Item 5 (active suicidal ideation with
    specific plan and intent) for suicidal ideation on the C-SSRS, or a history of suicidal
    behavior within the past year prior to the start of the screening phase. Subjects
    reporting suicidal ideation with intent to act or suicidal behavior prior to the start of
    the double-blind treatment phase should be excluded.
    9. Cognitive impairment that would render the informed consent invalid or limit the
    ability of the subject to comply with the study requirements. Subject has
    neurodegenerative disorder (e.g., Alzheimer's disease, vascular dementia,
    Parkinson's disease with clinical evidence of cognitive impairment) or evidence of
    MCI. Subjects of age ≥65 years: has a MMSE <25 or <23 for those subjects with
    less than high school equivalent education.
    10. Current or history of seizures (uncomplicated childhood febrile seizures with no
    sequelae are not exclusionary).
    11. Clinically significant electrocardiogram (ECG) abnormalities at screening or Day
    1 prior to randomization that may jeopardize the subjects' safety or the integrity of
    the study defined as:
    During screening and/or Day 1, a QT interval corrected according to
    Fridericia's formula (QTcF): ≥450 msec (males); ≥470 msec (females).
    Evidence of second- and third-degree atrioventricular block.
    Features of new ischemia.
    Other clinically important arrhythmia or cardiac abnormalities.
    12. History of, or symptoms and signs suggestive of, liver cirrhosis (e.g., esophageal
    varices, ascites, and increased prothrombin time) OR ALT or AST values ≥3 × the
    ULN or total bilirubin >1.5 × the ULN in the screening phase. Repeat of screening
    test for abnormal ALT and AST is permitted during the screening period provided
    there is an alternative explanation for the out of range value.
    13. For elevations in bilirubin if the elevation in bilirubin is consistent with Gilbert's
    disease, the subject may participate in the study.
    14. Positive test results for drugs of abuse (e.g., barbiturates, methadone, opiates,
    cocaine, PCP, MDMA, and amphetamine/methamphetamine) at the start of the
    screening phase or Day 1 of the double-blind treatment phase prior to randomization.
    15. Subjects who have a positive test result at screening due to prescribed
    psychostimulants taken for any indication must discontinue the medication at least
    2 weeks before Day 1 of the double-blind treatment phase (prior to randomization).
    The result of the Day 1 (prior to randomization) test for drugs of abuse must be
    negative for the subject to be randomized. Otherwise, subjects who have a positive
    test result at screening due to prescribed/over-the-counter opiates or barbiturates
    may be permitted to continue in the screening phase if the medication is discontinued
    at least 1 week or 5 half-lives, whichever is longer, before Day 1 of the double-blind
    treatment phase (prior to randomization). The result of the Day 1 (prior to
    randomization) test for drugs of abuse must be negative for the subject to be
    randomized.
    16. Intermittent use of cannabinoids prior to the start of the screening phase is not
    exclusionary as long as the subject does not meet the criteria for substance use
    disorder. A positive test for cannabinoids at the start of the screening phase is not
    exclusionary; however, a positive test result for cannabinoids predose on Day 1 of
    the double-blind treatment phase is exclusionary.
    17. Taking a total daily dose of benzodiazepines greater than the equivalent of 6 mg/day
    of lorazepam at the start of the screening phase.
    18. Recent (last 3 months) history of, or current signs and symptoms of:
    Severe renal insufficiency (creatinine clearance <30mL/min)
    Clinically significant or unstable
    cardiovascular,
    respiratory,
    gastrointestinal, neurologic, hematologic, rheumatologic, immunologic or
    endocrine disorders.
    Uncontrolled Type 1 or Type 2 diabetes mellitus. Subjects with Type 1 or
    Type 2 diabetes mellitus who are controlled (hemoglobin Alc ≤8.0% and
    glucose ≤150 mg/dL at screening) may be eligible to participate if
    otherwise medically healthy, and if on a stable regimen of glucose-
    lowering medications for at least 2 months prior to screening).
    19. Current signs/symptoms of hypothyroidism or hyperthyroidism. For subjects with a
    history of thyroid disease and for subjects who, regardless of thyroid history have
    the TSH value out of range, a FT4 test will be conducted. If the FT4 value is
    abnormal and considered to be clinically significant the subject is not eligible.
    20. Subjects with a pre-existing history of thyroid disease/disorder who are treated with
    thyroid hormones need to be on a stable dosage for 3 months prior to the start of the
    screening phase. Subjects taking thyroid supplementation for antidepressant
    purposes are not allowed.
    21. Cushing's Disease, Addison's Disease, primary amenorrhea, or other evidence of
    significant medical disorders of the hypothalamic-pituitary-adrenal axis.
    22. Significant medical illness, particularly unstable medical problem
    23. Ongoing psychological treatments (e.g., Cognitive Behavior Therapy, Interpersonal
    Psychotherapy, Psychodynamic Psychotherapy etc.), initiated within 6 weeks prior
    to start of screening. A subject who has been receiving ongoing psychological
    treatment for a period of greater than 6 weeks is eligible.
    24. Significant medical illness, particularly unstable medical problem.
    25. Clinically-relevant GI complaints (unless symptoms of Axis I disorder) at screening
    or baseline or history of gastric disease (including but not limited to documented
    peptic ulcer disease, gastritis [including atrophic gastritis], upper GI bleeding,
    Barret's esophagus, Crohn's disease, ulcerative colitis, GI precancerous conditions
    or any other clinically-relevant GI disease irritable bowel syndrome).
    26. Requires chronic use of a PPIs. A history of chronic NSAID or aspirin use. (Low
    dose aspirin e.g., in cardiovascular disease prevention is allowed).
    27. History of malignancy within 5 years before the start of the screening phase
    (exceptions are squamous and basal cell carcinomas of the skin and carcinoma in
    situ of the cervix, or malignancy that is considered cured with minimal risk of
    recurrence).
    28. Known allergies, hypersensitivity, intolerance, or contraindications to aticaprant
    and/or its excipients.
    29. Has taken any prohibited therapies that would not permit dosing on Day 1.
    30. Taking a total daily dose of benzodiazepines greater than the equivalent of 6 mg/day
    of lorazepam at the start of the screening phase.
    31. Received an investigational drug (including investigational vaccines) or used an
    invasive investigational medical device within 60 days before the start of the
    screening phase, or has participated in 2 or more MDD or other psychiatric condition
    clinical interventional studies (with different investigational medication) in the
    previous 1 year before the start of the screening phase, or is currently enrolled in an
    investigational interventional study.
    32. A woman who is pregnant, breastfeeding, or planning to become pregnant while
    enrolled in this study or within 6 weeks after the last dose of the study medication.
    33. Plans to father a child while enrolled in this study or within 90 days after the last
    dose of study intervention.
    34. Diagnosis of acquired immunodeficiency syndrome. Human immunodeficiency
    virus testing is not required for this study.
    35. Any condition or situation/circumstance for which participation would not be in the
    best interest of the subject (e.g., compromise the well-being) or that could prevent,
    limit, or confound the protocol specified assessments.
  • A. Efficacy Objectives and Endpoints
  • The assessment of primary and secondary (key and other) endpoints will be conducted on the full analysis set (FAS) which includes adult (not elderly) subjects with MDD with prominent anhedonia who took at least 1 dose of study medication.
  • Primary: Evaluate the efficacy of 2 fixed doses of aticaprant (5 mg and 10 mg) compared with placebo as adjunctive therapy to an antidepressant (SSRI or SNRI) in improving depressive symptoms in adult subjects (18-64 years) with MDD with prominent anhedonia and inadequate response to the current antidepressant Change from baseline to Day 43 in the MADRS total score.
  • Key Secondary: To assess efficacy of aticaprant 10 mg compared with placebo in adult subjects with MDD with prominent anhedonia as adjunctive therapy to an antidepressant on patient-reported assessment of anhedonia outcomes:
      • Change from baseline to Day 43 in the Dimensional Anhedonia Rating Scale (DARS) total score.
  • Other Secondary: Assess the efficacy of aticaprant compared with placebo as adjunctive therapy to an antidepressant (SSRI or SNRI) in adult subjects with MDD with prominent anhedonia:
      • Proportion of responders at Day 43 and Day 57 (≥50% reduction in MADRS total score).
      • Proportion of subjects with remission of depressive symptoms, defined as a MADRS total score ≤12 at Day 43 and Day 57.
      • Change from baseline to Day 43 and Day 57 in MADRS-6
      • Change from baseline to Day 43 and Day 57 in Patient Health Questionnaire, 9-Item (PHQ-9) total score.
  • Exploratory: To assess the efficacy of aticaprant compared with placebo in adult subjects with MDD with prominent anhedonia as adjunctive therapy on the following:
      • Change from baseline over time in the MADRS total score.
      • Change from baseline over time in MADRS anhedonia items factor score.
      • Change from baseline over time in patient-reported outcomes of anhedonia (SHAPS, DARS).
      • Change from baseline over time in PHQ-9 total score.
      • Change from baseline to Day 43 in health-related quality of life and health status, as assessed by the EQ-5D-5L questionnaire.
      • Change from baseline to Day 43 in the Sheehan Disability Scale (SDS) total score.
      • Change from baseline over time in the CGI-S score.
      • Change from baseline over time in symptoms of anxiety using the GAD-7.
      • Change from baseline over time in depressive symptoms using the PGI-S.
      • Change from baseline to Day 43 in patient-reported sexual functioning using the ASEX.
  • Safety Objectives (All): The following safety endpoints will be assessed separately for the adult and elderly subjects; the safety analysis set for each age group will include all randomized subjects who have received at least one dose of study medication:
      • AEs including AESI
      • Vital signs
      • ECG
      • Laboratory Values
      • Weight/BMI
      • Suicidality assessment using the C-SSRS
      • Withdrawal symptoms assessment using the PWC-20
  • Other Objectives (Exploratory):
      • To identify diagnostic biomarkers and to investigate changes in MDD-related biomarkers in relation to clinical response on depression symptoms and anhedonia upon monotherapy with aticaprant.
      • To identify genetic and other factors that may influence the pharmacokinetics (PK), safety, or tolerability of aticaprant.
  • B. Concomitant Therapies and Prohibited Therapies
  • Background therapy: All subjects will continue their baseline antidepressant (SSRI/SNRT) during the entire study. The following antidepressants are permitted: citalopram, duloxetine, escitalopram, fluvoxamine, fluoxetine, milnacipran, levomilnacipran, paroxetine, sertraline, venlafaxine, and desvenlafaxine. Subjects will only continue one of these allowed antidepressants at an adequate and tolerated dose (i.e., monotherapy) during the study. No changes in antidepressant or dose are permitted from screening until the end of the study.
  • Prohibited Therapies:
  • Subjects must not use the following medications or food supplements prior to or during the study, as indicated, except to treat an AE or breakthrough symptoms, preferably after the EOT visit:
      • MAOIs within 4 weeks before screening until the first follow-up visit.
      • Antipsychotic drugs from at least 14 days before Day 1 until the first follow-up visit.
      • Hypnotic drugs or food supplements (from at least 7 days prior to Day 1 until the first follow-up visit), including but not limited to benzodiazepines, non-benzodiazepine hypnotics (e.g., zolpidem, zopiclone, zaleplon, eszopiclone, suvorexant and ramelteon), sedating antihistamines including over-the-counter hypnotics (e.g., diphenhydramine, doxylamine, and hydroxyzine), and melatonin. Subjects who were taking benzodiazepines and/or permitted non-benzodiazepine sleep medications during the screening phase can continue these medications (at dosages equal to or less than the equivalent of 6 mg/day of lorazepam) during the double-blind treatment phase. No dose increases beyond the equivalent of 6 mg/day of lorazepam, or new benzodiazepine medications are permitted during the double-blind treatment phase.
      • Non-SSRI/SNRI antidepressants (e.g., doxepin, trazodone, mirtazapine, bupropion, tricyclic antidepressants, agomelatine, and SAMe) from at least 7 days before Day 1 until the first follow-up visit.
      • Any form of new psychotherapy or change in current psychotherapy is prohibited during the screening and double-blind phase of this study.
      • Opiates and mood stabilizers (e.g., lithium and anticonvulsants) from at least 7 days prior to Day 1 until the first follow-up visit.
      • Stimulants (e.g., dexamphetamine, methylphenidate, dexmethylphenidate), oral systemic steroids, and appetite suppressants (ephedrine), and isoxsuprine from at least 7 days before Day 1 until EOT.
      • Magnetic and electrical stimulation therapies: electroconvulsive therapy, vagal nerve stimulation, deep brain stimulations, TMS of any type, or DCS or electrical stimulation, from screening to End-of-Study visit. TMS or DCS or electrical stimulation use prior to screening is not exclusionary.
      • T3, thyroid hormone or other thyroid function supplementation prescribed for depression. These medications are allowed when given to control pre-existing thyroid disease/disorder.
      • Ketamine or esketamine within 5 years prior to and during the study (up to 2 doses are allowed in lifetime prior to screening).
      • Psychedelics (e.g., psilocybin).
      • Memantine.
      • Other investigational drugs within 30 days prior to and during the study.
    Example 9
  • This is a Phase 1, open-label, single dose, multicenter, 4-part study in healthy adult participants.
  • A total of approximately 80 qualified healthy adult participants are planned to be enrolled in this study: 24 participants each are to be enrolled to ensure at least 20 participants in each part complete all required PK assessments. Eligible participants can be enrolled in more than one part of the study if sufficient wash-out period is completed between periods by participants.
  • Potential participants will be screened from Day −28 to Day −2 to determine participants' eligibility for study participation. For Part 1, qualified participants will be admitted on Day −1 of each treatment period and will remain in-house for the total duration of the treatment (Day −1 until Day 5, with single-dose treatment on Day 1 and 96 hours of PK), whereas for Part 2, PK sampling will be done up to 120 hours (Day 6). Each dosed participant will have a safety follow-up on Day 10 to Day 14 after last dose of the study intervention.
  • Part 1
  • The Part 1 of the study involves determination of relative bioavailability for tablet (Formulation Concept 1, i.e., unmilled aticaprant formulation, see Table 10) and capsule formulations (see Example 6, study design, for description of capsule formulation) and dose proportionality and food effect for tablet formulation (Formulation Concept 1) in healthy adult participants (FIG. 25 ). Part 1 will consist of Subpart 1A and Subpart 1B consisting of a total of 4 periods. Subpart 1A is a randomized, open label, 3-way crossover, 3-period study to be conducted in 24 healthy participants to evaluate the relative bioavailability of a single dose of 10 mg aticaprant administered as 1×10 mg oral tablet (Formulation Concept 1) under fasted conditions (Treatment B) compared to 10 mg aticaprant administered as 2×5 mg oral capsules under fasted conditions (Treatment A) and to evaluate the dose proportionality of a single dose of 5 mg aticaprant administered as 1×5 mg oral tablet (Formulation Concept 1) under fasted conditions (Treatment C) compared to the potential Phase 3 oral tablet (Formulation Concept 1) under fasted conditions (1×10 mg, Treatment B; Table 49). Participants will be assigned to 1 of 6 treatment sequences (Table 51) and will be administered the 3 treatments in a 3-way crossover. The same 24 participants who complete Subpart 1A will be enrolled in Subpart 1B. Subpart 1B consists of a fourth period to evaluate the food effect of a single dose of 10 mg aticaprant administered as 1×10 mg oral tablet (Formulation Concept 1) under fed conditions (Treatment D; Table 50 and Table 52). A preliminary PK analysis will be conducted at the end of the food effect part (Subpart 1B) for all the periods from Part 1 and will include the food effect data.
  • TABLE 49
    Study Treatment Regimens in Subpart 1A
    Treatment Formulation Dose Food
    A
    5 mg oral capsule 10 mg (2 × 5 mg)  Fasted
    B Formulation Concept 1 10 mg (1 × 10 mg) Fasted
    (10 mg oral tablet)
    C Formulation Concept 1 5 mg (1 × 5 mg) Fasted
    (5 mg oral tablet)
    Treatment A: 2 × 5 mg oral capsule administered in the morning, after at least 10-hour overnight fasting
    Treatment B: 1 × 10 mg Formulation Concept 1 administered in the morning, after at least 10-hour overnight fasting
    Treatment C: 1 × 5 mg Formulation Concept 1 administered in the morning, after at least 10-hour overnight fasting
  • TABLE 50
    Study Treatment Regimen in Subpart 1B
    Treatment Formulation Dose Food
    D Formulation Concept 1 10 mg Fed
    (10 mg oral tablet) (1 × 10 mg)
    Treatment D: 1 × 10 mg Formulation Concept 1 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
  • TABLE 51
    Treatment Sequences in Subpart 1A
    Treatment Periods
    Sequence
    1 2 3
    Sequence 1 (n = 4) A B C
    Sequence 2 (n = 4) B C A
    Sequence 3 (n = 4) C A B
    Sequence 4 (n = 4) A C B
    Sequence 5 (n = 4) B A C
    Sequence 6 (n = 4) C B A
    Treatment A: 2 × 5 mg oral capsule administered in the morning, after at least 10-hour overnight fasting;
    Treatment B: 1 × 10 mg Formulation Concept 1 administered in the morning, after at least 10-hour overnight fasting
    Treatment C: 1 × 5 mg Formulation Concept 1 administered in the morning, after at least 10-hour overnight fasting
  • TABLE 52
    Treatment Sequence in Subpart 1B
    Treatment Period
    Sequence
    4
    All Sequences from D
    Subpart 1A (n = 24)
    Treatment D: 1 × 10 mg Formulation Concept 1 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
  • Primary Objectives:
      • To evaluate the relative oral bioavailability of potential Phase 3 tablet concept formulations (unmilled API formulation concept; 1×10 mg) compared with the oral capsule formulation (2×5 mg) of aticaprant when administered as a single oral dose of 10 mg aticaprant in healthy adult participants under fasting conditions.
      • To evaluate the dose proportionality of potential Phase 3 tablet concept formulation (unmilled API formulation concept; 1×5 mg) relative to the potential Phase 3 tablet concept formulation (unmilled API formulation concept; 1×10 mg) of aticaprant when administered in healthy adult participants under fasting conditions.
      • To evaluate the PK of a single oral dose of potential Phase 3 tablet concept formulation (unmilled API formulation concept; 1×10 mg) of aticaprant in healthy adult participants under fasting and fed (high-fat meal) conditions.
  • Secondary Objectives:
      • To assess the safety and tolerability of oral doses of aticaprant in healthy adult participants.
  • Part 2
  • The Part 2 of the study involves determination of relative bioavailability for tablet (Formulation Concept 2, i.e., milled (microfine) aticaprant formulation; see Table 10) and capsule formulations (see Example 6, study design, for description of capsule formulation) and dose proportionality and food effect for tablet formulation (Formulation Concept 2) in healthy adult participants (FIG. 26 ). Part 2 will consist of Subpart 2A and Subpart 2B consisting of a total of 4 periods. Subpart 2A is a randomized, open label, 3-way crossover, 3-period study to be conducted in 24 healthy participants to evaluate the relative bioavailability of a single dose of 10 mg aticaprant administered as 1×10 mg oral tablet (Formulation Concept 2) under fasted conditions (Treatment F) compared to 10 mg aticaprant administered as 2×5 mg oral capsules under fasted conditions (Treatment E) and to evaluate the dose proportionality of a single dose of 5 mg aticaprant administered as 1×5 mg oral tablet (Formulation Concept 2) under fasted conditions (Treatment G) compared to the potential Phase 3 oral tablet (Formulation Concept 2) under fasted conditions (1×10 mg, Treatment F; Table 53). Participants will be assigned to 1 of 6 treatment sequences (Table 55) and will be administered the 3 treatments in a 3-way crossover. The same 24 participants who complete Subpart 2A will be enrolled in Subpart 2B. Subpart 2B consists of a fourth period to evaluate the food effect of a single dose of 10 mg aticaprant administered as 1×10 mg oral tablet (Formulation Concept 2) under fed conditions (Treatment H; Tables 54 and 56). A preliminary PK analysis will be conducted at the end of the food effect part (Subpart 2B) for all the periods from Part 2 and will include the food effect data.
  • TABLE 53
    Study Treatment Regimens in Subpart 2A
    Treatment Formulation Dose Food
    E
    5 mg oral capsule 10 mg (2 × 5 mg)  Fasted
    F Formulation Concept 2 10 mg (1 × 10 mg) Fasted
    (10 mg oral tablet)
    G Formulation Concept 2 5 mg (1 × 5 mg) Fasted
    (5 mg oral tablet)
    Treatment E: 2 × 5 mg oral capsule administered in the morning, after at least 10-hour overnight fasting
    Treatment F: 1 × 10 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting
    Treatment G: 1 × 5 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting
  • TABLE 54
    Study Treatment Regimen in Subpart 2B
    Treatment Formulation Dose Food
    H Formulation Concept 2 10 mg Fed
    (10 mg oral tablet) (1 × 10 mg)
    Treatment H: 1 × 10 mg Formulation Concept 2 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
  • TABLE 55
    Treatment Sequences in Subpart 2A
    Treatment Periods
    Sequence
    1 2 3
    Sequence 1 (n = 4) E F G
    Sequence 2 (n = 4) F G E
    Sequence 3 (n = 4) G E F
    Sequence 4 (n = 4) E G F
    Sequence 5 (n = 4) F E G
    Sequence 6 (n = 4) G F E
    Treatment E: 2 × 5 mg oral capsule administered in the morning, after at least 10-hour overnight fasting
    Treatment F: 1 × 10 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting
    Treatment G: 1 × 5 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting
  • TABLE 56
    Treatment Sequences in Subpart 2B
    Treatment Period
    Sequence
    4
    All Sequences from E
    Subpart 2A (n = 24)
    Treatment H: 1 × 10 mg Formulation Concept 2 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
  • Primary Objectives:
      • To evaluate the relative oral bioavailability of potential Phase 3 tablet concept formulations (milled aticaprant formulation concept; 1×10 mg) compared with the oral capsule formulation (2×5 mg) of aticaprant when administered as a single oral dose of 10 mg aticaprant in healthy adult participants under fasting conditions.
      • To evaluate the dose proportionality of potential Phase 3 tablet concept formulation (milled API formulation concept; 1×5 mg) relative to the potential Phase 3 tablet concept formulation (milled aticaprant formulation concept; 1×10 mg) of aticaprant when administered in healthy adult participants under fasting conditions.
      • To evaluate the PK of a single oral dose of potential Phase 3 tablet concept formulation (milled aticaprant formulation concept; 1×10 mg) of aticaprant in healthy adult participants under fasting and fed (high-fat meal) conditions.
  • Additional Points
  • For each individual participant, there will be a washout period of at least 7 days for Part 1 and at least 8 days for Part 2 between subsequent intakes of the study intervention. Day 1 of a treatment period (day of study intervention intake) is the first day of the washout period (also in between the study parts, if applicable).
  • Participants will be fasting in Part 1A and Part 2A. Participants will have been fed in Parts 1B and 2B. For a fasted condition, participants will fast (nothing to eat or drink except noncarbonated water) overnight for at least 10 hours before and until 4 hours after study intervention administration during each fasted treatment period. Approximately, 4 hours post-dose and after the 4-hour PK sampling, a standard lunch will be served at the study-site. Intake of water is allowed until 2 hours before the intake of the study intervention. Thereafter, water intake is only allowed for study intervention intake and for breakfast, if applicable. Drinking of water is allowed ad libitum from approximately 2 hours after dosing. For a fed condition, participants will consume, after an overnight fast (at least 10 hours), a standardized high-fat breakfast within a 20-minute period. A high-fat (approximately 50 percent of total caloric content of the meal) and high-calorie (approximately 800 to 1000 calories) meal is recommended for food effect bioavailability studies (e.g., 2 strips of fried bacon, 2 eggs fried in butter, 4 ounces [120 gram] hash brown potatoes fried in butter, 2 buttered pieces of whole wheat bread, and 240 mL whole milk). Study intervention will be administered approximately 30 minutes after the start of the breakfast.
  • In Parts 1 and 2, plasma concentrations will be determined for aticaprant. Blood samples for determination of plasma concentrations of aticaprant will be collected predose and at the postdose time points starting on Day 1 as indicated in the Tables 57-58.
  • Parts 1 and 2, of the study will start at any time, irrespective of other parts of the study.
  • For Parts 1 and 2, the study will consist of a screening phase (within 28 days before study intervention administration), an open-label treatment phase (Day −1 until Day 5, with single-dose treatment on Day 1 and at least 96 hours of PK for Part 1 and 120 hours of PK (Day 6) for Part 2).
  • TABLE 57
    Part 1 Schedule of Activities
    Open-Label (washout of 7 days between each administration of
    Phase Screening study intervention) For Part 1: Periods 1-4
    Study Day Days −28 Day
    to −2 −1 Day 1
    Time Predose −30 m 0 +30 m +1 h +1 h 30 m +2 h +2 h 30 m +3 h +4 h +6 h +8 h +12 h
    Inclusion/exclusion X X
    criteria
    Medical history X
    Demographic X
    information
    Physical X X
    examination
    Height X
    Weight X X
    BMI X
    Body temperature X X
    12-Lead ECGa X X X X X
    Vital signs (supine X X X X
    BP, pulse / heart
    rate)a,o
    Serology (HIV, X
    HBsAg, and hepatitis
    C virus antibody)
    Urine drug screen X X
    Alcohol screenp X X
    Urine cotinine test X X
    Hematology, X X
    chemistry, and
    urinalysisª
    Suicidality by C- X X
    SSRSa,k
    Severe acute X
    respiratory
    syndrome coronavirus
    2 (SARS-COV-2) testj
    FSHf X
    Serum beta-HCGb X
    Urine pregnancy X
    testb
    Admission to X
    clinical unit
    Randomization to X
    sequencec
    High-fat breakfastd X
    Oral dose aticaprante X
    Blood sample for X XXXX X X X XX X
    PK; sample for
    aticaprantª
    Lunchg X
    Residence in Continuous
    clinical unit
    Adverse events Continuous
    Concomitant Continuous
    medication
  • TABLE 57
    Part 1 Schedule of Activities
    Phase Open-Label (washout of 7 days between each End-of-Study (Day 10
    administration of study intervention) For to Day 14) or Early
    Part 1: Periods 1-4 Withdrawal
    Study Day Day 2 Day 3 Day 4 Day 5
    Time +24 h +36 h +48 h +60 h +72 h +96 h
    Physical examination X
    Weight X X
    Body temperature X X
    12-Lead ECGa X X X
    Vital signs (supine BP, X X X X
    pulse/heart rate )a,o
    Hematology, chemistry, and X X X
    urinalysisª
    Suicidality by C-SSRSa,k X X
    Serum beta-HCGb X
    Blood sample for PK; sample X X X X X X
    for aticapranta
    Discharge from clinical unit X
    Residence in clinical unit Continuous
    Adverse events Continuous
    Concomitant medication Continuous
  • TABLE 58
    Part 2 Schedule of Activities
    Phase Screening Open-Label (washout of 8 days between each administration of study
    intervention) For Part 2: Periods 1-4
    Study Day Days − Day
    28 −1
    to −2 Day 1
    Time Predose −30 m 0 +30 m +1 h +1 h 30 m +2 h +2 h 30 m + +3 h +4 h +6 h +8 h +12 h
    Inclusion/exclusion X X
    criteria
    Medical history X
    Demographic X
    information
    Physical X X
    examination
    Height X
    Weight X X
    BMI X
    Body temperature X X
    12-Lead ECGa X X X X X
    Vital signs (supine X X X X
    BP, pulse / heart
    rate)a,o
    Serology (HIV, X
    HBsAg, and hepatitis
    C virus antibody)
    Urine drug screen X X
    Alcohol screenp X X
    Urine cotinine test X X
    Hematology, X X
    chemistry, and
    urinalysis(a)
    Suicidality by C- X X
    SSRSa,k
    Severe acute X
    respiratory syndrome
    coronavirus 2
    (SARS-COV-2) testj
    ESHf X
    Serum beta-HCGb X
    Urine pregnancy X
    testb
    Admission to X
    clinical unit
    Randomization to X
    sequencec
    High-fat breakfastd X
    Oral dose X
    aticaprante
    Blood sample for X X X X X X X X X x X
    PK; sample for
    aticaprantª
    Lunchg X
    Residence in Continuous
    clinical unit
    Adverse events Continuous
    Concomitant Continuous
    medication
  • TABLE 58
    Part 2 Schedule of Activities
    Phase Open-Label (washout of 8 days between each End-of-Study (Day 10
    administration of study intervention) For Part 2: Periods 1- to Day 14) or
    4 Early Withdrawal
    Study Day Day 2 Day 3 Day 4 Day 5 Day 6
    Time 4 h +2 6 h +3 8 h + 4 0 h + 6 2 h + 7 6 h + 9 0 h + 12
    Physical X
    examination
    Weight X X X
    Body temperature X X X
    12-Lead ECGa X X X X X
    Vital signs (supine X X X X X
    BP, pulse / heart
    rate )ao
    Hematology, X X X
    chemistry, and
    urinalysisª
    Suicidality by C- X X
    SSRSask
    Serum beta-HCG b X
    Blood sample for PK; X X X X X X X
    sample for aticapranta
    Discharge from X
    clinical unit
    Residence in clinical Continuous
    unit
    Adverse events Continuous
    Concomitant Continuous
    medication
  • For Tables 57-58:
      • (a) When scheduled procedures coincide, they should preferably take place in the following order: 12-lead ECG, vital signs (supine blood pressure, pulse/heart rate), blood/CSF draws for PK, or laboratory measurements, and C-SSRS.
      • (b) For all female participants.
      • (c) Period 1 only.
      • (d) Only in the period with dosing in fed condition. Standardized high-fat breakfast should be consumed within a 20-minute period.
      • (e) After at least 10-hour overnight fasting, study intervention will be administered in the morning in fasting condition where dosing is under fasting condition and 30 minutes after breakfast for the periods where dosing is under fed condition.
      • (f) For all postmenopausal women, FSH is done to confirm post-menopausal state in women without an alternative medical cause.
      • (g) After collection of the 4-hour PK blood sample and/or CSF sample.
      • (h) 6 mL additional blood will be collected prior to dosing in each participant for experimental work related to protein binding of parent and metabolites.
      • (i) Additional severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) tests may be performed per site-specific guidelines or practice.
      • (j) There are 2 versions of the C-SSRS. A baseline/screening version of the C-SSRS will be completed at screening, and subsequently a since-your-last-visit version of the C-SSRS will be completed predose on Day −1, prior to discharge on Day 5 of each treatment period (for Part 1) and prior to discharge on Day 6 of each treatment period (for Part 2), and at end-of-study or early withdrawal.
      • (k) After discharge from clinic, participants may be contacted telephonically for assessment of adverse events.
      • (l) Free as well as total plasma concentrations of aticaprant will be assayed.
      • (m)
      • (n) Blood pressure, pulse/heart rate, and respiratory rate will be measured after 5 minutes rest in a supine position.
      • (o) Either urine alcohol test or alcohol breath test will be used for alcohol screen per site-specific guidelines or practice.
      • (p) Prior to the insertion of the spinal catheter.
      • (q) Catheter tip will be used for culture analyses whenever a catheter is kept in a place for more than 24 hours.
  • A. Study Population
  • A total of approximately 80 qualified healthy adult participants are planned to be enrolled in this study: 24 participants each are to be enrolled in Parts 1 and 2 to ensure at least 20 participants in each part complete all required PK assessments. Eligible participants can be enrolled in more than one part of study if sufficient wash-out period is completed between periods by participants.
  • Screening for eligible participants will be performed within 28 days before administration of the study intervention.
  • (i) Inclusion Criteria
  • Each potential participant must satisfy all of the following criteria to be enrolled in the study:
      • For all Participants
  •
    Age
    Healthy male and female participants between 18 and 55 years of age,
    inclusive.
    Type of Participant and Disease Characteristic
    Healthy on the basis of physical examination, medical history (screening
    only), vital signs, and 12-lead ECG performed at screening and admission
    to the clinical unit on Day −1 of the first treatment period. Minor
    abnormalities in ECG, which are not considered to be of clinical
    significance are acceptable.
    Healthy on the basis of clinical laboratory tests performed at screening
    and at admission to the study center. If the results of the serum chemistry
    panel, hematology, or urinalysis are outside the normal reference ranges,
    the participant may be included. If the results of the serum chemistry
    panel, hematology, or urinalysis are outside the normal reference ranges,
    retesting of an abnormal lab value(s) that may lead to exclusion will be
    allowed once during the screening phase. At screening and baselinr
    (Period 1, Day −1), ALT, AST, alkaline phosphatase and bilirubin must
    be within 1.5 times of upper limit of normal range and not clinically
    significant.
    Weight
    BMI (weight [kg]/height2 [m]2) between 18 and 29.9 kg/m2 (inclusive),
    and body weight not less than 50 kg.
    Sex and Contraceptive/Barrier Requirements
    Male or female
    All women participants must have a negative highly sensitive serum
    β-hCG pregnancy test at screening and all women participants must have
    a negative urine pregnancy test on Day −1 of each treatment period.
    A woman must be
    a. Not of childbearing potential
    b. Of childbearing potential and
     Practicing a highly effective method of contraception (failure rate
    of <1% per year when used consistently and correctly) and agrees to
    remain on a highly effective method while receiving study intervention
    and until 90 days after last dose - the end of relevant systemic exposure.
    A woman must agree not to donate eggs (ova, oocytes) or freeze for future
    use for the purposes of assisted reproduction during the study and for a
    period of at least 90 days after receiving the last dose of study
    intervention.
    During the study and for a minimum of 1 spermatogenesis cycle (defined
    as approximately 3 months) after receiving the last dose of study
    intervention:
    A male participant must agree to use a barrier method of contraception
    (e.g., condom) when engaging in any activity that allows for passage of
    ejaculate to another person.
    A male participant who is sexually active with a woman who is pregnant
    must use a condom.
    Male participants should also be advised of the benefit for a female
    partner to use a highly effective method of contraception as condom
    may break or leak.
    A male participant must agree not to donate sperm for the purpose of
    reproduction during the study and for a minimum of 1 spermatogenesis
    cycle (defined as approximately 3 months) after receiving the last
    dose of study intervention.
  • Other Inclusions
  •
    Blood pressure (after the participant is [supine] for 5 minutes) between
    90 mmHg and 140 mmHg systolic, inclusive, and no higher than 90
    mmHg diastolic at screening and Day −1 of each treatment period.
    A 12-lead ECG consistent with normal cardiac conduction and function, at
    screening and Day −1 of each treatment period, including:
    Sinus rhythm
    Heart rate between 40 and 100 beats per minute, extremes included
    QTc interval ≤450 ms for males, ≤470 for females (corrected cf.
    Fridericia 1920; ICH E14 2005)
    QRS interval of <120 ms
    PR interval <210 ms
    Morphology consistent with healthy cardiac conduction and function
  • (ii) Exclusion Criteria
  • Any potential participant who meets any of the following criteria will be excluded from participating in the study:
  • For all Participants:
  •
    Medical Conditions
    History of or current significant medical illness including (but not
    limited to) cardiac arrhythmias or other cardiac disease,
    hematological disease, lipid abnormalities, bronchospastic
    respiratory disease, diabetes mellitus, renal or hepatic
    insufficiency, thyroid disease, neurologic or psychiatric disease,
    seizure disorder (uncomplicated childhood febrile seizures with no
    sequelae are not exclusionary) Parkinson's disease, infection,
    hypertension, vascular disorder, significant pulmonary disease, or
    any other illness.
    History of malignancy within 5 years before screening
    (exceptions are squamous and basal cell carcinomas of the skin and
    carcinoma in situ of the cervix, or malignancy, which is considered
    cured with minimal risk of recurrence).
    Known allergies, hypersensitivity, or intolerance to aticaprant
    or its excipients.
    Presence of LBBB, AV block (second degree or higher), or a
    permanent pacemaker or implantable cardioverter defibrillator.
    Clinically relevant GI complaints per clinical judgment at
    screening or baseline or history of documented gastric disease
    (including but not limited to documented peptic ulcer disease,
    gastritis [including atrophic gastritis], upper GI bleeding, Barret's
    esophagus, Crohn disease, ulcerative colitis, GI precancerous
    conditions or any other clinically relevant GI disease irritable
    bowel syndrome).
    Participant has current or past homicidal ideation/intent within
    the last 6 months, or has current or past suicidal ideation with some
    intent to act within 6 months prior to the start of the screening
    phase, corresponding to a response of “Yes” on Item 4 (active
    suicidal ideation with some intent to act, without specific plan) or
    Item 5 (active suicidal ideation with specific plan and intent) for
    suicidal ideation on the C-SSRS, or a history of suicidal behavior
    within the past year prior to the start of the screening phase.
    Participants reporting suicidal ideation with intent to act or suicidal
    behavior on Day −1 prior to the start of the treatment should be
    excluded.
    Serology positive for HbsAg, HCV antibodies or HIV antibodies
    at screening.
    Prior/Concomitant Therapy
    Contraindications to the use of aticaprant or similar class of drugs
    (not limited to drugs such as mu-antagonists, kappa-antagonists)
    per local prescribing information.
    Participant requires chronic use of a PPIs.
    History of chronic NSAID or aspirin use. (Low dose aspirin e.g.,
    in cardiovascular disease prevention is allowed).
    Taken any disallowed therapies, Concomitant Therapy before the
    planned first dose of study intervention.
    Use of any prescription or nonprescription medication (including
    vitamins, herbal supplements, and mineral supplements), except
    for paracetamol, hormone-based contraceptives and hormonal
    replacement therapy within 14 days before the first dose of the
    study intervention is scheduled until completion of the study.
    Prior/Concurrent Clinical Study Experience
    Received an investigational intervention (including
    investigational vaccines) or used an invasive investigational
    medical device within at least 1 month, before the planned first
    dose of study intervention or is currently enrolled in an
    investigational study.
    Pregnant, or breast-feeding, or planning to become pregnant
    while enrolled in this study or within 1 month after the last dose of
    study intervention.
    Plans to father a child while enrolled in this study or within 3
    months after the last dose of study intervention.
    Diagnostic Assessments
    Had major surgery, (e.g., requiring general anesthesia) within 12
    weeks before screening, or will not have fully recovered from
    surgery, or has surgery planned during the time the participant is
    expected to participate in the study.
    History of substance or alcohol use disorder according to DSM-5
    criteria within 6 months before Screening or positive test result(s)
    for alcohol, nicotine metabolites or drugs of abuse (including
    barbiturates, opioids [including methadone], cocaine,
    cannabinoids, amphetamines, methamphetamines, hallucinogens
    such as PCP and LSD, and benzodiazepines) at Screening or Day −1
    of each treatment period.
  • Other Exclusions
      • Donated blood or blood products or plasma or had substantial loss of blood (more than 500 mL) within 3 months before the first administration of study intervention in each part of the study or intention to donate blood or blood products during the study.
      • Unable to swallow solid, oral dosage forms whole with the aid of water (participants may not chew, divide, dissolve, or crush the study intervention).
      • History of smoking or use of nicotine-containing substances within the previous 3 months prior to screening, as determined by medical history or participant's verbal report.
      • Vulnerable participants (e.g., a person kept in detention).
      • Drinks, on average, more than 8 cups of tea/coffee/cocoa/cola or other caffeinated beverages per day.
      • Clinically significant acute illness within 7 days prior to study intervention administration.
      • History of clinically significant drug and/or food allergies.
  • (iii) Meals and Dietary Restrictions
      • 1. Participants may not consume any food or beverages containing, grapefruit juice, Seville oranges (including any orange marmalade), or quinine (e.g., tonic water) from 48 hours (72 hours in the case of grapefruit juice and Seville oranges) before the first dose of study intervention until the last dose of study intervention.
      • 2. No water will be allowed within 2 hours before study intervention with the exception of 240 mL of noncarbonated water to take the oral study intervention and water given with high-fat breakfast. No water is allowed until 2 hours after dosing, after which time, water is allowed ad libitum.
      • 3. Must not consume any foods or drinks (including additional salt or sugar) other than those provided by the study site personnel during domiciled inpatient periods.
      • 4. Must refrain from the use of any methylxanthine-containing products, (e.g., chocolate bars or beverages, energy drinks if it contains methylxanthine, coffee, teas, or colas) from 48 hours before administration of study intervention and during confinement, and also must avoid excessive use of caffeine (i.e., no more than approximately 500 mg/day, as contained in 5 cups of tea or coffee or 8 cans of cola) for the entire study period (including the screening period and follow-up visit).
      • 5. May not consume food containing poppy seeds during the study starting 72 hours before screening or 72 hours before admission to study site in each treatment period (in order to avoid false positive urine drug test for codeine).
  • Caffeine, Alcohol, Tobacco, and Drugs of Abuse
      • 1. Smoking cigarettes (or equivalent) and/or the use of nicotine-based products is not allowed from 3 months prior to screening until completion of the follow-up visit.
      • 2. The use of alcohol should be limited to the absolute minimum. Best is to use no alcohol at all from the first screening visit until the follow-up visit. If any alcohol is taken, up to 2 standard drinks consumptions daily, will be allowed. A standard drink is defined as: a 350 mL glass of 5% ABV beer, a 150 mL glass of 12% ABV wine, or a 45 mL glass of a 40% ABV (80 proof) spirit.
  • Activity
      • 1. Strenuous exercise may affect study specified assessments and safety laboratory results; for this reason, strenuous exercise should be avoided within 48 hours before all planned study visits and during stays in the CRC. Prior exercise will be allowed if the participant's serum creatinine concentration is within the normal range. Minor abnormalities, which are not considered to be of clinical relevance, are acceptable.
      • 2. Participants will be advised not to donate blood for at least 3 months after completion of the study or to participate in an investigational drug study for at least 1 month after completion of the study.
  • B. Study Intervention
  • All study intervention will be taken in the morning on Day 1 of each treatment period with 240 mL of noncarbonated water. Study intervention must be swallowed whole and not chewed, divided, dissolved, or crushed.
  • For each participant, all doses must be administered at approximately the same time.
  • Participants receiving study intervention in the fasted condition will fast overnight for at least 10 hours.
  • Participants receiving study intervention in the fed condition will fast overnight (at least 10 hours) followed by the consumption of a high-fat breakfast within a 20-minute period. The high-fat breakfast will be the same on the day of dosing in the fed period (Period 4 for Part 1 and Part 2). Study intervention will be administered approximately 30 minutes after the start of the breakfast.
  • Noncarbonated water will be allowed up to 2 hours before study intervention administration. Participants will continue fasting until at least 4 hours after study intervention administration. At approximately 2 hours after dosing (but not earlier), drinking of water is allowed ad-libitum onwards. A standardized lunch will be served on Day 1 for all participants after collection of the 4-hour PK blood sample. Participant can resume their normal diet after 4 hours.
  • The exact composition of breakfast and the lunch will be recorded. The lunch will be the same in all intervention periods. The exact start and end time of breakfast, as well as the start time of lunch will be recorded, together with any deviation regarding the timing of the meals.
  • Aticaprant will be supplied for this study as 5 mg capsule and 5 mg and 10 mg tablet formulation.
  • Concomitant Therapy
  • Prestudy therapies administered up to 30 days before first dose of study intervention must be recorded at screening.
  • All therapies (prescription or over-the-counter medications, including vaccines, vitamins, herbal supplements; non-pharmacologic therapies such as electrical stimulation, acupuncture, special diets, exercise regimens, or other specific categories of interest) different from the study intervention must be recorded. Recorded information will include a description of the type of therapy, duration of use, dosing regimen, route of administration, and indication. Modification of an effective preexisting therapy should not be made for the explicit purpose of entering a participant into the study.
  • All concomitant therapies that are considered to be a CYP inhibitor or inducer or a transport inhibitor or inducer are disallowed during the study and disallowed for at least 1 month before receiving the first intake of study intervention.
  • Throughout the study, prescription or nonprescription medication (including vitamins and herbal supplements) other than the study intervention are prohibited, except for paracetamol. Throughout the study, a maximum of 3 doses per day of 500 mg paracetamol, and no more than 3 g per week, will be allowed for the treatment of headache or other pain.
  • Women using hormonal contraceptives as a means of birth control must continue to use the same hormonal contraceptives throughout the study. Women using hormone replacement therapy must continue to use the same hormone replacement therapy throughout the study.
  • C. Study Assessments
  • Tables 59-60 summarize the frequency and timing of PK measurements applicable to this study.
  • If multiple assessments are scheduled for the same timepoint, they should preferably take place in the following order: 12-lead ECG, vital signs (supine blood pressure, pulse/heart rate), blood/CSF draws for PK or laboratory measurements, and C-SSRS. Blood collections for PK assessments should be kept as close to the specified time as possible. Other measurements may be done earlier than specified timepoints, if needed.
  • For each participant, the maximum amount of blood drawn from each participant will not exceed 500 mL.
  • The total volume of CSF collected per participant enrolled in CSF PK will not exceed 52.3 mL which is considered to be acceptable considering the daily CSF production rate.
  • TABLE 59
    Volume of Blood to be Collected From Each Participant (Part 1)
    No. of Approximate
    Volume per Samples per Total Volume
    Type of Sample Sample (mL) Participant of Blood (mL)a
    Pharmacokinetic samples 4 mL 68 272
    Loss by use of indwelling 1 mL 68 68
    intravenous cannula
    Approximate Totalc 442
    aCalculated as number of samples multiplied by amount of blood per sample.
    b.
    cRepeat or unscheduled samples may be taken.
    Note:
    An indwelling intravenous cannula may be used for blood sample collection. If a mandarin (obturator) is used, blood loss due to discard is not expected.
  • TABLE 60
    Volume of Blood to be Collected From Each Participant (Part 2)
    No. of Approximate
    Volume per Samples per Total Volume
    Type of Sample Sample (mL) Participant of Blood (mL)a
    Pharmacokinetic samples 4 mL 72 288
    Loss by use of indwelling 1 mL 72 72
    intravenous cannula
    Approximate Totalc 462
    aCalculated as number of samples multiplied by amount of blood per sample.
    b.
    cRepeat or unscheduled samples may be taken.
    Note:
    An indwelling intravenous cannula may be used for blood sample collection. If a mandarin (obturator) is used, blood loss due to discard is not expected.
  • (i) Vital Signs
  • Body temperature, pulse/heart rate, respiratory rate, blood pressure will be assessed.
  • Blood pressure and pulse/heart rate measurements will be assessed with a completely automated device consisting of an inflatable cuff and an oscillatory detection system. All values will be registered on a built-in recorder so that measurements are observer-independent. Blood pressure and pulse/heart rate measurements will be recorded after 5 minutes rest in a quiet setting without distractions (e.g., television, cell phones) in a supine position.
  • (ii) Electrocardiograms
  • During the collection of ECGs, participants should be in a quiet setting without distractions (e.g., television, cell phones). Participants should rest in a supine position for at least 5 minutes before ECG collection and should refrain from talking or moving arms or legs. If blood sampling or vital sign measurement is scheduled for the same time point as ECG recording, they should preferably take place in the following order: 12-lead ECG, vital signs (supine blood pressure, pulse/heart rate), blood/CSF draws for PK, or laboratory measurements, and C-SSRS.
  • (iii) Columbia Suicide Severity Rating Scale (C-SSRS)
  • The C-SSRS is a measure of the spectrum of suicidal ideation and behavior that was developed to assess severity and track suicidal events through any treatment studies. It is a clinical interview to assess the risk of treatment-emergent suicidal ideation/behavior.
  • There are 2 versions of the C-SSRS. A baseline/screening version of the C-SSRS will be completed at screening, and subsequently a since-your-last-visit version of the C-SSRS will be completed predose on Day −1, prior to discharge on Day 5 of each treatment period (for Part 1), prior to discharge on Day 6 of each treatment period (for Part 2) and at end-of-study or early withdrawal.
  • (iv) Fundoscopy
  • Fundoscopy is a form of examination of the fundus of the eye. The WelchAllyn® PanOptic™ Ophthalmoscope (model 11810) is used according to the internal standard operating procedure.
  • (v) Pharmacokinetics
  • Plasma and CSF samples will be used to evaluate the PK of aticaprant.
  • Evaluations
  • Blood samples (4 mL each) for determination of aticaprant plasma concentrations will be collected at the time points indicated in Tables 59-60.
  • Analytical Procedures
  • During the study, serial blood samples (4 mL each) for determination of aticaprant plasma concentrations, will be collected at the time points as indicated in Tables 59-60.
  • Plasma samples will be analyzed to determine concentrations of aticaprant using a validated, specific, and sensitive Liquid chromatography coupled to tandem mass spectrometry (LC-MS/MS) method.
  • Parameters
  • The following plasma PK parameters of aticaprant will be determined. A noncompartmental model with extravascular input will be used for the pharmacokinetic analysis.
  • Based on the individual concentration-time data, using the actual sampling times, the following PK parameters will be derived for aticaprant:
  •
    Cmax Maximum observed plasma concentration
    Tmax The actual sampling time to reach Cmax
    AUClast area under the plasma concentration-time curve from 0 to t last
    hours postdosing, calculated by trapezoidal summation (time t
    last is the time of the last quantifiable concentration Clast)
    AUC∞ AUClast extrapolated to infinity, calculated as AUClast + Clast/λz
    Terminal half-life, defined as 0.693/λz
    λz Elimination rate constant, determined by linear regression of the
    terminal points of the log-linear plasma concentration-time curve
    CL/F Apparent clearance (assessed for aticaprant)
    Vd/F Apparent volume of distribution (assessed for aticaprant)
  • The following requirements should be met for an acceptable calculation of t1/2, λz, and AUC:
      • A) at least 3 data points are used in the calculation, otherwise t1/2, λz and AUC are not assessable.
      • B) coefficient of determination (r2 adj) is at least 0.90.
  • If requirement (B) is not met, t1/2, λz, and AUC will be reported as approximations.
  • Actual sampling times will be checked for major aberrations. In case a major aberration occurs for an actual sampling time of >20.00% deviation from the scheduled time, this plasma concentration will be excluded from descriptive statistics in the plasma concentration table.
  • Sample Size Determination
  • The intra-participant coefficient of variation (CV) for PK parameters (AUC and Cmax) is estimated to be between 8.3% and 10.4% for AUC and between 14.4% and 24.3% for Cmax. Thus, an intra-participant CV of 25% was used for this sample size justification.
  • With the selected intra-participant CV of 25% and N=20 or 24 completers, the limits where the point estimate of the ratio of geometric means for PK parameters (AUC and Cmax) in relative bioavailability (test formulation versus reference formulation), food effect (fed versus fasted condition), and dose proportionality with normalized PK parameters will fall are given in Table 61.
  • TABLE 61
    Precision Estimates for Relative Bioavailability, Dose Proportionality, and
    Food Effect of Study Subpart 1A, Subpart 1B, Subpart 2A, Subpart 2B
    Lower Upper
    Limit Limit
    Study Part Purpose N (%) (%)
    Subpart 1A, and/or Relative Bioavailability 20 87.7 114.0
    Subpart 2A and/or Dose
    Proportionality
    24 88.7 112.7
    Subpart 1B, Food Effect 20 87.4 114.4
    Subpart 2B 24 88.5 113.0
    Lower and Upper limit are given as % of true ratio of means with 90% confidence.
  • 24 participants will be enrolled to ensure 20 participants complete the study. If 20 participants do not complete the study, additional participants can be recruited.
  • Populations for Analysis Sets
  • For purposes of analysis, the following populations are defined:
  • Population Description
    Enrolled All participants who sign the consent and not screen
    failures.
    Randomized All participants who were randomized in the study
    Pharmacokinetics All randomized participants who take at least 1 dose
    of study intervention and have at least one estimated
    PK parameter.
  • Statistical Analyses
  • The statistical analysis plan will be finalized prior to DBL and it will include a more technical and detailed description of the statistical analyses described in this section. This section is a summary of the planned statistical analyses of the most important endpoints.
  • Initial Participant Characteristics
  • For all participants who received at least one dose of study intervention, descriptive statistics (mean, standard deviation, median, minimum, and maximum) will be performed for age, BMI, weight, and height. Sex and race will be listed and tabulated.
  • Pharmacokinetic Analyses
  • Data will be listed for all participants with available plasma concentrations per intervention. All concentrations below the limit of quantification (LOQ) or missing data will be labeled as such in the concentration data listings. Concentrations below the LOQ will be treated as zero in the summary statistics and for the calculation of pharmacokinetic parameters. All participants and samples excluded from analysis will be clearly documented in the clinical study report.
  • Factors that may influence the plasma concentrations (e.g., vomiting, high predose concentration) will be checked.
  • Reasons for exclusion of a participant or a sample from the analysis include, but are not limited, to the following:
      • Predose aticaprant plasma concentrations higher than 5% of Cmax
      • Vomiting (within 3 hours post-dose under fasting conditions and 8 hours post-dose under fed conditions) after study intervention administration for immediate-release products. (Considering median Tmax of 1.5 hours under fasting conditions and median Tmax of 4 hours under fed conditions)
      • If the % AUC∞,ex exceeds 20% for a given participant, that participant will be excluded from the statistical analysis of AUC∞
      • Too few data (greater than 10% missing values per each participant)
      • Noncompliance with study procedures affecting pharmacokinetics (e.g., comedication)
  • All participants and samples excluded from the analysis will be clearly documented in the study report.
  • For each intervention, descriptive statistics, including arithmetic mean, standard deviation (SD), coefficient of variation (CV), geometric mean, median, minimum, and maximum will be calculated for the aticaprant plasma concentrations at each sampling time and for all PK parameters of aticaprant.
  • For relative bioavailability, graphical representations of the results will include (but are not limited to) the following graphs for aticaprant:
      • Log-linear and linear-linear plasma concentration-time profiles for each individual
      • Log-linear and linear-linear plasma concentration-time profiles for the mean values per intervention
      • Log-linear and linear-linear plasma concentration-time profiles for the median values per intervention
      • Log-linear and linear-linear overlay plots of the individual plasma concentration-time profiles for each intervention
      • A graphical comparison of the individual and mean (±SD) primary PK parameters of aticaprant for each intervention
  • For dose proportionality, graphical representations of the results will include (but are not limited to) the following graphs for aticaprant:
      • Log-linear and linear-linear plasma concentration-time profiles for each individual, for all dose levels.
      • Overlay graph with the observed mean plasma concentration-time profiles on a log-linear and linear-linear scale for all dose levels. Overlay graph with the mean dose-normalized plasma concentration-time profiles on a log-linear and linear-linear scale.
      • A graph with the observed individual values of Cmax, AUC∝, AUClast and/or AUC truncated to a common time point versus the dose;
      • A graph with the observed dose-normalized individual values of Cmax, AUC∝, AUClast and/or AUC truncated to a common time point versus the dose;
  • The primary objective of the statistical analysis will be to estimate the relative bioavailability of aticaprant test formulations with respect to aticaprant reference formulations, dose proportionality of aticaprant test formulations, and the effect of food on the PK of aticaprant test formulations.
  • The primary parameters of interest for the statistical analysis will be the log-transformed estimated AUCs, AUClast, AUC, and Cmax. The AUC will be rejected as primary parameter for a group if more than half of the participants do not have a reliable value. If one of PK parameter of interest is not estimable for a given participant in one or more periods, the participant's data will not be included in the statistical analysis of that particular PK parameter.
  • For the relative bioavailability and dose proportionality in Subpart 1A (i.e., only the first 3 periods will be included in this analysis), after dose-normalized AUClast, AUC, and Cmax for Treatment C, a mixed-effects model that includes treatment, period, and treatment sequence as fixed effects, and participant as a random effect will be used to estimate the least squares means and intra-participant variance. Using these estimated least squares means and intra-participant variance, the point estimate and 90% confidence intervals for the difference in means on a log scale between Treatment B (Test) and Treatment A (Reference), and between Treatment C (Test) and Treatment B (Reference) will be constructed. The limits of the confidence intervals will be back-transformed using antilogarithms to obtain 90% confidence intervals for the ratios of the mean AUCs and Cmax of the test to reference formulation (Treatment B/Treatment A and Treatment C/Treatment B). For the relative bioavailability and dose proportionality in Subpart 2A, similar analyses will be carried out for Treatment E, Treatment F, and Treatment G.
  • For the food effect in both Subpart 1B (Treatment D versus Treatment B) and Subpart 2B (Treatment H versus Treatment F), mixed-effects models will be fit to the data with the logarithm of PK parameters as the dependent variable, treatment (fed versus fasted) as a fixed effect, and participant as a random effect. Using these estimated least squares means and intra-participant variance from the mixed-effects models, the point estimate and 90% confidence intervals for the difference in means on a log scale between Treatment D (fed) and Treatment B (fasted), and Treatment H (fed) and Treatment F (fasted) will be constructed. The limits of the confidence intervals will be back-transformed using antilogarithms to obtain 90% confidence intervals for the corresponding ratios of the mean AUCs and Cmax under fed to fasted conditions.
  • D. Results
  • This study included two parts with similar study design to investigate two different tablet formulation concepts with part 1 (unmilled API tablet) and part 2 (milled API tablet). Within each part, the evaluations included relative bioavailability of immediate-release tablet formulation (1×10 mg) versus API in capsule formulation (2×5 mg), dose-proportionality between 10 and 5 mg tablet strengths, and food effect assessment at 10 mg of tablet strength. Each part consisted of a subpart A and subpart B with a total of 4 periods. Subpart A was a randomized, open label, 3-way crossover, 3-period study conducted in 24 healthy participants to evaluate the relative bioavailability of a single dose of 10 mg aticaprant administered as 1×10 mg oral tablet under fasted conditions compared to 10 mg aticaprant administered as 2×5 mg oral capsules under fasted conditions and to evaluate the dose proportionality of a single dose of 5 mg aticaprant administered as 1×5 mg oral tablet under fasted conditions compared to the 1×10 mg oral tablet under fasted conditions. The same 24 participants who completed subpart A were enrolled in subpart B which consisted of a fourth period to evaluate the food effect of a single dose of 10 mg aticaprant administered as 1×10 mg oral tablet under fed conditions.
  • The PK analysis results for part 1 (unmilled API tablet formulation) including the PK parameters across treatments and statistical comparisons between treatments of interest are shown in Tables 62-65. Table 62 summarizes PK parameters across treatments in Part 1. Table 63 shows the statistical comparison results of the relative bioavailability of a 1×10 mg unmilled API tablet with 2×5 mg API in capsule formulation. Table 64 shows the statistical comparison results of the dose-proportionality between 1×10 mg unmilled API tablet and 1×5 mg unmilled API tablet formulation. Table 65 shows the statistical comparison results of food effect assessment with 1×10 mg unmilled API tablet when administered in the presence of high-fat diet to that of fasted condition. The results of the PK parameters were comparable between unmilled API tablet (1×10 mg) and API in capsule (2×5 mg) formulation and the statistical assessment using calculated geometric mean ratios indicated that these two formulations are comparable and within the BE limits of criteria. A dose-proportionality was established between 10 and 5 mg unmilled API tablet formulation strengths based on dose-dependent increase in PK parameters, a comparison of dose-normalized PK parameters and statistical assessment of calculated geometric mean ratios being within BE limits of 0.8 to 1.25. Finally, unmilled API tablet formulation showed ˜40% increase in AUC when 10 mg given in the presence of high-fat diet compared to fasted condition administration as evident from geometric mean ratio calculated for AUC.
  • The PK analysis results for part 2 (milled API tablet formulation) including the PK parameters across treatments and statistical comparisons between treatments of interest are shown in Tables 66-73. Table 70 summarizes PK parameters across treatments in Part 2. Table 71 shows the statistical comparison results of the relative bioavailability of a 1×10 mg milled API tablet with 2×5 mg API in capsule formulation. Table 72 shows the statistical comparison results of the dose-proportionality between 1×10 mg milled API tablet and 1×5 mg milled API tablet formulation. Table 73 shows the statistical comparison results of food effect assessment with 1×10 mg milled API tablet when administered in the presence of high-fat diet to that of fasted condition. The results of the PK parameters were comparable between milled API tablet (1×10 mg) and API in capsule (2×5 mg) formulation and the statistical assessment using calculated geometric mean ratios indicated that these two formulations are comparable and within the BE limits of criteria. A dose-proportionality was established between 10 and 5 mg milled API tablet formulation strengths based on dose-dependent increase in PK parameters, a comparison of dose-normalized PK parameters and statistical assessment of calculated geometric mean ratios being within BE limits of 0.8 to 1.25. Finally, milled API tablet formulation showed ˜30% increase in AUC when 10 mg given in the presence of high-fat diet compared to fasted condition administration as evident from geometric mean ratio calculated for AUC.
  • In summary, both the milled and unmilled API tablet formulations of 1×10 mg showed similar comparable exposures for aticaprant as those were observed with 10 mg reference API in capsule formulation (2×5 mg API in capsules) and were bioequivalent. A dose-proportionality was observed between 10 and 5 mg tablet formulation strengths of each of the tablet formulation concepts of unmilled and milled API. A modest food effect of ˜30% (milled API tablet) and ˜40% (unmilled API tablet) increase in AUC was observed at 10 mg with a slightly delayed median Tmax of 2.00 hours (milled API tablet) and 2.75 hours (unmilled API tablet) in presence of high-fat diet vs. 1.5 hours in the fasted condition administration. A 40% food effect is not considered clinically relevant for many drugs given it is part of PK variability and no safety concerns exist at higher aticaprant exposures. Aticaprant can therefore be administered with or without food.
  • (i) PK Parameters
  • TABLE 66
    Summarized PK Parameters of Aticaprant
    Pharmacokinetic
    Parameters of Treatment
    Aticaprant (mean [SD], C Dose
    tmax: median [range]) A B C Normalized D
    n 23 21 21 21 20
    Cmax (ng/mL) 31.2 (6.90) 34.1 (10.0) 17.0 (4.48) 33.9 (8.97)  37.7 (9.18)
    tmax (h) 1.50 (1.00-2.50) 1.50 (1.00-2.00) 1.50 (1.00-3.00) 2.75 (1.00-4.00)
    AUClast (h*ng/mL) 304 (77.7) 283 (76.2) 143 (39.9) 286 (79.7) 398 (87.6)
    AUC (h*ng/mL) 315 (83.7)a 301 (80.1) 155 (43.2) 309 (86.4) 425 (101)b
    Λz (1/h) 0.030 (0.010)a 0.029 (0.010) 0.035 (0.017) 0.031 (0.010)b
    t1/2 (h) 26.3 (10.2)a 26.6 (8.12) 24.7 (11.2) 24.5 (8.05)b
    CL/F (L/h) 34.5 (11.6)a 36.2 (12.5) 35.8 (14.4) 25.0 (6.83)b
    Vd/F (L) 1248 (546)a 1335 (448) 1150 (394) 835 (187)b
    Treatment A: 2 × 5 mg oral capsule administered in the morning, after at least 10-hour overnight fasting
    Treatment B: 1 × 10 mg Formulation Concept 1 administered in the morning, after at least 10-hour overnight fasting
    Treatment C: 1 × 5 mg Formulation Concept 1 administered in the morning, after at least 10-hour overnight fasting
    Treatment D: 1 × 10 mg Formulation Concept 1 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting
    an = 21,
    bn = 19
    5 mg dose normalized to 10 mg
  • (ii) Relative BA Assessment
  • 1×10 mg unmilled API tablet concept may show similar exposures for aticaprant as those were observed with 10 mg reference API in capsule formulation (2×5 mg API in capsules)
  • TABLE 67
    Relative BA Testing (10 mg Tablet vs. 10 mg reference capsule) - Summarized statistical results
    for Estimated Ratio of Means and 90% Confidence Interval : Treatment B/Treatment A-Aticaprant-For
    completers (Relative Bioavailability); Phamacokinetics Data Analysis Set
    Geometric Means
    N Ratio of
    Treatment Geometric Intra-
    PK A A Means 90% participant
    Analyte Parameter (Reference) B (Test) (Reference) B (Test) (%) CI (%) CV (%)
    Aticaprant C max 20 20  30.2  32.8 108.64 99.25- 17.0
    118.92
    AUC last 20 20 291 271  93.31 87.41- 12.2
    99.62
    AUC 19 19 305 287  94.14 88.19- 11.9
    100.49
    Note:
    Log transformed PK parameters were analyzed by mixed model analysis of variance with treatment, sequence, and period as fixed effects, and participant in sequence as a random effect and the results were back-transformed using anti-logarithm.
    Participants who completed all treatment periods and for which an evaluable PK parameter could be obtained in all treatment periods are included in the analysis.
    N: number of participants who completed the study and for which an evaluable PK parameter could be obtained.
    Intra-participant CV(%) = 100* (sqrt(exp(MSE)-1).
    Treatment A: 2 × 5 mg oral capsule administered in the morning, after at least 10-hour overnight fasting (Reference)
    Treatment B: 1 × 10 mg Formulation Concept 1 administered in the morning, after at least 10-hour overnight fasting (Test)
  • (iii) Dose-Proportionality
  • Dose-proportionality may be observed between 1×10 mg unmilled API tablet vs. 1×5 mg unmilled API tablet
  • TABLE 68
    Dose-proportionality testing (10 mg Tablet vs. 5 mg tablet) - Summarized statistical results
    for Estimated Ratio of Means and 90% Confidence Interval: Treatment B/Treatment A-
    ATICPARANT-For completers (Dose proportionality); Pharmacokinetics Data Analysis Set
    Geometric Means
    N Ratio of
    Treatment Geometric 90% Intra-
    PK B B C Means CI participant
    Analyte Parameter (Reference) C (Test) (Reference) (Test) (%) (%) CV (%)
    Aticaprant C max 20 20  32.8  33.5 102.12 93.23- 17.0
    111.86
    AUC last 20 20 271 280 103.20 96.63- 12.2
    110.23
    AUC 19 19 287 299 103.93 97.34- 11.9
    110.98
    Note:
    Log transformed PK parameters were analyzed by mixed model analysis of variance with treatment, sequence, and period as fixed effects, and participant in sequence as a random effect and the results were back-transformed using anti-logarithm. Participants who completed all treatment periods and for which an evaluable PK parameter could be obtained in all treatment periods are included in the analysis.
    N: number of participants who completed the study and for which an evaluable PK parameter could be obtained.
    Intra-participant CV(%) = 100* (sqrt(exp(MSE)-1).
    Treatment B: 1 × 10 mg Formulation Concept 1 administered in the morning, after at least 10-hour overnight fasting (Reference)
    Treatment C: 1 × 5 mg Formulation Concept 1 administered in the morning, after at least 10-hour overnight fasting (Test)
    5 mg dose normalized to 10 mg
  • (iv) Food-Effect
  • Food effect (high-fat diet) was observed for 10 mg unmilled API tablet (˜44% increase in AUC) with delayed Tmax to ˜3 hours in presence of high-fat diet vs. 1.5 hours in the absence of high-fat diet.
  • TABLE 69
    Food Effect testing (10 mg Tablet vs. 10 mg tablet in presence of high-fat diet) -
    Summarized statistical results for Estimated Ratio of Means and 90% Confidence Interval for
    Aticaprant: Treatment D/Treatment B-For completers (Food Effect); Pharmacokinetics Data
    Analysis Set
    Geometric Means
    N Ratio of Intra-
    Treatment Geometric participant
    PK B D B D Means 90% CV
    Analyte Parameter (Reference) (Test) (Reference) (Test) (%) CI (%) (%)
    Aticaprant C max 20 20  32.6  36.6 112.49 100.49- 20.9
    125.93
    AUC last 20 20 270 388 144.01 135.53- 11.1
    153.02
    AUC 19 19 287 413 143.84 135.29- 10.9
    152.94
    Note:
    Log transformed PK parameters were analyzed by mixed model analysis of variance with treatment as fixed effect and participant as a random effect and the results were back-transformed using anti-logarithm.
    Participants who completed all treatment periods and for which an evaluable PK parameter could be obtained in all treatment periods are included in the analysis.
    N: number of participants who completed the study and for which an evaluable PK parameter could be obtained.
    Intra-participant CV(%) = 100* (sqrt(exp(MSE)-1).
    Treatment B: 1 × 10 mg Formulation Concept 1 administered in the morning, after at least 10-hour overnight fasting (Reference)
    Treatment D: 1 × 10 mg Formulation Concept 1 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting (Test)
  • TABLE 70
    Summarized PK Parameters of Aticaprant in Part 2
    Pharmacokinetic
    Parameters of Treatment
    Aticaprant (mean [SD], G Dose
    tmax: median [range]) E F G Normalized H
    n 22 22 23 23 21
    Cmax (ng/mL) 31.7 (9.41) 32.4 (7.39) 17.4 (5.81) 34.7 (11.6) 34.0 (9.99)
    tmax (h) 2.00 (1.00-6.00)   1.50 (1.00-2.50) 1.00 (1.00-4.00) 2.00 (1.00-6.00)
    AUClast (h*ng/mL) 308 (108) 297 (123) 157 (80.1) 314 (160) 388 (135)
    AUC (h*ng/mL) 307 (80.8)a 318 (148) 154 (37.0)a 308 (74.1)a 388 (81.7)b
    λz (1/h) 0.024 (0.006)a 0.024 (0.007) 0.030 (0.013)a 0.025 (0.009)b
    t1/2 (h) 30.5 (6.98)a 31.0 (8.05) 26.6 (9.45)a 30.8 (8.27)b
    % AUC∞, ex (%) 5.02 (2.06)a 5.50 (3.17) 6.93 (2.25)a 4.92 (2.51)c
    CL/F (L/h) 34.8 (9.82)a 35.8 (12.1) 34.7 (10.7)a 27.0 (6.38)b
    an = 21,
    bn = 19,
    cn = 20
    Treatment E: 2 × 5 mg oral capsule administered in the morning, after at least 10-hour overnight fasting
    Treatment F: 1 × 10 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting
    Treatment G: 1 × 5 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting
    Treatment H: 1 × 10 mg Formulation Concept 2 administered in the morning approximately 30 minutes after the start of a standardized high-fat breakfast following at least 10-hour overnight fasting Participant 100029, Treatment F (incomplete profile) and 100031 (vomiting) hence excluded
  • TABLE 71
    Statistical comparison results of the relative bioavailability of a 1 × 10 mg milled API tablet
    (test) with 2 × 5 mg API in capsule formulation (reference).
    Summarized statistical results for Estimated Ratio of Means and 90% Confidence Interval:
    Treatment F/Treatment E - Aticaprant - For completers (Relative Bioavailability); Pharmacokinetics
    Data Analysis Set
    Geometric Means
    N Ratio of
    Treatment Geometric 90% Intra-
    PK E F E F Means CI participant
    Analyte Parameter (Reference) (Test) (Reference) (Test) (%) (%) CV (%)
    Aticaprant C max 21 21  30.2  30.9 102.30 94.30- 15.6
    110.97
    AUC last 21 21 291 274  94.31 89.93-  9.1
    98.90
    AUC 20 20 297 279  93.66 89.58-  8.3
    97.93
    Note:
    Log transformed PK parameters were analyzed by mixed model analysis of variance with treatment, sequence, and period as fixed effects, and participant in sequence as a random effect and the results were back-transformed using anti-logarithm.
    Participants who completed all treatment periods and for which an evaluable PK parameter could be obtained in all treatment periods are included in the analysis.
    N: number of participants who completed the study and for which an evaluable PK parameter could be obtained.
    Intra-participant CV(%) = 100* (sqrt(exp(MSE)-1).
    Treatment E: 2 × 5 mg oral capsule administered in the morning, after at least 10-hour overnight fasting (Reference)
    Treatment F: 1 × 10 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting (Test).
  • TABLE 72
    Statistical comparison results of the dose-proportionality between 1 × 10 mg milled API tablet
    (reference) and 1 × 5 mg milled API tablet formulation (test).
    Summarized statistical results for Estimated Ratio of Means and 90% Confidence Interval: Treatment
    G/Treatment F- ATICAPTANT- For completers (Dose proportionality); Pharmacokinetics Data Analysis
    Set
    Geometric Means
    N Ratio of
    Treatment Geometric 90% Intra-
    PK F G F G Means CI participant
    Analyte Parameter (Reference) (Test) (Reference) (Test) (%) (%) CV (%)
    Aticaprant C max 21 21  30.9  32.5 105.13 96.97- 15.6
    113.98
    AUC last 21 21 274 285 104.15 99.35-  9.1
    109.19
    AUC 20 20 279 296 106.40 101.79  8.3
    111.22
    Note:
    Log transformed PK parameters were analyzed by mixed model analysis of variance with treatment, sequence, and period as fixed effects, and participant in sequence as a random effect and the results were back-transformed using anti-logarithm.
    Participants who completed all treatment periods and for which an evaluable PK parameter could be obtained in all treatment periods are included in the analysis.
    N: number of participants who completed the study and for which an evaluable PK parameter could be obtained.
    Intra-participant CV(%) = 100* (sqrt(exp(MSE)-1).
    Treatment F: 1 × 10 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting (Reference)
    Treatment G: 1 × 5 mg Formulation Concept 2 administered in the morning, after at least 10-hour overnight fasting (Test)
    Note:
    Treatment G, Dose Normalized to 10 mg
    Participants 100029 (incomplete PK profile) and 100031 (vomiting) from treatment F were excluded from the analysis.
  • TABLE 73
    Statistical comparison results of food effect assessment with 1 × 10 mg milled API tablet when
    administered in the presence of high-fat diet (test) to that of fasted condition administration (reference) -
    Summarized statistical results for Estimated Ratio of Means and 90% Confidence Interval for
    Aticaprant: Treatment H/Treatment F- For completers (Food Effect); Pharmacokinetics Data Analysis
    Set
    Geometric Means
    N Ratio of Intra-
    Treatment Geometric participant
    PK F H F H Means 90% CV
    Analyte Parameter (Reference) (Test) (Reference) (Test) (%) CI (%) (%)
    Aticaprant C max 20 20  31.3  33.5 107.30 97.03- 18.6
    118.66
    AUC last 20 20 279 377 134.90 128.72-  8.6
    141.39
    AUC 19 19 280 379 135.55 129.65-  7.9
    141.72
    Note:
    Log transformed PK parameters were analyzed by mixed model analysis of variance with treatment, sequence, and period as fixed effects, and participant in sequence as a random effect and the results were back-transformed using anti-logarithm.
    Participants who completed all treatment periods and for which an evaluable PK parameter could be obtained in all treatment periods are included in the analysis.
    N: number of participants who completed the study and for which an evaluable PK parameter could be obtained.
    Intra-participant CV(%) = 100* (sqrt(exp(MSE)-1).
    Participant 100031 (vomiting) from treatment F excluded from the analysis.

Claims (22)

What is claimed is:
1. A method of treating major depressive disorder in a human patient, comprising administering a pharmaceutical composition comprising aticaprant and one or more pharmaceutically acceptable excipients to the human patient, wherein the patient had a previous inadequate response to other antidepressant therapy and wherein the pharmaceutical composition is administered orally once daily.
2. The method of claim 1, wherein the pharmaceutical composition is administered with or without food.
3. The method of claim 1, wherein the pharmaceutical composition is an oral tablet.
4. The method of claim 1, wherein the pharmaceutical composition comprises about 5 mg to about 10 mg aticaprant.
5. The method of claim 1, wherein the pharmaceutical composition comprises about 10 mg aticaprant.
6. The method of claim 3, wherein the pharmaceutical composition comprises about 5 mg to about 10 mg aticaprant.
7. The method of claim 3, wherein the pharmaceutical composition comprises about 10 mg aticaprant.
8. The method of claim 1, wherein the other antidepressant therapy comprised one or more antidepressants.
9. The method of claim 8, wherein the one or more antidepressants comprised a SSRI, SNRI, or a combination thereof.
10. The method of claim 1, wherein the aticaprant is S-aticaprant.
11. The method of claim 1, wherein the aticaprant is crystalline aticaprant.
12. The method of claim 1, further comprising treatment with an effective amount of one or more antidepressants.
13. The method of claim 12, wherein the one or more antidepressants is a SSRI, SNRT, or combination thereof.
14. The method of claim 1, wherein the patient has anhedonia.
15. The method of claim 1, wherein the pharmaceutical composition comprises one or more of: a filler, a disintegrant, a glidant, a lubricant, a binder, and a coloring agent.
16. The method of claim 15, wherein the filler is selected from: microcrystalline cellulose, lactose monohydrate, and silicified microcrystalline cellulose; the disintegrant is croscarmellose sodium; the glidant is silica, colloidal anhydrous; and the lubricant is magnesium stearate.
17. The method of claim 1, wherein the pharmaceutical composition comprises between about 0.1% and 90% aticaprant by weight.
18. The method of claim 1, wherein the pharmaceutical composition comprises between about 1% to about 10% aticaprant by weight.
19. The method of claim 1, wherein the pharmaceutical composition comprises between about 10% and 99.9% filler by weight.
20. The method of claim 1, wherein the pharmaceutical composition is a film coated oral tablet, comprising (i) a film coat and (ii) a core tablet, wherein the core tablet comprises about 5% aticaprant by weight, about 88.5% filler by weight, about 5% disintegrant by weight, about 1% glidant by weight, and about 0.5% lubricant by weight.
21. The method of claim 20, wherein the film coated oral tablet comprises about 97% core tablet by weight and about 3% film coat by weight.
22. The method of claim 1, wherein the pharmaceutical composition is an oral tablet comprising about 10 mg aticaprant, wherein the oral tablet comprises a core tablet of about 200 mg, wherein the core tablet comprises an intragranular and extragranular phase, wherein the intragranular phase comprises about 60 mg microcrystalline cellulose, about 60 mg lactose monohydrate, about 5 mg croscarmellose sodium, and about 1 mg silica, colloidal anhydrous; and wherein the extragranular phase comprises about 57 mg silicified microcrystalline cellulose, about 5 mg croscarmellose sodium, about 1 mg silica, colloidal anhydrous, and about 1 mg magnesium stearate.
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