[go: up one dir, main page]

AP906A - Dofetilide polymorphs - Google Patents

Dofetilide polymorphs Download PDF

Info

Publication number
AP906A
AP906A APAP/P/1998/001371A AP9801371A AP906A AP 906 A AP906 A AP 906A AP 9801371 A AP9801371 A AP 9801371A AP 906 A AP906 A AP 906A
Authority
AP
ARIPO
Prior art keywords
dofetilide
polymorph
dofetilide polymorph
pharmaceutically acceptable
heart failure
Prior art date
Application number
APAP/P/1998/001371A
Other versions
AP9801371A0 (en
Inventor
Ian Colin Appleby
Trevor Jack Newbury
Gary Nicholas
Original Assignee
Pfizer Res & Development Company N V /S A
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Family has litigation
First worldwide family litigation filed litigation Critical https://patents.darts-ip.com/?family=10821150&utm_source=google_patent&utm_medium=platform_link&utm_campaign=public_patent_search&patent=AP906(A) "Global patent litigation dataset” by Darts-ip is licensed under a Creative Commons Attribution 4.0 International License.
Application filed by Pfizer Res & Development Company N V /S A filed Critical Pfizer Res & Development Company N V /S A
Publication of AP9801371A0 publication Critical patent/AP9801371A0/en
Application granted granted Critical
Publication of AP906A publication Critical patent/AP906A/en

Links

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C311/00Amides of sulfonic acids, i.e. compounds having singly-bound oxygen atoms of sulfo groups replaced by nitrogen atoms, not being part of nitro or nitroso groups
    • C07C311/01Sulfonamides having sulfur atoms of sulfonamide groups bound to acyclic carbon atoms
    • C07C311/02Sulfonamides having sulfur atoms of sulfonamide groups bound to acyclic carbon atoms of an acyclic saturated carbon skeleton
    • C07C311/08Sulfonamides having sulfur atoms of sulfonamide groups bound to acyclic carbon atoms of an acyclic saturated carbon skeleton having the nitrogen atom of at least one of the sulfonamide groups bound to a carbon atom of a six-membered aromatic ring
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/18Antipsychotics, i.e. neuroleptics; Drugs for mania or schizophrenia
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/04Inotropic agents, i.e. stimulants of cardiac contraction; Drugs for heart failure
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/06Antiarrhythmics

Landscapes

  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Health & Medical Sciences (AREA)
  • Engineering & Computer Science (AREA)
  • Bioinformatics & Cheminformatics (AREA)
  • General Health & Medical Sciences (AREA)
  • Chemical Kinetics & Catalysis (AREA)
  • General Chemical & Material Sciences (AREA)
  • Medicinal Chemistry (AREA)
  • Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
  • Pharmacology & Pharmacy (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • Animal Behavior & Ethology (AREA)
  • Cardiology (AREA)
  • Public Health (AREA)
  • Veterinary Medicine (AREA)
  • Heart & Thoracic Surgery (AREA)
  • Psychiatry (AREA)
  • Hospice & Palliative Care (AREA)
  • Biomedical Technology (AREA)
  • Neurology (AREA)
  • Neurosurgery (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Saccharide Compounds (AREA)
  • Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)
  • Steroid Compounds (AREA)
  • Organic Low-Molecular-Weight Compounds And Preparation Thereof (AREA)
  • Heterocyclic Carbon Compounds Containing A Hetero Ring Having Oxygen Or Sulfur (AREA)
  • Pyrrole Compounds (AREA)
  • Preparation Of Compounds By Using Micro-Organisms (AREA)

Abstract

The invention relates to the substantially pure polymorphs P162, P162a and P143 of the compound dofetilide (N-[4-(2-[2-[4-(methanesuiphonamido) phenoxy]-N1 -methylethy!amino]ethyl)phenyi]methanesulphonamide) having the structure • and to processes for the preparation of, compositions containing and to the uses of, such polymorphs.

Description

DOFETILIDE POLYMORPHS
The present invention relates to polymorphs of the compound known as dofetilide. More particularly, the invention relates to the novel dofetilide polymorphs known as P162, P162a and P143, and to processes for the preparation of, compositions containing and to the uses of, such polymorphs.
Dofetilide, N-[4-(2-[2-[4-(methanesulphonamido)phenoxy]-N1methylethylamino]ethyl)phenyl]methanesulphonamide, has the following structure:
Dofetilide is disclosed in EP-A-0245997 as an antiarrhythmic agent that prolongs the duration of the action potential in cardiac muscle and conducting tissue, thereby increasing refractoriness to premature stimuli. It is therefore a Class III antiarrhythmic agent according to the classification of Vaughan
Williams (“Anti-Arrhythmic Action”, E.M. Vaughan Williams, Academic Press, 1980). It is effective in atria, ventricles and conducting tissue both in vitro and •i.
in vivo and could therefore be useful for the prevention and treatment of a wide variety of ventricular and supraventricular arrhythmias including atrial and ventricular fibrillation. Since it does not alter the speed at which impulses are conducted, it has less propensity than other antiarrhythmic drugs (mostly Class I) to precipitate or aggravate arrhythmias and it also produces less neurological side effects. It also lacks negative inotropic activity and therefore offers advantages over other antiarrhythmic agents in patients with impaired cardiac pump function.
The use of dofetilide in treating heart failure, particularly congestive heart failure, is described in European Patent Application no. 98306188.8, the teaching of which is incorporated herein by reference.
AP/P/ 9 8 / 0 1 3 7 1
ΑΡΟ 0 0 9 0 6
-2Α capsule formulation of dofetilide is currently preferred. Dofetilide is a very potent drug and is therefore to be used in very low dosage. Since a very low drug loading will be required for the capsule formulation, it is essential that the active ingredient has a small particle size to ensure that a homogeneous blend is achieved.
The previously known methods of preparing dofetilide that are described in EP-A-0245997 are difficult to reproduce and have either produced a mixture of dofetilide polymorphs P162/P162a, P162b/P136 or P162b/P136/P143 or, essentially, dofetilide polymorph P136 or P162b, all of which tend to crystallise in an agglomerated form that would have to be deagglomerated (e.g. by milling or micronisation) to achieve the required small particle size. Hence, none of these products would be directly suitable for use in a capsule formulation.
It is an object of this invention to provide a suitable, substantially pure, crystalline, polymorphic form of dofetilide that can be easily, economically and reproducibly prepared with the required small particle size for use in a capsule formulation, preferably without any milling of the drug being necessary in the production process.
It has now been surprisingly found that this object has been achieved by the present invention which provides a substantially pure, crystalline, polymorphic form of dofetilide known as P162 and an inventive process for the preparation thereof. Dofetilide polymorph P162 crystallises from aqueous acetonitrile as flakes/plates with a consistently small particle size distribution, 90% of the particles being less than 45pm in size. This form therefore does not require milling before use in a capsule formulation. It is also non-hygroscopic over a broad range of relative humidities, is chemically and physically stable, is rapidly absorbed in vivo and it can be routinely and reproducibly prepared in commercial quantities by the crystallisation process described herein.
Accordingly, the present invention provides substantially pure, crystalline, dofetilide polymorph P162 which is characterised by differential
AP/P/ 9 8 / 0 1 3 7 1
-3scanning calorimetry (DSC) in which it exhibits an endothermic thermal event at about 162°C.
Dofetilide polymorph P162 is further characterised by a powder X-ray diffraction (PXRD) pattern obtained by irradiation with copper K-alpha·, X-rays (wavelength = 1.5406 Angstroms) which shows main peaks with interplanar spacings at dA 21.303, 10.597, 7.053, 5.288, 5.088, 4.856, 4.793, 4.569, 4.504, 4.430, 4.256, 4.230, 4.133, 3.956, 3.911, 3.866, 3.674, 3.606, 3.524, 3.424, 3.384, 3.309, 3.255, 3.171, 3.083, 3.038, 3.021, 2.893, 2.842, 2.776, 2.679,
2.598, 2.557, 2.503, 2.482, 2.436, 2.419, 2.399, 2.345 and 2.323.
Dofetilide polymorph P162 is yet further characterised by an infrared (IR) spectrum as a mull in nujol which shows absorption bands at 3246, 3013, 2807, 2776, 1907, 1611, 1593, 1510, 1398, 1366, 1357, 1321, 1300, 1277, 1251, 1220, 1171, 1146, 1106, 1091, 1051, 1031, 1023, 994, 966, 934, 925, 903,
851, 825, 808, 774, 723, 657, 603, 586, 559, 538, 528, 509, 499, 461 and 431 cm .
Dofetilide polymorph P162 has been made available by the surprising finding that crystallisation of any other form of dofetilide from aqueous acetonitrile produces this polymorph as the product.
The present invention further provides the substantially pure, crystalline, dofetilide polymorphs P162a and P143. It will be appreciated that these polymorphs are not only to be regarded as synthetic intermediates that can be further processed to dofetilide polymorph P162 by crystallisation from aqueous acetonitrile, they also have the same therapeutic properties thereas. However, dofetilide polymorphs P162a and P143, and P162b and P136, are not as suitable as dofetilide polymorph P162 for use in preparing capsule formulations of the drug, principally because milling to achieve the required particle size is often required. Dofetilide polymorphs P162a and P162b have similar PXRD patterns and IR spectra, but different DSC characteristics, to dofetilide polymorph P162. The differences in the melting points of these polymorphs are
AP/P/ 9 8 / 0 1 3 71
AP 0 0 0 9 0 6
-4-
5 due to varying degrees of disorder within the crystal structures of the polymorphs. Substantially pure, crystalline, dofetilide polymorph P162a is characterised by DSC in which it exhibits an endothermic thermal event at
_ 10 about 160°C. Dofetilide polymorph P162a is further characterised by a PXRD pattern obtained by irradiation with copper Κ-alpha-, X-rays (wavelength = 1.5406 Angstroms) which shows main peaks with interplanar spacings at dA 21.306, 10.603, 7.054, 5.289, 5.114, 5.094, 4.860, 4.572, 4.431, 4.260, 4.247, 4.228, 4.153, 4.136, 3.955, 3.870, 3.676, 3.607, 3.524, 3.435, 3.421, 3.384, 3.176, 3.038, 2.895, 2.778, 2.684, 2.559, 2.501,2.486, 2.433, 2.326, 2.283, 2.248, 2.216, 2.171, 2.119, 2.051, 1.989 and 1.948.
15 Dofetilide polymorph P162a is yet further characterised by an IR spectrum as a mull in nujol which shows absorption bands at 3246, 3013, 2807, 2776, 1907, 1611, 1593, 1510, 1397, 1366, 1357, 1321, 1300, 1277, 1251, 1220, 1171, 1146, 1106, 1091, 1051, 1031, 1023, 994, 966, 934, 926, 903,
20 851,825, 807, 774, 726, 657, 602, 586, 559, 538, 528, 509, 499, 461 and 430 cm'1. Substantially pure, crystalline, dofetilide polymorph P143 is characterised by DSC in which it exhibits an endothermic thermal event at about144°C.
25 Dofetilide polymorph P143 is further characterised by a PXRD pattern obtained by irradiation with copper K-alpha1 X-rays (wavelength = 1.5406 Angstroms) which shows main peaks with interplanar spacings at dA 10.993, 9.006, 8.243, 6.769, 5.807, 5.530, 5.375, 5.104, 4.998, 4.735, 4.575, 4.539, 4.237, 4.179, 4.159, 4.019, 3.854, 3.705, 3.682, 3.601, 3.562, 3.482, 3.392, 3.343, 3.331, 3.263, 3.227, 3.173, 3.135, 3.082, 3.009, 2.946, 2.905, 2.859, 2.830, 2.803, 2.769, 2.672, 2.608 and 2.567.
AP/P/ 9 8 / 0 1 3 7 1
AP ο Ο Ο 9 Ο 6
-5Dofetilide polymorph Ρ143 is yet further characterised by an IR spectrum as a mull in nujol which shows absorption bands at 3266, 3123, 3107, 3041, 3027, 3013, 2766, 2723, 2610, 1895, 1614, 1607, 1587, 1511, 1414, 1395,
1337, 1319, 1301, 1287, 1248, 1230, 1215, 1202, 1187, 1157, 1148, 1130, 1110, 1060, 1042, 1018, 1005, 980, 975, 959, 940, 917, 853, 844, 831, 803, 785, 766, 752, 743, 718, 640, 613, 553, 536, 526, 509, 499, 455 and 429 cm'1.
The expression “substantially pure” when used in conjunction with dofetilide polymorphs P162, P162a and P143 means at least 95% by weight pure. More preferably, “substantially pure” means at least 98% by weight pure and most preferably means at least 99% by weight pure.
Dofetilide polymorph P162 can be prepared by crystallisation of any other form of dofetilide, including polymorphic mixtures thereof, from aqueous acetonitrile. Preferably, from 98.5:1.5 to 99.5:0.5, by volume, acetonitrile:water is used as the crystallisation solvent. Most preferably, about 99:1, by volume, acetonitrile:water is used.
Dofetilide polymorph P162a can be prepared by dissolving any other form of dofetilide in an aqueous solution of a suitable base such as sodium hydroxide, adjusting the solution to about pH 8.5 using a suitable mineral acid,
e.g. hydrochloric acid, and collecting the product. In this process, when sodium hydroxide and hydrochloric acid are used, sodium chloride may be coprecipitated as an impurity.
Dofetilide polymorph P143 can be prepared by dissolving any other form of dofetilide in methanol, applying the solution obtained to a silica column, eluting the column with methanol and concentrating the eluted solution to dryness under reduced pressure to provide a crystalline product
Synthetic routes to prepare dofetilide are described in EP-A-0245997 and in the present Reference Examples section.
AP/P/ 9 8 / 0 1 3 7 1
APO *· 0 9 Ο 6
-6For assessment of the antiarrhythmic pharmacological effects of the dofetilide polymorphs, dog isolated cardiac tissue is used. Right ventricular trabeculae, papillary muscle or Purkinje fibres are isolated from either ventricle, mounted in an organ bath containing physiological salt solution and stimulated electrically. The resultant action potentials are recorded using intracellular microelectrodes. The effect of increasing the concentration of the polymorph within the bathing solution on the action potential duration and on the effective refractory period (ERP) are assessed. ERP is measured by stimulating the tissue with extra stimuli at progressively shorter inter-stimulus intervals until the extra stimulus fails to elicit an action potential. Essentially, the methods used are as described by Gwilt M., Arrowsmith J.E., Blackburn K.J. et al., “UK-68798. A novel, potent and highly selective class ill antiarrhythmic agent which blocks potassium channels in cardiac cells”, J. Pharmacol. Exp. Ther., 256. 318-24 (1991).
Methods for assessing the activity of the dofetilide polymorphs in treating heart failure are described in European Patent Application no. 98306188.8.
The dofetilide polymorphs can be administered alone but will generally be administered in admixture with a pharmaceutically acceptable diluent or carrier selected with regard to the intended route of administration and standard W pharmaceutical practice. For example, they may be administered orally in the form of tablets containing such excipients as starch or lactose, or in capsules either alone or in admixture with excipients, or in the form of elixirs or suspensions containing flavouring or colouring agents. They may be injected parenterally, for example, intravenously, intramuscularly or subcutaneously.
For parenteral administration, they are best used in the form of a sterile aqueous solution which may contain other solutes, for example, enough salts or glucose to make the solution isotonic with blood.
AP/P/ 9 8 / 0 1 3 7 1
APO00906
-7The dofetilide polymorphs are preferably administered as capsule formulations. Such formulations may be prepared by mixing the dofetilide polymorph together with suitable carriers or excipients such as microcrystalline cellulose, dried maize starch, colloidal silicon dioxide and magnesium stearate.
For administration to man in the treatment of cardiac conditions such as ventricular and supraventricular arrhythmias, including atrial and ventricular fibrillation, it is expected that oral dosages of the compounds of the formula (I) will be in the range of from 0.125 to 1 mg, preferably from 0.25 to 1 mg, daily, taken in up to two divided doses per day, for an average adult patient (70 kg). Thus, for a typical adult patient, individual tablets or capsules might, for example, contain from 0.125 to 0.5 mg of active compound together with a suitable pharmaceutically acceptable diluent, excipient or carrier. Variations may occur depending on the weight and condition of the subject to be treated as will be known to medical practitioners.
Appropriate dosages of the dofetilide polymorphs for treating heart failure are described in European Patent Application no. 98306188.8.
AP/P/ 9 8 / 0 1 3 7 1
APO « Ο 9 ο 6
-8lt will be appreciated that reference to medical treatment means curative, palliative or prophylactic treatment.
The invention therefore provides;
(i) substantially pure, crystalline, dofetilide polymorph P162, P162a or
P143;
(ii) a process for the preparation of substantially pure, crystalline, dofetilide polymorph P162, P162a or P143;
(iii) a pharmaceutical composition comprising substantially pure, crystalline, dofetilide polymorph P162, P162a or P143, together with a pharmaceutically acceptable diluent or carrier;
(iv) a pharmaceutical capsule composition comprising substantially pure, crystalline, dofetilide polymorph P162, P162a or P143, together with a pharmaceutically acceptable diluent or carrier;
(v) substantially pure, crystalline, dofetilide polymorph P162, P162a or P143 for use as a medicament;
(vi) the use of substantially pure, crystalline, dofetilide polymorph P162, P162a or P143 for the manufacture of an antiarrhythmic agent;
(vii) a method of treating cardiac arrhythmia which comprises administering an effective amount of substantially pure, crystalline, dofetilide polymorph P162, P162a or P143, or a pharmaceutically acceptable composition thereof, to an animal, including a human being, in need of such treatment;
(viii) the use of substantially pure, crystalline, dofetilide polymorph P162,
P162a or P143 for the manufacture of a medicament for treating heart failure, particularly congestive heart failure; and (ix) a method of treating heart failure, particularly congestive heart failure, which comprises administering an effective amount of substantially pure, crystalline, dofetilide polymorph P162, P162a or P143, or a pharmaceutically acceptable composition thereof, to an animal, including a human being, in need of such treatment.
AP/P/ 9 8 / 0 1 3 7 1
APO00906
-9EXAMPLES 1-8
The following Examples illustrate the preparation of the novel dofetilide polymorphs P162, P162a and P143, and the known dofetilide polymorph P162b. PXRD, IR, DSC and particle size analytical data for representative samples of these polymorphs are given in Tables 1 to 5.
EXAMPLE 1
Dofetilide polymorph P162
To a stirred solution of acetonitrile (18 litres) and water (180 ml) was added dofetilide1 (3.62 kg) and the mixture heated to achieve complete dissolution of the solid material.
The hot solution was filtered through a pad of CLARCEL-FLO (trade mark) filter aid (prepared as described in Footnote 1 below) and the pad was washed with acetonitrile. The filtrate was stirred and cooled to ambient temperature. The suspension was granulated for 18 hours at ambient temperature, the solid collected by filtration, washed with acetonitrile (2 x 400 ml) and the product dried under reduced pressure at 7.0oC to provide the title compound (3.043 kg).
Footnote
1. The starting material may be pre-treated with charcoal to remove impurities before use using the following method.
To a stirred solution of acetonitrile (10,145 ml) and water (101 ml) was added dofetilide (2028.9 g) and the mixture heated to achieve complete dissolution of the solid material. Decolourising carbon (BDH [trade mark], 202.9 g) was added and the mixture heated under reflux for 15 minutes.
A pre-coated filter pad was prepared by suspending CLARCEL-FLO (trade mark) filter aid (200 g) in acetonitrile (1000 ml) and filtering the mixture with suction onto a paper membrane. The filtrate was discarded and the pad
AP/P/ 9 8 / 0 1 3 7 1
ΑΡ ο ο ο 9 ο 6
-10washed with acetonitrile (1000 ml) until the filtrate ran clear. The pad was sucked until firm but damp and the washings discarded.
The hot dofetilide solution was filtered through the pad with suction and the filtrate cooled to ambient temperature with stirring. The suspension was granulated for 18 hours at ambient temperature. The solid was collected by filtration, washed with acetonitrile (2 x 200 ml) and the product dried under reduced pressure at 70°C to provide 1525.6 g of material.
EXAMPLE 2
Dofetilide polymorph P162a
Dofetilide (100 g) was dissolved with stirring in a solution of sodium hydroxide (25 g) in water (1000 ml). The solution was treated with decolourising carbon (5 g) for 30 minutes at ambient temperature and the carbon filtered off. The filtrate was adjusted to pH 8.5 with concentrated hydrochloric acid and the mixture granulated for 90 minutes. The solid was collected by filtration and washed with water (2 x 100 ml). The solid was dissolved in a solution of sodium hydroxide (25 g) in water (1000 ml) and the treatment with decolourising carbon repeated as before. The filtrate was adjusted to pH 8.5 as Ri/ before and the mixture granulated for 90 minutes. The solid was filtered off, washed with water and dried under reduced pressure at 70°C to give the title compound (93.3 g).
AP/P/ 9 8 / 0 1 3 7 1
APO00906
-11- EXAMPLE 3 (for reference) Dofetilide Dolvmorph P162b
5 Dofetilide (37.0 g) was dissolved with stirring in acetone (750 ml) at ambient
10 temperature and the solution clarified by filtration through a pad of CLARCEL- FLO (trade mark) filter aid. The filtrate was evaporated under reduced pressure ensuring that the temperature did not exceed 20°C. The resulting syrup crystallised and acetone (100 ml) was added. The solid was collected by filtration and dried under reduced pressure at 70°C overnight to give the title compound (29.1 g).
15 EXAMPLE 4 (for reference) Dofetilide polvmorph P162b Dofetilide is heated to about 5°C above the melting point and then cooled to ambient temperature to provide a non-crystalline glass-like solid. This glass is then heated to from 70 to 125°C to provide the title compound as a crystalline solid. ' - ’
20 Θ EXAMPLE 5 Dofetilide polvmorph P143
25 Dofetilide (60 g) was dissolved with stirring in methanol (6000 ml) and the resulting solution applied to a column of silica (WOELM Type TSC [trade mark]) (1000 g). The column was eluted with methanol and the initial 12 litres of the eluted solution was concentrated to dryness under reduced pressure to provide the title compound as a powder that was dried under reduced pressure at 60°C (54.9 g).
AP/P/ 9 8 / 0 1 3 7 1
ΑΡ Ο Ο Ο 9 ο 6
-12EXAMPLE 6
Dofetilide polymorph Ρ162
Dofetilide polymorph P162a was crystallised from aqueous acetonitrile by a similar method to that used in Example 1 to provide dofetilide polymorph P162.
EXAMPLE 7
Dofetilide polymorph P162
Dofetilide polymorph P162b was crystallised from aqueous acetonitrile by a similar method to that used in Example 1 to provide dofetilide polymorph P162.
EXAMPLE 8
Dofetilide polymorph P162
Dofetilide polymorph P143 was crystallised from aqueous acetonitrile by a similar method to that used in Example 1 to provide dofetilide polymorph P162.
AP/P/ 9 8 / 0 1 3 7 1
?
ΑΡΟ 0 0 90 6
-13REFERENCE EXAMPLES 1. 1A, 2, 2A, 3. 3A and 4
In the following Reference Examples 1, 1A, 2, 2A, 3 and 3A, the crystallisation 5 conditions of Examples 7, 19, 20, 21 and 22 of EP-A-0245997 were repeated.
The skilled person will appreciate that the synthetic routes used to prepare dofetiiide in each of the Examples described in EP-A-0245997 will have no effect on the polymorph/polymorph mixture produced. It is solely the crystallisation conditions used that will determine this. The melting points were x-., 10 determined using an Electrothermal IA9100 apparatus in conjunction with a benzanilide reference standard.
PXRD, IR, DSC and particle size data for the products of these Reference Examples are given in Tables 1 to 5.
None of Reference Examples 1, 1A, 2, 2A, 3 and 3A provides substantially pure dofetiiide polymorph P162, P162a or P143.
Reference Example 4 describes the preparation of dofetiiide used as the /» starting material in Examples 1 to 5 and Reference Examples 1, 1A, 2, 2A, 3 L·’ and 3A.
REFERENCE EXAMPLE 1 (re. Examples 21 and 22 of EP-A-0245997)
Dofetiiide polymorph P136/P162b mixture 25
Dofetiiide (5.0 g) was suspended in ethyl acetate (100 ml) and the stirred mixture heated to the reflux temperature. After 15 minutes under reflux, further ethyl acetate (100 ml) was added and after an additional 15 minutes, more ethyl acetate (100 ml) was added. The hot solution was filtered and cooled but
AP/P/ 98/0137 1
APO 0 0 9 0 6
-14no crystallisation occurred. The solution was heated under reflux, reduced to a volume of ca. 100 ml by evaporation of the solvent, cooled and allowed to stand at room temperature overnight. The crystalline product was collected by filtration, washed with cold ethyl acetate and dried (1.7 g). m.p. 160-1 °C*.
* Benzanilide standard (Literature m.p. 163°C) m.p. 164-5°C.
REFERENCE EXAMPLE 1A (re. Examples 21 and 22 of EP-A-0245997)
Dofetilide polymorph P162/P162a mixture
KJ)
The lack of reproducibility of Examples 21 and 22 of EP-A-0245997 is demonstrated by the fact that on repeating the crystallisation conditions of Reference Example 1 using dofetilide (20.0 g), a mixture of dofetilide polymorphs P162/P162a was obtained.
REFERENCE EXAMPLE 2 (re. Examples 19 and 20 of EP-A-0245997)
Dofetilide polymorph P136/P162b mixture
Dofetilide (5.0 g) was added to ethyl acetate (300 ml) and the mixture stirred 20 and heated under reflux to achieve complete dissolution. The hot solution was
O filtered and the filtrate treated with n-hexane (100 ml). A white precipitate resulted and the suspension was granulated at room temperature overnight.
The solid was collected by filtration, washed with n-hexane and dried (3.7 g). m.p. 158-60°C.* * Benzanilide standard (Literature m.p. 163°C) m.p. 164-5°C.
AP/P/ 9 8 / 0 1 3 7 1
AP 0 0 0 9 0 6
-15REFERENCE EXAMPLE 2A (re. Examples 19 and 20 of EP-A-0245997)
Dofetilide Polymorph P136/P162b/P143 mixture
The lack of reproducibility of Examples 19 and 20 of EP-A-0245997 is demonstrated by the fact that on repeating the crystallisation conditions of Reference Example 2 using dofetilide (20.0 g), a mixture of dofetilide polymorphs P136/P162b/P143 was obtained.
REFERENCE EXAMPLE 3 (re. Example 7 of EP-A-0245997)
Dofetilide polymorph P136
Dofetilide (10.0 g) was added to ethyl acetate (200 ml) and the mixture stirred and heated under reflux. The resulting suspension was treated with methanol, dropwise, until complete dissolution occurred. The hot solution was filtered and cooled but crystallisation did not occur. The solution was heated under reflux to evaporate the solvent until crystallisation commenced. The mixture was cooled, granulated for 4 hours, filtered and dried (2.6 g). m.p. 147-8°C*.
>· * Benzanilide standard (Literature m.p. 163°C) m.p. 164-5°C.
REFERENCE EXAMPLE 3A (re. Example 7 of EP-A-0245997)
Dofetilide polymorph P162b
The lack of reproducibility of Example 7 of EP-A-0245997 is demonstrated by the fact that on repeating the crystallisation conditions of Reference Example 3 using dofetilide (20.0 g), dofetilide polymorph P162b was obtained.
AP/P/ 9 8 / 0 1 3 7 1
APO 0 0 9 0 6
-16REFERENCE EXAMPLE 4
N-[4-(2-[2-[4-(Methanesulphonamido)phenoxy]-N1methylethylamino]ethyl)phenyl]methanesulphonamide (dofetilide) '·>«»*
(ii)
AP/P/ 9 8 / 0 1 3 7 1
APO00906
-17(i) N-Methyl-N-[2-(4-nitrophenoxy)ethyl]-4-nitrophenethylamine
To stirred de-ionised water (60 ml) was added N-methyl-2-(4nitrophenyl)ethylamine hydrochloride1 (20.0 g), 4-(2chloroethoxy)nitrobenzene2 (18.61 g), anhydrous potassium carbonate (14.04 g), potassium iodide (3.06 g) and tetra-n-butylammonium iodide (1.70 g). The mixture was heated under reflux for 3 hours, cooled to ca.
40°C, ethyl acetate (100 ml) added and stirred for 10 minutes. The organic phase was separated and the aqueous phase washed with ethyl acetate (2 x 100 ml). The combined organic phases were washed with water3 (50 ml), concentrated under reduced pressure to a volume containing 2 ml per gram of the title compound (based on the theoretical yield) and then two volumes of ethanol added. The mixture was stirred and granulated at ambient temperature overnight, the solid collected by filtration, washed with ethanol (2 x 100 ml) and dried under reduced pressure at 40°C to give the title compound (21.34 g, 67%).
J.
μ
Footnotes
1. J. Med. Chem., 33, 873-7 (1990).
2. J. Org. Chem., 49, 3114-21 (1984).
3. Brine may be used.
AP/P/ 9 8 / 0 1 3 7 1
APOΟ Ο 906
(ii) N-Methvl-N-[2-(4-aminophenoxv)ethvll-4-aminoDhenethvlamine
5 To methanol (2000 ml) was added the compound of part (i) (200 g) and 5% w/w palladium-on-carbon (containing 50% water) (20 g). The mixture was stirred and hydrogenated at 60 p.s.i. (414 kPa) until hydrogen uptake ceased. The catalyst was filtered off, washed with methanol (2 x
Θ 10 100 ml) and the combined filtrate and washings evaporated to low volume under reduced pressure. The residual solvents were replaced with toluene by azeotropic distillation and on completion of this process the volume of the solution was adjusted to ca. 400 ml with toluene (ca. 800 ml of toluene was used in total). The solution was cooled to ambient
15 temperature and granulated for ca. 90 minutes. The solid was collected by filtration, washed with toluene (100 ml) and dried under reduced pressure at 40°C to yield the title compound (152.3 g, 93%). I
20 (iii) N-[4-(2-[2-[4-(Methanesulphonamido)phenoxv]-N1- methvlethvlamino]ethvl)phenvl]methanesulphonamide (dofetilide) To stirred acetonitrile (235 ml) was added the compound of part (ii) (57.0 g), followed by triethylamine (50.5 g). To this mixture was slowly added a solution of methanesulphonyl chloride (57.2 g) in acetonitrile (50 ml) over 30 minutes1. The mixture was stirred for 90 minutes and quenched
25 with water (200 ml). Sodium carbonate (26.7 g) was added
ΛΡ'Ρ' 9 8 / 0 1 3 7 1
ΑΡΟ 0 0 90 6
-19and the mixture stirred for 20 minutes. The reaction mixture was reduced to half-volume by distillation2, water (200 ml) added and distilled to half-volume again. The mixture was cooled, sodium hydroxide pellets (16.0 g) added and the mixture stirred for 3 hours at ambient temperature3. Concentrated hydrochloric acid (35 ml) was added, dropwise, over 30 minutes and the mixture granulated for 90 minutes. The solid was collected by filtration, washed with water (2 x 70 ml) and dried under reduced pressure at 60°C to provide the title compound4 (87.4g, 99%).
Footnotes
1. The temperature of the reaction mixture was not allowed to rise above
50°C during the addition.
2. This may also be achieved by evaporation under reduced pressure.
3. It should be ensured that the mixture has a pH>13 after this period. If not, further base should be added to achieve this pH.
4. HPLC indicated this material to be >99% pure. It can be further purified by carbon treatment (see Example 1, Footnote 1).
AP/P/ 9 8 / 0 1 3 7 1
APO00906
-20ANALYTICAL DATA
a) PXRD
The powder X-ray diffraction patterns were determined using a Siemens D5000 powder X-ray diffractometer fitted with an automatic sample changer, a theta-theta goniometer, automatic beam divergence slits, a secondary monochromator and a scintillation counter.
The samples were prepared for analysis by packing the powder into 12 mm diameter, 0.25 mm deep cavities that had been cut into silicon wafer specimen mounts. Each specimen was rotated whilst being irradiated with copper K-alpha! X-rays (wavelength = 1.5406 Angstroms) with the
X-ray tube operated at 40 kV/40 mA. The analyses were performed with the goniometer running in step-scan mode set for a 5 second count per 0.02° step over a two-theta range of 2° to 55°.
’ Figure 1 shows the PXRD pattern of dofetilide polymorph P162.
Figure 2 shows the PXRD pattern of dofetilide polymorph P162a.
ζί;) Figure 3 shows the PXRD pattern of dofetilide polymorph P162b.
Figure 4 shows the PXRD pattern of dofetilide polymorph P143.
Figure 5 shows the PXRD pattern of the product of Reference Example
1.
Figure 5A shows the PXRD pattern of the product of Reference Example
1A.
Figure 6 shows the PXRD pattern of the product of Reference Example
2.
Figure 6A shows the PXRD pattern of the product of Reference Example
2A.
AP/P/ 9 8 / 0 1 3 7 1
APO 0 0 9 0 6
-21Figure 7 shows the PXRD pattern of the product of Reference Example
3.
Figure 7A shows the PXRD pattern of the product of Reference Example
3A.
Figure 7B shows the PXRD pattern of the product of Example 6.
Figure 7C shows the PXRD pattern of the product of Example 7.
Figure 7D shows the PXRD pattern of the product of Example 8.
The peak listings for the above Figures are given in Table 1 in which dA is a measurement of the interplanar spacing and I/I, is a measurement of the relative intensity.
AP/P/ 9 8 / 0 1 3 7 1
APOΟ Ο 906
-22TABLE 1
P162 P162a(l) P162b P143
dA l/lj l/h dA I/Ij dA l/li
21.303 74 21.306 40 21.508 24 10.993 5
10.597 5 10.603 2 10.640 2 9.006 3
7.053 4 7.054 2 7.073 3 8.243 12
5.288 4 5.289 2 5.292 3 6.769 5
5.088 18 5.114 16 5.098 20 5.807 7
4.856 36 5.094 19 4.868 37 5.530 18
4.793 3 4.860 34 4.580 17 5.375 100
4.569 15 4.572 16 4.436 100 5.104 5
4.504 3 4.431 100 4.270 16 4.998 54
4.430 100 4.260 15 4.250 17 4.735 11
4.256 17 4.247 14 4.234 20 4.575 62
4.230 36 4.228 16 4.140 17 4.539 33
4.133 18 4.153 11 3.961 23 4.237 20
3.956 28 4.136 16 3.921 9 4.179 25
3.911 8 3.955 20 3.679 11 4.159 41
3.866 5 3.870 4 3.528 19 4.019 45
3.674 15 3.676 9 3.426 6 3.854 24
3.606 3 3.607 4 3.388 6 3.705 4
3.524 24 3.524 17 3.172 4 3.682 7
3.424 7 3.435 5 3.090 4 3.601 18
3.384 8 3.421 6 3.040 8 3.562 5
3.309 3 3.384 6 2.895 7 3.482 9
3.255 2 3.176 3 2.842 5 3.392 40
3.171 3 3.038 6 2.782 4 3.343 18
3.083 4 2.895 7 2.684 3 3.331 22
3.038 9 2.778 3 2.559 6 3.263 6
3.021 6 2.684 3 2.504 5 3.227 5
2.893 8 2.559 5 2.492 6 3.173 10
2.842 ' 5 2.501 6 2.482 7 3.135 7
2.776 2 2.486 6 2.431 10 3.082 10
2.679 3 2.433 10 2.326 5 3.009 12
2.598 4 2.326 5 2.283 5 2.946 8
2.557 4 2.283 4 2.250 5 2.905 8
2.503 5 2.248 5 2.216 8 2.859 13
2.482 6 2.216 8 2.164 4 2.830 9
2.436 12 2.171 4 2.119 5 2.803 6
2.419 7 2.119 5 2.047 5 2.769 6
2.399 4 2.051 5 1.798 5 2.672 11
2.345 3 1.989 7 1.748 3 2.608 17
2.323 5 1.948 3 - - 2.567 9
AP/P/ 9 8 / 0 1 3 7 1
AP 0 Ο Ο 9 ο 6
-23TABLE 1 (Continued)
Reference Example 1<2) Reference Example 2(3) Reference Example 3(4)
dA l/lj dA l/lj dA l/lj
21.243 26 21.252 25 11.793 3
11.808 3 12.384 1 11.028 1
10.606 2 11.815 2 9.911 6
9.937 6 10.567 2 9.183 2
9.207 2 9.925 4 8.513 1
8.540 2 9.135 2 8.262 1
8.317 2 7.721 4 7.715 5
7.755 8 7.042 2 6.638 4
7.049 2 6.633 2 6.280 9
6.658 4 6.300 7 6.237 10
6.309 10 6.229 7 5.874 1
6.243 10 5.603 7 5.610 11
5.624 10 5.418 8 5.411 12
5.428 9 5.147 21 5.159 25
5.170 22 5.078 20 4.968 100
5.081 18 4.966 55 4.653 6
4.977 84 4.850 31 4.586 20
4.857 26 4.569 24 4.516 12
4.662 8 4.546 19 4.426 46
4.583 26 4.426 100 4.263 24
4.518 13 4.255 29 4.144 19
4.432 100 4.137 26 4.082 43
4.263 44 4.088 28 4.025 23
4.145 28 4.027 18 3.924 12
4.093 39 3.969 14 3.857 13
4.031 24 3.936 19 3.835 10
3.966 15 3.859 13 3.783 22
3.943 21 3.840 12 3.760 16
3.858 19 3.779 17 3.655 3
3.782 22 3.670 8 3.614 6
3.670 10 3.617 9 3.495 3
3.628 7 3.520 16 3.420 18
3.612 7 3.422 16 3.363 12
3.522 14 3.368 12 3.317 3
3.425 20 3.311 6 3.216 13
3.370 15 3.217 9 3.155 12
3.222 11 3.158 10 3.113 7
3.164 13 3.116 7 3.063 5
3.123 10 3.048 8 3.022 3
3.109 10 2.901 9 2.950 5
AP/F/ 9 8/01371
Footnotes
1. Peaks due to any sodium chloride impurity have been omitted.
2. Dofetilide polymorph P136ZP 162b mixture.
3. Dofetilide polymorph P136/P 162b mixture.
4. Dofetilide polymorph P136.
AP U Ο Ο 9 Ο 6
-24TABLE 1 (Continued)
Reference Example 1A<5) Reference Example 2A(6) Reference Example 3A(?1
dA l/lj dA l/lj dA I/Ii
21.415 20 21.514 15 21.346 29
10.615 2 9.939 3 10.617 2
7.054 3 8.302 3 7.064 4
5.286 3 7.755 3 5.295 4
5.087 18 7.039 3 5.093 17
4.859 34 6.819 3 4.857 34
4.775 4 6.299 6 4.573 18
4.571 17 5.865 4 4.431 100
4.430 100 5.607 5 4.237 28
4.237 20 5.409 23 4.137 17
4.135 16 5.163 13 3.956 23
3.958 22 5.080 22 3.867 5
3.907 7 5.025 28 3.676 11
3.861 4 4.975 40 3.602 4
3.675 10 4.852 34 3.524 20
3.607 4 4.749 9 3.423 8
3.524 19 4.577 26 3.384 7
3.420 6 4.548 28 3.173 5
3.386 6 4.429 100 3.088 6
3.309 3 4.259 31 3.038 9
3.175 3 4.214 25 2.892 8
3.076 5 4.156 24 2.850 6
3.039 8 4.141 27 2.778 3
2.895 8 4.097 26 2.682 4
2.848 5 4.031 22 2.599 4
2.836 5 3.866 17 2.555 5
2.777 4 3.782 14 2.503 6
2.682 4 3.687 11 2.483 7
2.599 4 3.521 20 2.433 9
2.556 5 3.417 16 2.322 6
2.500 5 3.340 11 2.245 6
2.481 6 3.229 8 2.216 11
2.431 9 3.161 9 2.163 5
2.398 5 3.018 10 2.118 6
2.324 5 2.910 10 2.052 5'
2.277 4 2.899 10 - -
2.245 6 2.844 11 - -
2.215 9 2.744 8 - -
2.161 4 2.714 7 - -
2.116 6 2.681 10 - -
AP//-/ 9 8/01371
Footnotes
5. Dofetilide polymorph P162/P162a mixture
6. Dofetilide polymorph P136/P162b/P143 mixture
7. Dofetilide polymorph P 162b
AP U Ο Ο 9 Ο 6
-25TABLE 1 (Continued)
Ρ162 EXAMPLE 6 Ρ162 EXAMPLE 7 P162 EXAMPLE 8
dA l/li dA l/lj dA l/li
21.318 76 21.547 14 21.422 51
10.580 6 10.630 2 10.622 5
7.042 6 7.067 3 7.054 7
5.282 7 5.300 5 5.291 8
5.095 16 5.104 15 5.091 16
4.861 33 4.871 29 4.856 37
4.790 4 4.798 3 4.782 3
4.574 15 4.438 100 4.568 15
4.501 5 4.279 15 4.505 5
4.429 100 4.237 34 4.429 100
4.224 52 4.143 20 4.230 66
4.137 19 3.964 28 4.132 19
3.956 28 3.921 9 3.956 29
3.907 8 3.876 5 3.907 9
3.870 6 3.678 15 3.866 6
3.672 16 3.611 4 3.673 16
3.607 4 3.530 26 3.606 4
3.524 28 3.431 8 3.523 34
3.425 10 3.391 8 3.422 8
3.386 9 3.315 3 3.382 8
3.307 3 3.264 3 3.307 3
3.252 3 3.178 5 3.256 3
3.172 5 3.087 4 3.172 5
3.083 5 3.043 11 3.083 4
3.038 12 2.896 10 3.041 12
3.019 8 2.849 6 3.023 9
2.894 11 2.778 3 2.893 9
2.847 6 2.684 4 2.847 5
2.777 3 2.601 5 2.828 5
2.679 4 2.559 6 2.775 3
2.602 5 2.508 6 2.682 4
2.559 5 2.486 7 2.556 4
2.504 6 2.439 13 2.503 5
2.482 7 2.419 8 2.482 6
2.438 13 2.400 5 2.437 Ϊ2
2.416 9 2.346 5 2.398 5
2.398 5 2.328 6 2.347 5
2.346 5 2.284 5 2.323 5
2.325 7 2.247 7 2.280 4
2.287 4 2.218 13 2.244 7
ΑΡ/Ρ/ 98/01371
ΑΡ ϋ Ο Ο 9 Ο 6
-26b) DSC
Differential scanning calorimetry (DSC) was performed using a Perkin
Elmer DSC-7 machine fitted with an automatic sample changer.
Approximately 2 mg of each sample was accurately weighed into a 50 microlitre aluminium pan and crimp-sealed with a perforated lid.
The samples were heated at 20°C/minute over the range 40°C to 200°C with a nitrogen gas purge.
Figure 8 shows the DSC thermogram for dofetilide polymorph P162. Figure 9 shows the DSC thermogram for dofetilide polymorph P162a. Figure 10 shows the DSC thermogram for dofetilide polymorph P162b.
Figure 11 shows the DSC thermogram for dofetilide polymorph P143.
Figure 12 shows the DSC thermogram for Reference Example 1.
Figure 12A shows the DSC thermogram for Reference Example 1A. Figure 13 shows the DSC thermogram for Reference Example 2.
Figure 13A shows the DSC thermogram for Reference Example 2A.
Figure 14 shows the DSC thermogram for Reference Example 3.
Figure 14A shows the DSC thermogram for Reference Example 3A. Figure 14B shows the DSC thermogram for Example 6.
Figure 14C shows the DSC thermogram for Example Ί.
Figure 14D shows the DSC thermogram for Example 8.
AP/P/ 9 8 / 0 1 3 7 1
The thermal events for the above Figures are summarised in Table 2.
APO 0 0 9 0 6
PCS9440KSR
THERMAL EVENTS Peak=156.8°C (endotherm) Enthalpy= 67.1 J/g Peak=153.3°C (endotherm) Enthalpy= 86.3 J/g
Peak =141.2°C (endotherm) Peak=139.8°C (endotherm)
o o -'T co E ¥ k Peak =137.4°C (exotherm) Peak =140.7°C (endotherm)
Peak=162.5°C (endotherm) Enthalpy=114.6 J/g Peak =159.8°C (endotherm) Enthalpy= 104.9 J/g Peak=158.2°C (endotherm) Enthalpy=108.3 J/g Peak =144.3°C (endotherm) Enthalpy=138.2 J/g Peak=136.3°C (endotherm) Enthalpy=56.3 J/g Peak=134.4°C (endotherm) . Enthalpy= 17.7 J/g Peak =137.0°C (endotherm) Enthalpy=129.4 J/g
SAMPLE P162 P162a JQ CM CO £L P143 Reference Example 1 Reference Example 2 Reference Example 3
AP/P/ 9 8 / 0 1 3 7 1
APO00906
-28TABLE 2 (Continued)
THERMAL EVENTS Peak = 153.4°C (endotherm) Enthalpy = 50.7 J/g
Peak = 143.5°C (endotherm) °C Enthalpy = 12.6 J/g
Peak = 160.4°C (endotherm) Enthalpy = 106.8 J/g Peak = 136.3°C (endotherm) Enthalpy = 13.2 J/g Peak = 159.8°C (endotherm) Enthalpy = 106.1 J/g Peak=162.0°C (endotherm) °C Enthalpy = 115.2 J/g Peak= 164.1 °C (endotherm) Enthalpy = 111.8 J/g Peak= 162.8°C (endotherm) Enthalpy = 115.2 J/g
SAMPLE Reference Example 1A Reference Example 2A Reference Example 3A Example 6 Example 7 00 <U Q. E ro X LU
AP/P/ 98 / 0 1 3 7 1 ω
o
AP000906
-29c) IR
Infrared (IR) spectroscopy was performed on a Nicolet 800 FT-IR spectrometer fitted with an MCT-B detector. All spectra were acquired at
2cm'1 resolution. The samples were prepared as nujol mulls and mounted between two KBr plates prior to acquisition of the spectra.
Figure 15 shows the IR spectrum for dofetilide polymorph P162.
Figure 16 shows the IR spectrum for dofetilide polymorph P162a.
. 10 Figure 17 shows the IR spectrum for dofetilide polymorph P162b.
Figure 18 shows the IR spectrum for dofetilide polymorph P143.
Figure 19 shows the IR spectrum for Reference Example 1.
Figure 20 shows the IR spectrum for Reference Example 2.
Figure 21 shows the IR spectrum for Reference Example 3.
The peak listings for Figures 15 to 21 are shown in Table 3 in which the wavenumber (cm'1) of each peak is recorded.
The peak listings for Figures 15 to 18 are also shown in Table 4 in which both the wavenumber (cm'1) and percentage transmission (%T) of each peak are
AP/P/ 9 8 / 0 1 3 71 recorded.
AP Ο Ο Ο 9 Ο 6
-30Table 3
Ρ162 P162a P162b P143 Referenc e Example 1(1) Referenc e Example 2(z> Referenc e Example 3(3)
3285.9 3284.8 3286.3
3266 4
3245.6 3245.6 3245.7 3123.5 3246.2 3246.0 3123.0
3106.7 3105.9
3041.3 3026.7 3042.8
3012.8 3012.9 3012.6 3012.8 3011.5 3011.8 3010.1
2950 - 2850 nujol bands -Also see band s marked *
2807.1 2807.1 2807.0 2806.8 2807.0 2808.4
2776.2 2776.3 2776.2 2766.5 2776.4 2776.6 2774.9
2722.6 2721.0 2721.9
ca. 2610 ca. 2670 ca. 2670 ca. 2670
broad broad broad broad
1907.1 1907.1 1906.7 1894.6 1894.8 1894.8 1894.8
1614.0 1613.6 1614.6
1610.7 1610.6 1610.5 1606.6 1606.0 1606.4 1605.9
1592.9 1592.9 1592.8 1592.7 1592.8
1587.1 1587.2 1587.6 1586.6
1510,0 1509.9 1509.7 1511.2 1510.4 1510.4 1510.6
1463.6* 1463.7* 1463.5* 1464.4* 1462.6* 1462.7* 1462.3*
1414.3 1415.6 1415.3 1416.0
1397.6 1397.3 1397.1 1395.4 1395.4 1395.9 1394.3
1377.7* 1377.7* 1377.7* 1376.9* 1377.8* 1377.7* 1377.1*
1366.1 1366.1 1366.2 1369.3
1356.9 1356.8 1356.8 1356.5 1356.8
1337.3 1338.5 1338.1 1338.8
1321.4 1321.3 1321.2 1319.0 1316 3 1316.6 1315.9
1301.5 1301.8 1301.0 1302.9
1300.3 1300.2 1300.0 1287.4 1287.1 1288.0 1286.1
1276.8 1276.8 1276.6
1251.5 1251.2 1251.1 1248.0
ΑΡ/Ρ/ 9 8 / 0 1 3 7 1
ΑΡ ΰ Ο Ο 9 Ο 6
-31Table 3 (Continued)
Ρ162 P162a P162b P143 Reference Example 1(1) Reference Example 2(2) Reference Example 3(3)
1246.0 1246.3 1245.8
1230.5 1227.6
1219.9 1219.8 1219.6 1214.9 1220.0 1219.9 1215.1
1201.6 1197.7 1197.5
1186.8 1186.1 1186.0 1186.3 1177.4
1170.9 1171.0 1171.0 1157.0 1170.7 1170.9 1153.6
1148.3
1146.1 1146.0 1145.9 1129.9 1146.2 1146.3 1146.3 1130.1
1110.0 1109.7 1110.5
1106.4 1106.4 1106.2 1107.6
1091.3 1090.6 1089.6
ΙΙβΙβ 1059.7 1059.7
1051.4 1051.4 1051.3 1050.6 1051.0
1042.0 1042.9 1042.9 1042.9
1030.8 1031.4 1031.3 1032.6
1022.7 1022.8 1022.7 1023.7 1023.1 1024.1
1018.2 1019.5 1019.7 1019.3
1004.9 1004.9 1004.8 1005.1
993.9 993.8 993.5 979.6 993.9 993.9
975.0 973.4 973.5 973.5
966.0 965.7 965.6 958.9 966.1
949.0 949.2 948.8
940.2 939.1 939.1 939.5
934.1 934.0 933.9
925.5 925.6 917.1 917.7 924.6 917.8 917.4
903.5 903.4 903.2 904.1 903.9 904.8
853.3 854.3
851.3 851.2 1111852:6; 844.4 852.1
AP/P/ 9 8 / 0 1 3 7 1
-32Table 3 (Continued)
P162 P162a P162b P143 Reference Example (1) Reference Example 2P) Reference Example 3(3)
831.5 831.8 831.5 832.0
824.8 l|824i&ll 824.8 826.6 825.3 820.1
807.8 807.4 807.4 803.1 804.0 804.5 803.6
784.8 786.4
774.4 774.0 773.7 765.9 773.9 774.0 762.2
752.3 742.7
725.7(br) 725.5(br)
722.6(br 718.0 718.8 7228 718.6
657.3 657.3 656.0 656.5 656.8
639.7 639.3 639.3 639.3
613.2 611.3 611.2 611.3
602.6 602.4 602.3 590.1
585.9 585.8 585.7 586.4 586.2
559.0 559.1 559.0 552.7 549.6 549.5 549:8
538.4 538.3 538.2 535.8 537.9 537.9
528.3 528.3 528.2 526.2 526.6 526.7 526.5 520.8
509.2 509.0 508.9 508.9 508.0 508.1 507.9
499.2 499.2 499.0 499.2 498.5 498.6 498.0
461.0 460.8 461.0 454.7 459.7 460.0 459.6
430.7 430.4 430.1 428.6 430.5 431.1 432,8
Footnotes
AP/P/ 9 8 / 0 1 3 7 1
1. Dofetilide polymorph P136/P162b mixture.
2. Dofetilide polymorph P136/P162b mixture.
3. Dofetilide polymorph P136.
ΑΡΟ00906
-33Table 4
P162 P162a P162b P143
cm'1 %T —π cm %T cm' %T cm' %T
3266.4 20.29
3245.6 ....................... 26.38 ...................... ......,·...·.· 3245.6 .................... 24.48 3245.7 ........................... ..... 28.87 .......... ......................... . ... 61.04
3106.7 60.37
3041.3 47.85
3026.7 43.83
3012.8 51.44 3012.9 45.31 3012.6 47.55 3012.8 39.10
2950-2850 nujo bands. Also see bands *
2807.1 63.58 2807.1 59.32 2807 0 60.75
2776.2 64.40 2776.3 60.01 2776.2 61.17 2766.5 63.25
2722.6 58.68
ca. 2610 57.13
broad
1907.1 93.41 1907.1 94 68 1906.7 91.43 1894.6 82.75
1614.0 65.51
1610.7 84.73 1610.6 84.54 1610.5 84.22 1606.6 54.99
1592.9 86.23 1592.9 86.04 1592.8 85.52 1587.1 78.98
1510.0 31.50 1509.9 28.47 1509.7 33.45 1511.2 8.60
1463.6 23.69 |46i|i|i’ 16.35 1463.5 22.79 1464.4* 13.24
1414.3 66.53
1397.6 48.61 1397.3 42.16 1397 1 46.46 1395.4 35.58
1377.7 * 45.67 1377.7 39.58 1377.7 44.30 1376.9* 38.60
1366.1 66.03 1366.1 62.58 1366.2 64.98
1356.9 71.07 1356.8 67.92 1356.8 69.75 1337.3 12.86
1321.4 18.68 1321.3 .. 17.69 ... ... .,. ............. .... 1321.2 22.36 1319.0 10.65
1301.5 23.60
1300.3 39.81 1300.2 34.27 1300.0 38.52 1287.4 33.75
1276.8 57.92 1276 8 52.77 1276.6 55.61
1251.5 54.32 1251.2 48.86 1251.1 52.56 1248.0 35.37
AP/P/ 9 8 / 0 1 3 7 1
AP000906
-34Table 4 (Continued)
P162 P162a P162b P143
cm'1 %T -Π-- cm %T cm'1 %T cm %T
1230.5 27.28
1219.9 43.84 1219.8 37.96 1219.6 42.27 1214.9 44.47
1201.6 61.98
1186.8 65.50
1170.9 66.62 1171.0 62.74 1171.0 65.32 1157.0 7.06
1148.3 8.69
1146.1 10.87 1146.0 11.76 1145.9 15.56 1129.9 33.72
1110.0 42.71
1106.4 63.35 1106.4 57.85 1106.2 59.14
1091.3 81.66 1090.6 80.59 1089.6 78.73. 1059.7 72.50
1051.4 62.12 1051.4 57.89 1051.3 59.76 1042.0 25.15
1030.8 68.18 1031.4 65.66 1031.3 66.06
1022.7 73.40 1022.8 72.44 1022.7 71.73 1018.2 65.16
1004.9 39.30
993.9 43.34 993.8 38.47 993.5 42.33 979.6 14.24
975.0 16.68
966.0 54.49 965.7 49.36 965.6 51.61 958.9 56.46
940.2 55.22
934.1 79.38 934.0 79.14 933.9 77.31
925.5 72.03 925.6 70.33 925.4 70.06 917.1 30.82
903.5 60.15 903.4 55.00 903.2 56.70
851.3 70.46 851.2 68.87 851 2 68,50 852.6 53.44
844.4 57.06
AP/P/ 9 8 / 0 1 3 7 1 χ?Γ·
ΑΡ 0 0 0 9 0 6
-35Table 4 (Continued)
P162 P162a P162b P143
cm' %T cm'1 %T cm'1 %T cm1 %T
831.5 50.93
824.8 64 37 824.9 61.56 824.8 62.02
807.8 78.81 1807ΐιι 78.76 807.4 76.12 803.1 56.74
784.8 68.95
774.4 36.35 774.0 31.38 773.7 35.34 765.9 57.94
752.3 51.78
742.7 57.54
71725ί7ΐί 79.71 725.5 75.5
«βιι
722.6 77.86
(br) 718.0 78.20
657.3 67.41 657.3 65.23 656.0 64.07 639.7 61 93
613.2 58.32
602.6 81.33 602.4 . . .. ... ......... . ... ... . 84.03 602.3 78.67
585.9 80.63 585.8 83.12 585.7 77.98
559.0 78 39 559.1 80.71 559.0 76.17
$> 552.7 62.39
538.4 43.29 538.3 39.69 538.2 41.72 535.8 39.14
528.3 64.08 528.3 62.37 ................................. 528.2 60.02 526.2 18.67
509.2 69.57 509.0 70.43 508.9 66.94 508.9 53.06
499.2 55.62 499.2 52.44 499.0 52.02 499.2 38.97
461.0 85.33 460.8 90.56 461.0 82.53 454.7 81.65
430.7 83.14 430.4 86.76 430.1 80.77 428.6 83.40
AP/P/ 9 8 / 0 1 3 7 1
APO oo 90 6
-36d) Particle size
Particle size analyses were performed by laser light diffraction using a Malvern Mastersizer S machine. Approximately 0.5 g of each sample was added to 100 ml of propan-2-ol, the resulting saturated solution filtered, further sample added and dispersed by ultrasonication followed by stirring. From triplicate determinations, the mean values for the particle size given by the D(v, 0.9) were calculated.
The particle size analyses obtained for dofetilide polymorph P162 and for each of the products of Reference Examples 1 A, 2A and 3A are presented in Table 5.
Table 5
SAMPLE RESULT
Dofetilide polymorph P162 90% of particles less than 45 pm
Reference Example 1A1 90% of particles less than 53 pm
Reference Example 2AZ 90% of particles less than 368 pm
Reference Example 3A 90% of particles less than 14 pm
AP/P/ 9 8 / 0 1 3 7 1
Footnotes
1,2 . Unlike for dofetilide polymorph P162, each of the products of Reference Examples 1A, 2A and 3A contained a mixture of fine material and large lumps that were up to 6-8 mm across. After sonication of each of the products of Reference Examples 1A, 2A and 3A in the saturated solution, many large lumps remained in the products of Reference Examples 1A and 2A and these were not included in the particle size analyses that were performed. As a result the particle size data obtained for the products of Reference Examples 1A and 2A are not accurate since only the finer fractions were analysed.
APO 0 0 9 0 6
-37The results presented in Table 5 show that in addition to dofetilide polymorph P162, only the product of Reference Example 3A had 90% of its particles with a size of less than 45 pm. However, the product of Reference Example 3A had
90% of its particles less than 14 pm which is regarded as too small to be suitable for use in a capsule formulation.
It should be noted that in order to remove the large lumps of material from the products of Reference Examples 1A, 2A and 3A, a milling step would be required in the manufacturing process that is unnecessary for dofetilide polymorph P162.
AP/P/ 9 8/01371
A&ft ft ft η Λ iIavint- no'v Particularly described and v U V 9 Q ^vcriained· niy/our said invention and in iUii. manner the same is to be periormed
I/we declare that what l/we claim is —

Claims (30)

1. Substantially pure, crystalline, dofetilide polymorph P162 which is characterised by differential scanning calorimetry (DSC) in which it exhibits an
5 endothermic thermal event at about 162°C.
2. Dofetilide polymorph P162 as claimed in claim 1 which is further characterised by a powder X-ray diffraction (PXRD) pattern obtained by irradiation with copper K-alpha! X-rays (wavelength = 1.5406 Angstroms) which shows main peaks with interplanar spacings at dA 21.303, 10.597, 7.053,
10 5.288, 5.088, 4.856, 4.793, 4.569, 4.504, 4.430, 4.256, 4.230, 4.133, 3.956, 3.911, 3.866, 3.674, 3.606, 3.524, 3.424, 3.384, 3.309, 3.255, 3.171, 3.083, 3.038, 3.021,2.893, 2.842, 2.776, 2.679, 2.598, 2.557, 2.503, 2.482, 2.436, 2.419, 2.399, 2.345 and 2.323.
3. Dofetilide polymorph P162 as claimed in claim 1 or 2 which is further
15 characterised by an infrared (IR) spectrum as a mull in nujol which shows absorption bands at 3246, 3013,2807, 2776, 1907, 1611, 1593, 1510, 1398, 1366, 1357, 1321, 1300, 1277, 1251, 1220, 1171, 1146, 1106, 1091, 1051, 1031, 1023, 994, 966, 934, 925, 903, 851, 825, 808, 774, 723, 657, 603, 586, 559,<538, 528, 509, 499, 461 and 431 cm’1.
20
4. A process for the preparation of dofetilide polymorph P162 as claimed in claim 1, 2 or 3 which comprises crystallisation of any other form of dofetilide, including mixtures thereof, from aqueous acetonitrile.
5. A process as claimed in claim 4 wherein from 98.5:1.5 to 99.5:0.5, by volume, acetonitrile:water is used.
25
6. A process as claimed in claim 5 wherein about 99:1, by volume, acetonitrile:water is used.
7. A pharmaceutical composition comprising dofetilide polymorph P162 as claimed in claim 1, 2 or 3, together with a pharmaceutically acceptable diluent or carrier.
AP/P/ 9
8 / 0 1 3 7 1
ΑΡ ο ο Ο 9 Ο 6
-398. A composition as claimed in claim 7 which is a suitable for administration in a capsule dosage form.
9. Dofetilide polymorph P162 as claimed in claim 1, 2 or 3, or a
5 pharmaceutically acceptable composition thereof as claimed in claim 7 or 8, for use as a medicament.
10. The use of dofetilide polymorph P162 as claimed in claim 1, 2 or 3, or of a pharmaceutically acceptable composition thereof as claimed in claim 7 or 8, for the manufacture of an antiarrhythmic agent.
10
11. The use of dofetilide polymorph P162 as claimed in claim 1, 2 or 3, or of a pharmaceutically acceptable composition thereof as claimed in claim 7 or 8, for the manufacture of a medicament for treating heart failure, particularly congestive heart failure.
12. A method of treating cardiac arrhythmia which comprises administering
15 an effective amount of dofetilide polymorph P162 as claimed in claim 1, 2 or 3, or a pharmaceutically acceptable composition thereof as claimed in claim 7 or 8, to an animal, including a human being, in need of such treatment.
13. A method of treating heart failure, particularly congestive heart failure, which comprises administering an effective amount of dofetilide polymorph
20 P162 as claimed in claim 1, 2 or 3, or a pharmaceutically acceptable composition thereof as claimed in claim 7 or 8, to an animal, including a human being, in need of such treatment.
14. Substantially pure, crystalline, dofetilide polymorph P162a which is characterised by DSC in which it exhibits an endothermic thermal event at
25 about 160°C.
15. Dofetilide polymorph P162a as claimed in claim 14 which is further characterised by a PXRD pattern obtained by irradiation with copper K-alpha., X-rays (wavelength = 1.5406 Angstroms) which shows main peaks with interplanar spacings at dA 21.306, 10.603, 7.054, 5.289, 5.114, 5.094,4.860,
30 4.572, 4.431,4.260, 4.247, 4.228, 4.153, 4.136, 3.955, 3.870, 3.676, 3.607,
ΑΡ/ΡΛ9 8 /0 1 3 71
APO 0 0 9 0 6
-403.524, 3.435, 3.421, 3.384, 3.176, 3.038, 2.895, 2.778, 2.684, 2.559, 2.501, 2.486, 2.433, 2.326, 2.283, 2.248, 2.216, 2.171, 2.119, 2.051, 1.989 and 1.948.
16. Dofetilide polymorph P162a is as claimed in claim 14 or 15 which is
5 further characterised by an IR spectrum as a mull in nujol which shows absorption bands at 3246, 3013, 2807, 2776, 1907, 1611, 1593, 1510, 1397, 1366, 1357, 1321, 1300, 1277, 1251, 1220, 1171, 1146, 1106, 1091, 1051, 1031, 1023, 994, 966, 934, 926, 903, 851, 825, 807, 774, 726, 657, 602, 586, 559, 538, 528, 509, 499, 461 and 430 cm'1.
10
17. A process for the preparation of dofetilide polymorph P162a as claimed in claim 14, 15 or 16 which comprises dissolving any other form of dofetilide, including mixtures thereof, in an aqueous solution of a base, adjusting the solution to about pH 8.5 using an acid and collecting the product.
18. A process as claimed in claim 17 wherein the base is sodium hydroxide.
15
19. A process as claimed in claim 17 or 18 wherein the acid is a mineral acid such as hydrochloric acid.
20. Substantially pure, crystalline, dofetilide polymorph P143 which is characterised by DSC in which it exhibits an endothermic thermal event at about 144°C.
20
21. Dofetilide polymorph P143 as claimed in claim 20 which is further characterised by a PXRD pattern obtained by irradiation with copper K-alpha·, X-rays (wavelength = 1.5406 Angstroms) which shows main peaks with interplanar spacings at dA 10.993, 9.006, 8.243, 6.769, 5.807, 5.530, 5.375,
5.104, 4.998, 4.735, 4.575, 4.539, 4.237, 4.179, 4.159, 4.019, 3.854, 3.705,
25 3.682, 3.601, 3.562, 3.482, 3.392, 3.343, 3.331, 3.263, 3.227, 3.173, 3.135,
3.082, 3.009, 2.946, 2.905, 2.859, 2.830, 2.803, 2.769, 2.672, 2.608 and 2.567.
22. Dofetilide polymorph P143 as claimed in claim 20 or 21 which is yet further characterised by an IR spectrum as a mull in nujol which shows absorption bands at 3266, 3123, 3107, 3041, 3027, 3013, 2766, 2723, 2610,
AP/P/ 9 8 / 0 1 3 7 1
APOΟ Ο 906
-411895, 1614, 1607, 1587, 1511, 1414, 1395, 1337, 1319, 1301, 1287, 1248, 1230, 1215, 1202, 1187, 1157, 1148, 1130, 1110, 1060, 1042, 1018, 1005,
980, 975, 959, 940, 917, 853, 844, 831, 803, 785, 766, 752, 743, 718, 640,
5 613, 553, 536, 526, 509, 499, 455 and 429 cm'1.
23. A process for the preparation of dofetilide polymorph P143 as claimed in claim 20, 21 or 22 which comprises dissolving any other form of dofetilide, including mixtures thereof, in methanol, applying the solution obtained to a silica column, eluting the column with methanol and concentrating the eluted
10 solution to dryness to provide the product.
24. A pharmaceutical composition comprising dofetilide polymorph P162a or P143, as claimed in any one of claims 14 to 16 and 20 to 22, respectively, together with a pharmaceutical acceptable diluent or carrier.
25. Dofetilide polymorph P162a or P143, as claimed in any one of claims 14
15 to 16 and 20 to 22, respectively, or a pharmaceutically acceptable composition thereof as claimed in claim 24, for use as a medicament.
26. The use of dofetilide polymorph P162a or P143, as claimed in any one of claims 14 to 16 and 20 to 22, respectively, or of a pharmaceutically acceptable composition thereof as claimed in claim 24, for the manufacture of an
20 antiarrhythmic agent
27. The use of dofetilide polymorph P162a or P143, as claimed in any one of claims 14 to 16 and 20 to 22, respectively, or of a pharmaceutically acceptable composition thereof as claimed in claim 24, for the manufacture of a medicament for treating heart failure, particularly congestive heart failure.
25 28. A method of treating cardiac arrhythmia which comprises administering an effective amount of dofetilide polymorph P162a or P143, as claimed in any one of claims 14 to 16 and 20 to 22, respectively, or a pharmaceutically acceptable composition thereof as claimed in claim 24, to an animal, including a human being, in need of such treatment.
AP/P/ 9 8 / 0 1 3 7 1
AP Ο Ο ϋ 9 Ο 6
-4229. A method of treating heart failure, particularly congestive heart failure, which comprises administering an effective amount of dofetilide polymorph P162a or P143, as claimed in any one of claims 14 to 16 and 20 to 22,
5 respectively, or a pharmaceutically acceptable composition thereof as claimed in claim 24, to an animal, including a human being, in need of such treatment.
30. A polymorph as claimed in claim 1, 2, 3, 14, 15, 16, 20, 21 or 22 wherein substantially pure means at least 95% by weight pure.
31. A polymorph as claimed in claim 30 wherein substantially pure means at 10 least 98% by weight pure.
32. A polymorph as claimed in claim 31 wherein substantially pure means at least 99% by weight pure.
APAP/P/1998/001371A 1997-10-27 1998-10-22 Dofetilide polymorphs AP906A (en)

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
GBGB9722662.5A GB9722662D0 (en) 1997-10-27 1997-10-27 Polymorphs

Publications (2)

Publication Number Publication Date
AP9801371A0 AP9801371A0 (en) 1998-12-31
AP906A true AP906A (en) 2000-11-30

Family

ID=10821150

Family Applications (1)

Application Number Title Priority Date Filing Date
APAP/P/1998/001371A AP906A (en) 1997-10-27 1998-10-22 Dofetilide polymorphs

Country Status (46)

Country Link
US (1) US6124363A (en)
EP (1) EP1027329B1 (en)
JP (1) JP3569495B2 (en)
KR (1) KR100366167B1 (en)
CN (1) CN1146537C (en)
AP (1) AP906A (en)
AR (1) AR015193A1 (en)
AT (1) ATE232199T1 (en)
AU (1) AU737668B2 (en)
BG (1) BG64125B1 (en)
BR (1) BR9813308A (en)
CA (1) CA2307121C (en)
CO (1) CO4970768A1 (en)
DE (1) DE69811256T2 (en)
DK (1) DK1027329T3 (en)
DZ (1) DZ2632A1 (en)
EA (1) EA002656B1 (en)
ES (1) ES2190620T3 (en)
GB (1) GB9722662D0 (en)
GT (1) GT199800165A (en)
HN (1) HN1998000165A (en)
HR (1) HRP20000247B1 (en)
HU (1) HUP0004735A3 (en)
ID (1) ID24658A (en)
IL (1) IL135435A0 (en)
IS (1) IS2179B (en)
MA (1) MA24683A1 (en)
MY (1) MY123352A (en)
NO (1) NO325630B1 (en)
NZ (1) NZ503785A (en)
OA (1) OA11350A (en)
PA (1) PA8462001A1 (en)
PE (1) PE122199A1 (en)
PL (1) PL197379B1 (en)
PT (1) PT1027329E (en)
SA (1) SA98190834B1 (en)
SI (1) SI1027329T1 (en)
SK (1) SK5862000A3 (en)
TN (1) TNSN98193A1 (en)
TR (1) TR200001135T2 (en)
TW (1) TW449589B (en)
UA (1) UA67755C2 (en)
UY (2) UY25222A1 (en)
WO (1) WO1999021829A1 (en)
YU (1) YU24000A (en)
ZA (1) ZA989719B (en)

Families Citing this family (8)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
DE10019067C1 (en) * 2000-04-18 2001-10-04 Lohmann Therapie Syst Lts Transdermal plaster comprising dofetilide, is useful for treatment of cardiovascular disorders
US7326772B2 (en) * 2005-05-12 2008-02-05 Penta Biotech, Inc. Peptide for assaying hERG channel binding
CZ2017772A3 (en) 2017-12-01 2019-05-29 Farmak, A.S. Method of preparing N- [4- (2 - {[2- (4-methanesulfonamidophenoxy) ethyl] (methyl) amino} ethyl) phenyl] methanesulfonamide (Dofetilide)
US11344518B2 (en) 2018-08-14 2022-05-31 AltaThera Pharmaceuticals LLC Method of converting atrial fibrillation to normal sinus rhythm and loading oral sotalol in a shortened time frame
US11696902B2 (en) 2018-08-14 2023-07-11 AltaThera Pharmaceuticals, LLC Method of initiating and escalating sotalol hydrochloride dosing
US10512620B1 (en) 2018-08-14 2019-12-24 AltaThera Pharmaceuticals, LLC Method of initiating and escalating sotalol hydrochloride dosing
US12396970B2 (en) 2021-08-20 2025-08-26 AltaThera Pharmaceuticals LLC Anti-arrhythmic compositions and methods
US11610660B1 (en) 2021-08-20 2023-03-21 AltaThera Pharmaceuticals LLC Antiarrhythmic drug dosing methods, medical devices, and systems

Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0245997A2 (en) * 1986-05-01 1987-11-19 Pfizer Limited N-substituted p-aminoethylsulphon anilides as antiarrhythmic agents, and intermediates therefor

Family Cites Families (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0898964A1 (en) * 1997-08-19 1999-03-03 Pfizer Inc. Method for treating heart failure

Patent Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0245997A2 (en) * 1986-05-01 1987-11-19 Pfizer Limited N-substituted p-aminoethylsulphon anilides as antiarrhythmic agents, and intermediates therefor

Also Published As

Publication number Publication date
DE69811256T2 (en) 2003-09-18
NZ503785A (en) 2004-11-26
HRP20000247B1 (en) 2002-08-31
EP1027329B1 (en) 2003-02-05
CO4970768A1 (en) 2000-11-07
KR100366167B1 (en) 2003-01-09
AR015193A1 (en) 2001-04-18
WO1999021829A1 (en) 1999-05-06
AP9801371A0 (en) 1998-12-31
BG104373A (en) 2000-12-29
ZA989719B (en) 2000-04-26
KR20010031439A (en) 2001-04-16
PL197379B1 (en) 2008-03-31
NO20002191D0 (en) 2000-04-27
NO20002191L (en) 2000-04-27
HK1033933A1 (en) 2001-10-05
US6124363A (en) 2000-09-26
AU2151299A (en) 1999-05-17
PE122199A1 (en) 1999-12-02
OA11350A (en) 2003-12-17
PT1027329E (en) 2003-04-30
PA8462001A1 (en) 2000-05-24
SK5862000A3 (en) 2001-10-08
IS5426A (en) 2000-03-31
HN1998000165A (en) 1999-02-09
DE69811256D1 (en) 2003-03-13
YU24000A (en) 2003-02-28
SA98190834B1 (en) 2006-08-21
NO325630B1 (en) 2008-06-30
TNSN98193A1 (en) 2005-03-15
CA2307121A1 (en) 1999-05-06
CA2307121C (en) 2006-12-05
HRP20000247A2 (en) 2000-10-31
UY25341A1 (en) 1999-09-27
BG64125B1 (en) 2004-01-30
JP3569495B2 (en) 2004-09-22
BR9813308A (en) 2000-08-22
EA002656B1 (en) 2002-08-29
AU737668B2 (en) 2001-08-30
EP1027329A1 (en) 2000-08-16
CN1146537C (en) 2004-04-21
HUP0004735A3 (en) 2001-12-28
DK1027329T3 (en) 2003-02-24
IL135435A0 (en) 2001-05-20
JP2001521023A (en) 2001-11-06
TW449589B (en) 2001-08-11
PL340805A1 (en) 2001-02-26
IS2179B (en) 2006-12-15
SI1027329T1 (en) 2003-04-30
DZ2632A1 (en) 2003-03-08
UY25222A1 (en) 2000-12-29
MY123352A (en) 2006-05-31
UA67755C2 (en) 2004-07-15
ES2190620T3 (en) 2003-08-01
GB9722662D0 (en) 1997-12-24
HUP0004735A2 (en) 2001-10-28
MA24683A1 (en) 1999-07-01
ID24658A (en) 2000-07-27
TR200001135T2 (en) 2000-09-21
ATE232199T1 (en) 2003-02-15
CN1278246A (en) 2000-12-27
EA200000365A1 (en) 2000-12-25
GT199800165A (en) 2000-04-19

Similar Documents

Publication Publication Date Title
DE69425736T2 (en) Formyl- or cyano-substituted indole derivatives with a dopaminergic effect
DE69428903T2 (en) SUBSTITUTED 2-AMINOTETRALINE
JP3087763B2 (en) Novel heterocyclic compound and pharmaceutical composition containing the same
DE69617995T2 (en) INDOLALKYL DERIVATIVES OF BENZODIOXANMENTHYLAMINE AS 5-HT1A RECEPTOR LIGANDS
JP2022517396A (en) EGFR inhibitor salt, crystalline form and method for producing it
AP906A (en) Dofetilide polymorphs
JP2823356B2 (en) Neuromuscular blocker
JPS6126996B2 (en)
EP0074014A1 (en) 2-(2&#39;-hydroxy-3&#39;-(1,1,-dimethyl propylamino)-propoxy)-beta propiophenone, its addition salts, process for its preparation and medicaments
PT2370440E (en) 8-chloro-3-pentyl-3,7-dihydro-1h-purine-2,6-dione 2-amino-2-(hydroxymethyl)-1,3-propanediol anhydrate for the treatment of diseases
DE69022442T2 (en) Aminoalkoxyphenyl derivatives, processes for their preparation and compositions containing them.
EP2649996A1 (en) Crystalline forms of sartans like telmisartan with beta blockers
MXPA00004059A (en) Dofetilide polymorphs
JP2507764B2 (en) Lower alkylsulfamoylamines, salts thereof and uses thereof
CZ20001516A3 (en) Dofetilide polymorphs
CN112851599B (en) A compound with dicationic quaternary ammonium salt structure and its preparation method and application
US12215085B2 (en) Cholinesterase inhibitor polymorph and application thereof
SE502323C2 (en) Use of N- (2-hydroxyethyl) nicotinamide nitrate or a pharmaceutically acceptable salt thereof for the manufacture of a drug actively for the treatment of diseases associated with cerebral ischemia
DE69515133T2 (en) ANTIARRHYTMIC (S) ENANTIOMERS OF METHANSULPHONAMIDES
JPH01175937A (en) Arrhythmia treatment agent
DE3421252A1 (en) 1-PHENOXY-3-HYDROXYINDOLYLALKYLAMINO-3-PROPANOL COMPOUNDS, METHOD FOR THE PRODUCTION THEREOF AND PHARMACEUTICAL AGENTS CONTAINING THESE COMPOUNDS
HK1033933B (en) Dofetilide polymorphs
WO2013103004A1 (en) Crystal form of (2e)-3-(1h-indazol-3-yl)-n-(3-methoxyphenyl)-n-[3-(methylsulfonyl)propyl]but-2-enamide
MXPA00000507A (en) Thermodynamically stable modification of 1-(4-carbazolyloxy)-3- [2-(2-methoxyphenoxy)ethylamino]-2- propanole, process for its preparation and pharmaceutical compositions containing it