[go: up one dir, main page]

WO2006069766A1 - Process for obtaining enantiomers of cizolirtine - Google Patents

Process for obtaining enantiomers of cizolirtine Download PDF

Info

Publication number
WO2006069766A1
WO2006069766A1 PCT/EP2005/014023 EP2005014023W WO2006069766A1 WO 2006069766 A1 WO2006069766 A1 WO 2006069766A1 EP 2005014023 W EP2005014023 W EP 2005014023W WO 2006069766 A1 WO2006069766 A1 WO 2006069766A1
Authority
WO
WIPO (PCT)
Prior art keywords
process according
formula
base
diamine
catalyst system
Prior art date
Legal status (The legal status 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 status listed.)
Ceased
Application number
PCT/EP2005/014023
Other languages
French (fr)
Inventor
Antoni Torrens Jover
Helmut H. Buschmann
Detleff Heller
Hans Joachim Drexler
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Esteve Pharmaceuticals SA
Original Assignee
Laboratorios del Dr Esteve SA
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
Priority claimed from EP04380274A external-priority patent/EP1674458A1/en
Application filed by Laboratorios del Dr Esteve SA filed Critical Laboratorios del Dr Esteve SA
Publication of WO2006069766A1 publication Critical patent/WO2006069766A1/en
Anticipated expiration legal-status Critical
Ceased legal-status Critical Current

Links

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D231/00Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings
    • C07D231/02Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings not condensed with other rings
    • C07D231/10Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings not condensed with other rings having two or three double bonds between ring members or between ring members and non-ring members
    • C07D231/12Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings not condensed with other rings having two or three double bonds between ring members or between ring members and non-ring members with only hydrogen atoms, hydrocarbon or substituted hydrocarbon radicals, directly attached to ring carbon atoms

Definitions

  • the present invention relates to the asymmetric reduction of ketones using chiral catalytic systems to render nonracemic chiral alcohols. More particularly, it relates to a new process for the preparation of the pure enantiomers of an intermediate alcohol which is used in the preparation of Cizolirtine, ( ⁇ )-2-[phenyl(l -methyl- lH-pyrazol-5- yl)methoxy]-7V,N-dimethylethanamine and its enantiomers, comprising the enantioselective hydrogenation of a prochiral ketone.
  • (+)-I and (-)-I have been previously obtained by optical resolution of the Cizolirtine racemate by fractional crystallization with optically active acids (WO 99/02500) such as, for instance, with (-)- and (+)-di ⁇ p-toluoyltartaric acid (Torrens, A.; Castrillo, J. A.; Frigola,
  • the ( ⁇ )-Cizolirtine has been prepared by O-alkylation of compound ( ⁇ )-II of formula II:
  • the pure enantiomers of Cizolirtine (+)-I and (-)-I may be prepared by separately O-alkylating the enantiomerically pure intermediates (+)-II and (-)-II.
  • (+)-II and (-)-II are obtained either by reduction of a compound of formula III, which yields ( ⁇ )-II as a racemate, followed by procedures of optical resolution of the racemate ( ⁇ )-II, like fractional recrystallization from solvents or column chromatography [J.A: Hueso, J. Berrocal, B. Gutierrez, A.J. Farre y J. Frigola, Bioorg. Med. Chem. Lett. 1993, 3, 269], or by EPC synthesis starting from the prochiral ketone of formula III:
  • the chiral catalyst has to differentiate between the two aromatic rings. This can usually only be done with high selectivity if the two rings are different in terms of steric and/or electronic properties which is not obvious in the case of Cizolirtine.
  • the main strategy for the enantioselective reduction of aromatic and heteroaromatic prochiral ketones with high ee values comprises the use of an optically active diphosphane/Ru/-diamine/inorganic base catalyst system.
  • rhodium K. Kriis, T. Kanger, A.-M. Mu ⁇ risepp, M. Lopp, Tetrahedron: Asymmetry 2003, 14, 2271-2275.
  • cobalt K. Micskei, C. Hajdu, L. A. Wessjohann, L. Mercs,A. Kiss-Szikszai, T. Patonay, Tetrahedron: Asymmetry 2004, 15, 1735-1744] as metal for the asymmetric reduction of prochiral ketones.
  • Enantioselective hydrogenation of ketonic structures has been achieved with also a wide range of chiral ruthenium catalyst systems which can be prepared by different combinations of Ru (II) chiral phosphanes and diamine ligands.
  • the extent of the enantioselectivity obtained with the different ketones depends largely on the nature of the substituents of the prochiral ketone as shown by the state of the art [see, for instance, Table 2, on p. 53: R. Noyori, T. Ohl ⁇ ima, Angew. Chem. Int. Ed. 2001, 40, 40-73].
  • heteroaromatic ketones can be enantioselectively hydrogenated to nonracemic secondary alcohols with these chiral ruthenium catalysts systems [C. Chen, R. A. Reamer, J. R. Chilenski, C. J. McWilliams, Org. Lett. 2003 5, 5039;].
  • ketones with a phenyl and a heteroaryl in literature [K. Okano, K. Murata, T. Ikariya, Tetrahedron Lett. 2000, 41, 9277-9280].
  • the object of the present invention was to provide a process for the enantioselective hydrogenation of a phenyl pyrazoyl ketone.
  • This process should operate particularly well on industrial scale and be satisfactory as regards yield, conversion and enantiomer excess.
  • the process should be suitable for providing in an advantageous manner specific enantiomer-enriched alcohols as intermediates for the preparation of (+)- and (-)-Cizolirtine.
  • the inventors have achieved the enantioselective hydrogenation with a chiral ruthenium (II) catalyst system of a prochiral ketone with a phenyl and a methyl-pyrazol substituent comprising two nitrogen atoms, with high ee value and high conversion.
  • Investigations carried out by the inventors have shown in a no foreseeable manner, that the prochiral ketone with a phenyl and a methyl-pyrazol substituent provides the catalytical enantioselective hydrogenation of said ketone with high enantioselectivity and excellent conversion. This could not have been predicted from the nature of the substrate.
  • the present invention is directed to a process for the preparation of an enantiomerically enriched compound of formula (II):
  • the present invention is directed to a process for the preparation of an enantiomerically enriched compound of formula (II):
  • HI in the presence of a base and a chiral ruthenium (II) catalyst system comprising at least a bidentate phosphorous-containing ligand selected from ToIBINAP and BINAP and a diamine ligand selected DAIPEN and DPEN.
  • a chiral ruthenium (II) catalyst system comprising at least a bidentate phosphorous-containing ligand selected from ToIBINAP and BINAP and a diamine ligand selected DAIPEN and DPEN.
  • the process of the invention gives the desired product of formula II with high conversion and enantiomeric excess.
  • This process has the further advantage that the starting materials are not expensive and that it works under low or normal pressures. Similar hydrogenations are known, as mentioned above, but it is the first time they are applied to a pyrazol containing substrate. Although problems due to the coordination of the pyrazol could have been expected, on the contrary we have found that the reaction works remarkably well providing a simple route to the alcohols of formula (II) with very high conversion and enantiomeric excess. It allows the compounds of the above formula (II) to be synthesised directly from the compounds of formula (III), without any further intermediate steps or laborious separation of the isomeric forms.
  • the product of formula II is especially useful in the preparation of Cizolirtine enantiomers. The details of the process are discussed below.
  • the chiral ruthenium (II) catalyst system used in the process of the present invention is known to the person skilled in the art and is composed of Ruthenium (II) complexes with two different ligands, a bidentate phosphorous-containing ligand and a diamine, in the presence of a base.
  • Said catalyst system components can be provided to the reaction mixture individually to form the reactive catalyst system in situ o ⁇ they can be provided as preformed complexes.
  • the bidentate phosphorous-containing ligand is in general of the biphosphines or biphosphites types, more preferably it is of the biphosphine type.
  • nonracemic chiral diphosphines are 2,2'-bis(diphenyl-phosphino)-l,l '-binaphtyl (BINAP), ToIBINAP and XyIBINAP [R. Noyori, T. Ohkuma, Angew. Chem. Int. Ed., 2001, 40, 40-73], 2,2'-bis(diphenylphosphino)-l ,l '-dicyclopentane (BlCP) [P. Cao, X. Zhang, J. Org. Chem.
  • the diphosphine ligand comprises a binaphthyl group. They are more preferably selected from the group consisting of the enantiomers of 2,2'-bis(diphenyl-phosphino)-l,r-binaphtyl (BINAP), TOIBINAP and XyIBINAP [see R. Noyori, T. Ohkuma, Angew. Chem. Int. Ed., 2001 , 40, 40-73]. Suitable diamines are 1,2-diamine species that exhibit a sufficient activity or selectivity in the catalyst under consideration.
  • DAIPEN 1,2- butanediamine
  • DPEN 1,2-diphenylethylendiamine
  • DACH 1,2- diaminocyclohexane
  • Achiral amines are further discussed in US 6,743,921 which is incorporated herein by reference in its entirety.
  • the use of enantiomerically enriched diamines such as DAIPEN and DPEN has proved particularly advantageous; DPEN is preferable regarding costs and higher activity and selectivity.
  • the bidentate phosphorous-containing ligand together with the diamine and the ruthenium (II) form a complex referred to hereinafter as the ruthenium (II) component of the catalyst system.
  • Examples of preformed complexes of the ruthenium with the diphosphine ligand and the diamine include complexes represented by the formula RuX 2 LA wherein X represents a halogen atom or pseudo-halide group, preferably chloride or bromide, L represents the diphosphine ligand and A is the diamine.
  • Suitable examples are RuCl 2 [(S)-BINAP][(R,R)-DPEN], RuCl 2 [(S)-BTNAP] [(S 5 S)-DPEN], RuCl 2 [(R)-BINAP][(R,R)-DPEN], RuCl 2 [(R)-BINAP][(S,S)-DPEN], RuCl 2 [(R)- BINAP] [(R)-DAIPEN], RuCl 2 [(S)-BINAP][(S)-DAIPEN].
  • Said component is present in catalytic amounts, meaning less than stoichiometric relative to the ketone reactants and as low as possible while ensuring the optimum possible conversion rate.
  • the minimum amount of the ruthenium (II) component of the catalyst system may depend on the activity of the specific catalyst system composition, the reaction temperature, the concentration of the reactants and catalyst system components in the solution, the hydrogen pressure and the maximum time allowed for completion of the reaction. In a typical embodiments the molar ratio of the ruthenium
  • (II) component of the catalyst to the ketone reactant (s/c) is in the range from about 50 to 20000, preferably from about 200 to about 20.000, more preferably from about 10.000 to about 20.000.
  • Suitable bases include organic bases and inorganic bases which should not have a negative influence on, for example, the enantiomer purity of the products that are formed.
  • the base is selected from the group consisting of a hydroxide, Cp C 5 -alkoxide, bicarbonate, carbonate, di- and tribasic phosphate, borate, fluoride, amine optionally substituted with Ci-C 4 -alkyl or aryl, silane optionally substituted with Ci-C 3 - alkyl.
  • alkali metal alcoholates are advantageous, such as for example /-BuOK, as well as inorganic bases such as for example KOH or K 2 CO 3 .
  • organic nitrogen bases such as triethylamine and salts as for example AgCF 3 SO 3 .
  • /-BuOK is used.
  • the base used is /- BuOK it is preferably added to the reaction vessel in form of a solution of /-BuOK in /- BuOH. It has been found that a molar excess of base referred to the ruthenium (II) component of the catalyst system is advantageous.
  • the typical mole ratio base : ruthenium (II) component of the catalyst system is comprised between 10:1 and 1, more preferably between about 4:1 and about 2:1. It has been found that both the activity and the selectivity of the hydrogenation vary with the amount of the base. In this connection the activity of the hydrogenation increases with rising concentration of the base. However, if the concentration of base is too high there is a possibility of racemization of the end product, which is not desirable. A ratio of about 4:1 is particularly preferred.
  • the hydrogenation reaction is conducted in a solvent system that is capable of dissolving the catalyst system and is reaction-inert.
  • solvent system is used to indicate that a single solvent or a mixture of two or more solvents can be used.
  • reaction-inert is used to mean that the solvent system does not react unfavourably with the reactants, products, or the catalyst system.
  • the solvent system need not bring about complete solution of the ketone reactant or the chiral alcohol product.
  • the ketone reactant may be incompletely dissolved at the beginning of the reaction or the chiral alcohol product may be incompletely dissolved at the end of the reaction, or both.
  • Representative solvents are alcohol solvents such as methanol, ethanol, n-propanol, 2- propanol, n-butanol, sec-butanol or /-butanol and their mixtures, organic solvents containing heteroatoms such as DMF and ethers like THF.
  • the solvent system comprises an alcohol solvent, more preferably methanol, isopropanol, /-butanol and their mixtures. 7er/-butanol is particularly preferred.
  • the hydrogenation takes place in a suitable reactor known to the person skilled in the art, such as an autoclave. It is advisable to carry out the hydrogenation under an inert gas atmosphere.
  • suitable media are nitrogen gas or a noble gas such as argon.
  • the temperature during the reaction may in principle be chosen arbitrarily by the person skilled in the art as long as a sufficient quick and selective reaction is guaranteed. However, it has to be taken into account that the temperature depends strongly on solvent and that some catalyst systems are unstable above 40 0 C.
  • the reaction is suitably conducted at a temperature comprised between 10 and 45 °C, preferably between 20 and 35 0 C, and most preferably about 30 °C.
  • the hydrogenation refers to reacting the ketone with a source of hydrogen atoms under appropriate conditions so that two hydrogen atoms are added to the carbonyl group of the ketone to produce the hydroxyl group of the chiral alcohol.
  • the source of hydrogen atoms includes molecular hydrogen (H 2 ).
  • H 2 molecular hydrogen
  • the hydrogen pressure in the reaction is preferably low, typically at least about a 1.3 atm. Normally it is in the range from 0.8 to 100 bar. More typically the hydrogen pressure is in the range from 1.3 to 8 bar.
  • the ketone of formula (III) is known and can be prepared as described for example in WO99/07684 or any other method readily apparent to the person skilled in the art.
  • the ketone substrate (III), the catalyst system and the base are weighted and introduced in the reactor. Then the solvent is added and stirred to complete dissolution of the catalyst. Thereafter the base, if not a solid, is added. The reactor is brought to the adequate temperature and pressure to complete the reaction.
  • the ketone of formula (III) is dissolved in an appropriate solvent, then the constituents of the catalyst system or the catalyst in preformed form are added, and then the hydrogenation is performed at an appropriate temperature and suitable hydrogen pressure.
  • the ketone concentration ranges from about 0.025 to 0.1 mol/1, preferably from about 0.05 mol/1. In general the reaction is allowed to continue until complete conversion of the ketone. Times comprised between 1 to 1 10 hours are sufficient, although shorter times are preferred in terms of economy of the process.
  • the advantages associated with the invention are numerous:
  • the process according to the invention provides a simple means of access to isomers which were previously relatively difficult to obtain, and also allows this to be done on a large industrial scale with excellent productivity.
  • the process according to the invention makes it possible to prepare the desired product not only in high yields but also with very high enantioselectivity. No additional purification steps are needed, the products may be further processed directly just as they occur. Conversions of 100% of the ketone are achieved by the process of the present invention.
  • the enantiomers proportions achieved by the process of the invention are above 80 ee% and can be as high as 86 ee%.
  • the constituents of the catalyst may be used in several diasteromeric and enantiomeric forms and the complex in each case may therefore be present in so-called matched or mismatched configurations with regard to the chiral ketone, the person skilled in the art must check which pair works most suitably regarding selectivity.
  • the obtained hydrogenated product i.e. the enantiomers of the nonracemic alcohol mixtures [(+)-II and (-)-II]
  • additional purification for example one or more washing steps and/or recrystallisation from the solvent used, and may be separated off and worked up in the usual way.
  • the invention relates to a process as defined above which further comprises the step of O-alkylation of an enantiomerically enriched compound of formula (II) to yield the desired enantiomer of the pharmaceutically active Cizolirtine (I).
  • the compound of formula (II) is treated with an amine of formula
  • X is a suitable leaving group such as halogen, more preferably chlorine, bromine or iodine; a reactive esterif ⁇ ed hydroxyl, for example arylsulphonyloxy such as phenylsulphonyloxy; tosyloxy; mesyloxy; Ci -4 alkyl sulphonyloxy, for example methanesulphonyloxy; arylphosphoryloxy, for example diphenylphosphoryloxy, dibenzylphosphoryloxy or a Ci -4 alkyl phosphoryloxy, for example dimethylphosphoryloxy.
  • halogen more preferably chlorine, bromine or iodine
  • a reactive esterif ⁇ ed hydroxyl for example arylsulphonyloxy such as phenylsulphonyloxy; tosyloxy; mesyloxy; Ci -4 alkyl sulphonyloxy, for example methanesulphonyloxy; arylphosphoryloxy, for example diphen
  • the O-alkylation is carried out in conditions of phase transfer, using for example 2-chloro-N,iV,-dimethylethylamine (other leaving groups instead of chloro are possible), an alkaline aqueous solution such as NaOH or KOH, in the presence of a catalyst such as a quaternary ammonium salt.
  • a catalyst such as a quaternary ammonium salt.
  • the resulting product of formula I is enantiomerically enriched and it can be further purified using polar organic solvents.
  • a pharmaceutically acceptable salt of the compound of formula I can be formed.
  • the citrate salt can be prepared by dissolving the amine of formula I in ethanol and treating the solution with citric acid monohydrate.
  • the preparation of other salts will be readily apparent to the person skilled in the art. The following examples will further illustrate the invention, they should not be interpreted as limiting the scope of the invention.
  • the substrate and the components of the chiral ruthenium (II) catalyst system used in the process of the present invention bidentate phosphorous-containing ligand, amine and base (if the base is a solid) are weighed (not necessarily anaerobic) in a schlenk flask. With larger quantities of substrate (more than 1.5 mmol) the substrate is filled directly into the autoclave. The schlenk flask is securated and the solvent (stock solution) is added under anaerobic conditions. The formed suspension is stirred up to the dissolution of the chiral ruthenium (II) catalyst system (ca. 5 min).
  • the base solution is added with a securated Hamilton glass syringe and stirred again 5 min if it was not already added as a solid at the beginning. Afterwards the solution is transferred into the securated autoclave standing under vacuum (via capillary and argon pressure). The reaction solution is then heated up to the desired temperature. The desired hydrogen pressure is adjusted.
  • the substrate and the components of the chiral ruthenium (II) catalyst system used in the process of the present invention bidentate phosphorous-containing ligand, amine and base (if the base is a solid) are weighed (not necessarily anaerobic) and given in a temperaturable two neck reaction vessel. This is connected to a dropping funnel containing the solvent (stock solution, anaerobic conditions) and the normal pressure registration equipment. Afterwards this complete system is carefully securated. Furthermore the solution in the dropping funnel is added to the solids in the reaction vessel and the base solution is added to the suspension. Then the argon is replaced with hydrogen (3 x securation with hydrogen). Normal pressure is adjusted by deflating the overpressure over a bubble counter and the measurement is started.
  • Example 1 Preparation of the enantiomerically enriched phenyl l-methylpirazoyl carbiiiol
  • the compound was prepared from 0 5 mmol phenyl 1 -methylpyrazoyl ketone 0.01 mmol ⁇ -Ru(BINAP); 0.01 mmol R 1 R-DPEN
  • the compound was prepared from 1 mmol phenyl 1-methylpyrazoyl ketone 0.01 mmol /2-Ru(BINAP); 0.01 mmol R 1 R-DPEN
  • the compound was prepared from 1 mmol phenyl 1 -methylpyrazoyl ketone 0.01 mmol ⁇ -Ru(BiNAP); 0.01 mmol R 1 R-DPEN
  • the compound was prepared from 1 mmol phenyl 1-methylpyrazoyl ketone
  • the compound was prepared from 1 mmol phenyl 1 -methylpyrazoyl ketone
  • the compound was prepared from 2 mmol phenyl 1 -methylpirazoyl ketone
  • the compound was prepared from 50 mmol phenyl 1-methylpyrazoyl ketone

Landscapes

  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Organic Low-Molecular-Weight Compounds And Preparation Thereof (AREA)
  • Low-Molecular Organic Synthesis Reactions Using Catalysts (AREA)

Abstract

A process is described for the preparation of a precursor alcohol of Cizolirtine, (±)-2-[phenyl(1-methyl-1H-pyrazol-5-yl)methoxy]-N,N-dimethylethanamine and its enantiomers, it comprises the asymmetric reduction of a prochiral ketone in the presence of a chiral ruthenium (II) catalyst system comprising at least a bidentate phosphorous-containing ligand and a diamine ligand to render chiral alcohols. The chiral alcohols are further O-alkylated to render the corresponding pharmaceutically active ethanamines.

Description

PROCESS FOR OBTAINING ENANTIOMERS OF CIZOLIRTINE
FIELD OF THE INVENTION
The present invention relates to the asymmetric reduction of ketones using chiral catalytic systems to render nonracemic chiral alcohols. More particularly, it relates to a new process for the preparation of the pure enantiomers of an intermediate alcohol which is used in the preparation of Cizolirtine, (±)-2-[phenyl(l -methyl- lH-pyrazol-5- yl)methoxy]-7V,N-dimethylethanamine and its enantiomers, comprising the enantioselective hydrogenation of a prochiral ketone.
BACKGROUND OF THE INVENTION
The compound (±)-2-[phenyl(l -methyl- lH-pyrazol-5-yl)methoxy]-jV,N- dimethylethanamine, also referred to as (±)-5-[α-(2-dimethylaminoethoxy)benzyl]-l- methyl-l/-/-pyrazole, or Cizolirtine of formula (I)
Figure imgf000002_0001
(D was described in the European patent EP 289 380. This compound is a potent analgesic which is currently in phase II clinical trials.
The two enantiomers of Cizolirtine, hereinafter referred to as (+)-I and (-)-I, have been previously obtained by optical resolution of the Cizolirtine racemate by fractional crystallization with optically active acids (WO 99/02500) such as, for instance, with (-)- and (+)-di~p-toluoyltartaric acid (Torrens, A.; Castrillo, J. A.; Frigola,
J.; Salgado, L.; Redondo, J. Chirality, 1999, 1 1, 63). An enantiomerically pure compound synthesis (EPC synthesis) starting from ethyl (R)-mandelate of the intermediate permitted the assignation of the (R) absolute configuration to the (+)-I isomer (Hueso-Rodriguez, J. A.; Berrocal, J.; Gutierrez, B.; Farre, A..; Frigola, J. Bioorg. Med. Chem. Lett. 1993, 3, 269).
The (±)-Cizolirtine has been prepared by O-alkylation of compound (±)-II of formula II:
Figure imgf000003_0001
(H)
The pure enantiomers of Cizolirtine (+)-I and (-)-I may be prepared by separately O-alkylating the enantiomerically pure intermediates (+)-II and (-)-II.
The enantiomerically pure compounds (+)-II and (-)-II are obtained either by reduction of a compound of formula III, which yields (±)-II as a racemate, followed by procedures of optical resolution of the racemate (±)-II, like fractional recrystallization from solvents or column chromatography [J.A: Hueso, J. Berrocal, B. Gutierrez, A.J. Farre y J. Frigola, Bioorg. Med. Chem. Lett. 1993, 3, 269], or by EPC synthesis starting from the prochiral ketone of formula III:
Figure imgf000003_0002
(III)
The enantioselective reduction of prochiral ketones in organic synthesis to obtain secondary alcohols with high enantiomeric purity is of high interest since they can be valuable intermediates for the manufacture of active compounds. Accordingly, a number of strategies for the asymmetric reduction of prochiral ketones to single enantiomer alcohols have been developed [R. Noyori, T. Ohkuma, Angew. Chem. Int. Ed., 2001 , 40, 40-73].
A possibility exists in the use of oxazoborolidines as ligands or catalysts which constitutes a major advance in the asymmetric reduction of prochiral ketones. The use of said chiral ligands or catalysts in combination with achiral reducing agents for the preparation of (+)-I and (-)-I has been described in patent EP 1 029 852 Bl . Further examples can be found in the literature [E. J. Corey, Ch. J. Helal, Tetrahedron Lett. 1995, 36, 9153-9156; E. J. Corey, Ch. J. Helal, Tetrahedron Lett. 1996, 37, 5675-5678]. However, for diaryl methanols, the reduction of the corresponding ketone precursors is problematic. The chiral catalyst has to differentiate between the two aromatic rings. This can usually only be done with high selectivity if the two rings are different in terms of steric and/or electronic properties which is not obvious in the case of Cizolirtine. The main strategy for the enantioselective reduction of aromatic and heteroaromatic prochiral ketones with high ee values comprises the use of an optically active diphosphane/Ru/-diamine/inorganic base catalyst system. Moreover, there are also examples with rhodium [K. Kriis, T. Kanger, A.-M. Muϋrisepp, M. Lopp, Tetrahedron: Asymmetry 2003, 14, 2271-2275.] or cobalt [K. Micskei, C. Hajdu, L. A. Wessjohann, L. Mercs,A. Kiss-Szikszai, T. Patonay, Tetrahedron: Asymmetry 2004, 15, 1735-1744] as metal for the asymmetric reduction of prochiral ketones.
Enantioselective hydrogenation of ketonic structures has been achieved with also a wide range of chiral ruthenium catalyst systems which can be prepared by different combinations of Ru (II) chiral phosphanes and diamine ligands. The extent of the enantioselectivity obtained with the different ketones depends largely on the nature of the substituents of the prochiral ketone as shown by the state of the art [see, for instance, Table 2, on p. 53: R. Noyori, T. Ohlαima, Angew. Chem. Int. Ed. 2001, 40, 40-73]. It is also known that heteroaromatic ketones can be enantioselectively hydrogenated to nonracemic secondary alcohols with these chiral ruthenium catalysts systems [C. Chen, R. A. Reamer, J. R. Chilenski, C. J. McWilliams, Org. Lett. 2003 5, 5039;]. One finds further asymmetric hydrogenations with ketones with a phenyl and a heteroaryl in literature [K. Okano, K. Murata, T. Ikariya, Tetrahedron Lett. 2000, 41, 9277-9280].
However, it has been found that one specific catalyst or a class of catalysts cannot be used equally well in all hydrogenations. Thus, to attain satisfactory ee values by the enantioselective hydrogenation of prochiral ketones, each hydrogenation problem has to be investigated separately with regard to the substrate, the catalyst and the reaction conditions for finding the optimal conditions to obtain the best results.
The object of the present invention was to provide a process for the enantioselective hydrogenation of a phenyl pyrazoyl ketone. This process should operate particularly well on industrial scale and be satisfactory as regards yield, conversion and enantiomer excess. In particular the process should be suitable for providing in an advantageous manner specific enantiomer-enriched alcohols as intermediates for the preparation of (+)- and (-)-Cizolirtine.
SUMMARY OF THE INVENTION
Surprisingly, the inventors have achieved the enantioselective hydrogenation with a chiral ruthenium (II) catalyst system of a prochiral ketone with a phenyl and a methyl-pyrazol substituent comprising two nitrogen atoms, with high ee value and high conversion. Investigations carried out by the inventors have shown in a no foreseeable manner, that the prochiral ketone with a phenyl and a methyl-pyrazol substituent provides the catalytical enantioselective hydrogenation of said ketone with high enantioselectivity and excellent conversion. This could not have been predicted from the nature of the substrate. We have therefore applied this process to the synthesis of the enantiomerically pure intermediates (+)-H and (-)-II and to a process to obtain Cizolirtine and its enantiomers. This process should operate particularly well on an industrial scale and be satisfactory with regard to enantiomer excess, amount and availability of catalyst and in general raw material costs.
Accordingly, the present invention is directed to a process for the preparation of an enantiomerically enriched compound of formula (II):
Figure imgf000005_0001
(H) which comprises the asymmetric hydrogenation of a prochiral ketone of formula (III)
Figure imgf000006_0001
(III) in the presence of a base and a chiral ruthenium (II) catalyst system comprising at least a bidentate phosphorous-containing ligand and a diamine ligand.
Said process allows the preparation of the known intermediates of formula II, which can be optionally transformed in enantiomerically pure pharmaceutically active compounds such as (+)-Cizolirtine and (-)-Cizolirtine.
According to a further aspect, the present invention is directed to a process for the preparation of an enantiomerically enriched compound of formula (II):
Figure imgf000006_0002
(H) which comprises the asymmetric hydrogenation of a prochiral ketone of formula (III)
Figure imgf000006_0003
(HI) in the presence of a base and a chiral ruthenium (II) catalyst system comprising at least a bidentate phosphorous-containing ligand selected from ToIBINAP and BINAP and a diamine ligand selected DAIPEN and DPEN. DETAILED DESCRIPTION OF THE INVENTION
The process of the invention gives the desired product of formula II with high conversion and enantiomeric excess. This process has the further advantage that the starting materials are not expensive and that it works under low or normal pressures. Similar hydrogenations are known, as mentioned above, but it is the first time they are applied to a pyrazol containing substrate. Although problems due to the coordination of the pyrazol could have been expected, on the contrary we have found that the reaction works remarkably well providing a simple route to the alcohols of formula (II) with very high conversion and enantiomeric excess. It allows the compounds of the above formula (II) to be synthesised directly from the compounds of formula (III), without any further intermediate steps or laborious separation of the isomeric forms.
The product of formula II is especially useful in the preparation of Cizolirtine enantiomers. The details of the process are discussed below.
The chiral ruthenium (II) catalyst system used in the process of the present invention is known to the person skilled in the art and is composed of Ruthenium (II) complexes with two different ligands, a bidentate phosphorous-containing ligand and a diamine, in the presence of a base. Said catalyst system components can be provided to the reaction mixture individually to form the reactive catalyst system in situ oτ they can be provided as preformed complexes. The bidentate phosphorous-containing ligand is in general of the biphosphines or biphosphites types, more preferably it is of the biphosphine type. Illustrative examples of nonracemic chiral diphosphines are 2,2'-bis(diphenyl-phosphino)-l,l '-binaphtyl (BINAP), ToIBINAP and XyIBINAP [R. Noyori, T. Ohkuma, Angew. Chem. Int. Ed., 2001, 40, 40-73], 2,2'-bis(diphenylphosphino)-l ,l '-dicyclopentane (BlCP) [P. Cao, X. Zhang, J. Org. Chem. 1999 64, 2127-2129.], 2,2',6,6'-tetramethoxy-4,4'-bis-3,3'- bipyridine (P-Phos), Tol-P-Phos and Xyl-P-Phos [J. Wu, H. Chen, W. Kwok, R. Guo,Z. Zhou, C. Yeung, A. S. C. Chan, J. Org. Chem. 2002, 63, 7908-7910], 4,12- bis(diphenylphosphino)[2.2]paracyclophane (PhanePhos) and Xyl-PhanePhos [M. J. Burk, W. Hems, D. Herzberg, C. Malan, A. Zanotti-Gerosa, Org. Lett. 2000, 2, 4173- 4176] and equivalents thereto that are recognized by those skilled in the art. In one preferred embodiment the diphosphine ligand comprises a binaphthyl group. They are more preferably selected from the group consisting of the enantiomers of 2,2'-bis(diphenyl-phosphino)-l,r-binaphtyl (BINAP), TOIBINAP and XyIBINAP [see R. Noyori, T. Ohkuma, Angew. Chem. Int. Ed., 2001 , 40, 40-73]. Suitable diamines are 1,2-diamine species that exhibit a sufficient activity or selectivity in the catalyst under consideration. They can be chtral or non-chiral. Ilustrative examples are any stereoisomers of l ,l-bis(4-methoxyphenyl)-3 -methyl- 1,2- butanediamine (DAIPEN), 1 ,2-diphenylethylendiamine (DPEN), 1,2- diaminocyclohexane (DACH) or achiral diamines such as ethylenediamine. Achiral amines are further discussed in US 6,743,921 which is incorporated herein by reference in its entirety.
The use of enantiomerically enriched diamines such as DAIPEN and DPEN has proved particularly advantageous; DPEN is preferable regarding costs and higher activity and selectivity. The bidentate phosphorous-containing ligand together with the diamine and the ruthenium (II) form a complex referred to hereinafter as the ruthenium (II) component of the catalyst system. Examples of preformed complexes of the ruthenium with the diphosphine ligand and the diamine include complexes represented by the formula RuX2LA wherein X represents a halogen atom or pseudo-halide group, preferably chloride or bromide, L represents the diphosphine ligand and A is the diamine. Suitable examples are RuCl2 [(S)-BINAP][(R,R)-DPEN], RuCl2 [(S)-BTNAP] [(S5S)-DPEN], RuCl2 [(R)-BINAP][(R,R)-DPEN], RuCl2 [(R)-BINAP][(S,S)-DPEN], RuCl2 [(R)- BINAP] [(R)-DAIPEN], RuCl2 [(S)-BINAP][(S)-DAIPEN].
Said component is present in catalytic amounts, meaning less than stoichiometric relative to the ketone reactants and as low as possible while ensuring the optimum possible conversion rate. The minimum amount of the ruthenium (II) component of the catalyst system may depend on the activity of the specific catalyst system composition, the reaction temperature, the concentration of the reactants and catalyst system components in the solution, the hydrogen pressure and the maximum time allowed for completion of the reaction. In a typical embodiments the molar ratio of the ruthenium
(II) component of the catalyst to the ketone reactant (s/c) is in the range from about 50 to 20000, preferably from about 200 to about 20.000, more preferably from about 10.000 to about 20.000.
Suitable bases include organic bases and inorganic bases which should not have a negative influence on, for example, the enantiomer purity of the products that are formed. Preferably, the base is selected from the group consisting of a hydroxide, Cp C5-alkoxide, bicarbonate, carbonate, di- and tribasic phosphate, borate, fluoride, amine optionally substituted with Ci-C4-alkyl or aryl, silane optionally substituted with Ci-C3- alkyl.
In this connection alkali metal alcoholates are advantageous, such as for example /-BuOK, as well as inorganic bases such as for example KOH or K2CO3. Also used are organic nitrogen bases such as triethylamine and salts as for example AgCF3SO3. In a more preferred embodiment /-BuOK is used. When the base used is /- BuOK it is preferably added to the reaction vessel in form of a solution of /-BuOK in /- BuOH. It has been found that a molar excess of base referred to the ruthenium (II) component of the catalyst system is advantageous. The typical mole ratio base : ruthenium (II) component of the catalyst system is comprised between 10:1 and 1, more preferably between about 4:1 and about 2:1. It has been found that both the activity and the selectivity of the hydrogenation vary with the amount of the base. In this connection the activity of the hydrogenation increases with rising concentration of the base. However, if the concentration of base is too high there is a possibility of racemization of the end product, which is not desirable. A ratio of about 4:1 is particularly preferred.
The hydrogenation reaction is conducted in a solvent system that is capable of dissolving the catalyst system and is reaction-inert. The term solvent system is used to indicate that a single solvent or a mixture of two or more solvents can be used. The term reaction-inert is used to mean that the solvent system does not react unfavourably with the reactants, products, or the catalyst system. The solvent system need not bring about complete solution of the ketone reactant or the chiral alcohol product. The ketone reactant may be incompletely dissolved at the beginning of the reaction or the chiral alcohol product may be incompletely dissolved at the end of the reaction, or both. Representative solvents are alcohol solvents such as methanol, ethanol, n-propanol, 2- propanol, n-butanol, sec-butanol or /-butanol and their mixtures, organic solvents containing heteroatoms such as DMF and ethers like THF. Preferably the solvent system comprises an alcohol solvent, more preferably methanol, isopropanol, /-butanol and their mixtures. 7er/-butanol is particularly preferred.
The hydrogenation takes place in a suitable reactor known to the person skilled in the art, such as an autoclave. It is advisable to carry out the hydrogenation under an inert gas atmosphere. Suitable media are nitrogen gas or a noble gas such as argon.
The temperature during the reaction may in principle be chosen arbitrarily by the person skilled in the art as long as a sufficient quick and selective reaction is guaranteed. However, it has to be taken into account that the temperature depends strongly on solvent and that some catalyst systems are unstable above 40 0C. In typical embodiments the reaction is suitably conducted at a temperature comprised between 10 and 45 °C, preferably between 20 and 35 0C, and most preferably about 30 °C.
The hydrogenation refers to reacting the ketone with a source of hydrogen atoms under appropriate conditions so that two hydrogen atoms are added to the carbonyl group of the ketone to produce the hydroxyl group of the chiral alcohol. Preferably the source of hydrogen atoms includes molecular hydrogen (H2). If the hydrogenation is carried out in the presence of molecular hydrogen, the hydrogen pressure in the reaction is preferably low, typically at least about a 1.3 atm. Normally it is in the range from 0.8 to 100 bar. More typically the hydrogen pressure is in the range from 1.3 to 8 bar. The ketone of formula (III) is known and can be prepared as described for example in WO99/07684 or any other method readily apparent to the person skilled in the art. Normally the ketone substrate (III), the catalyst system and the base (if it is a solid) are weighted and introduced in the reactor. Then the solvent is added and stirred to complete dissolution of the catalyst. Thereafter the base, if not a solid, is added. The reactor is brought to the adequate temperature and pressure to complete the reaction. Alternatively, the ketone of formula (III) is dissolved in an appropriate solvent, then the constituents of the catalyst system or the catalyst in preformed form are added, and then the hydrogenation is performed at an appropriate temperature and suitable hydrogen pressure. The ketone concentration ranges from about 0.025 to 0.1 mol/1, preferably from about 0.05 mol/1. In general the reaction is allowed to continue until complete conversion of the ketone. Times comprised between 1 to 1 10 hours are sufficient, although shorter times are preferred in terms of economy of the process.
The advantages associated with the invention are numerous: The process according to the invention provides a simple means of access to isomers which were previously relatively difficult to obtain, and also allows this to be done on a large industrial scale with excellent productivity. The process according to the invention makes it possible to prepare the desired product not only in high yields but also with very high enantioselectivity. No additional purification steps are needed, the products may be further processed directly just as they occur. Conversions of 100% of the ketone are achieved by the process of the present invention. The enantiomers proportions achieved by the process of the invention are above 80 ee% and can be as high as 86 ee%. Since the constituents of the catalyst (diamine, ruthenium (II) and bidentate phosphorous containg ligand) may be used in several diasteromeric and enantiomeric forms and the complex in each case may therefore be present in so-called matched or mismatched configurations with regard to the chiral ketone, the person skilled in the art must check which pair works most suitably regarding selectivity.
In a preferred embodiment the process is directed to the synthesis of each of the following alcohols of formula II with the highest possible enantiomeric purity:
Figure imgf000011_0001
R
Once the hydrogenation is completed, the obtained hydrogenated product, i.e. the enantiomers of the nonracemic alcohol mixtures [(+)-II and (-)-II], may be subjected to additional purification, for example one or more washing steps and/or recrystallisation from the solvent used, and may be separated off and worked up in the usual way.
Thus, in another aspect, the invention relates to a process as defined above which further comprises the step of O-alkylation of an enantiomerically enriched compound of formula (II) to yield the desired enantiomer of the pharmaceutically active Cizolirtine (I). To this end, the compound of formula (II) is treated with an amine of formula
X-CH2CH2N(Me)2
wherein X is a suitable leaving group such as halogen, more preferably chlorine, bromine or iodine; a reactive esterifϊed hydroxyl, for example arylsulphonyloxy such as phenylsulphonyloxy; tosyloxy; mesyloxy; Ci-4 alkyl sulphonyloxy, for example methanesulphonyloxy; arylphosphoryloxy, for example diphenylphosphoryloxy, dibenzylphosphoryloxy or a Ci-4 alkyl phosphoryloxy, for example dimethylphosphoryloxy.
An appropriate O-alkylation has been described in EP289 380 or WO 99/07684, the content of these patent applications is incorporated herein in their entirety. The alkylation is preferably carried out directly in the same reaction medium resulting from the process of the invention, without further purification of the carbinol. Alternatively the solvent can be evaporated and an apolar solvent such as toluene added for the alkylation.
In general, the O-alkylation is carried out in conditions of phase transfer, using for example 2-chloro-N,iV,-dimethylethylamine (other leaving groups instead of chloro are possible), an alkaline aqueous solution such as NaOH or KOH, in the presence of a catalyst such as a quaternary ammonium salt. Accordingly, the same solvent as the one used in the process of the invention is used, such as toluene. In these conditions we have the further advantage that the impurities like any remaining zinc salts are also eliminated through the aqueous phase.
The resulting product of formula I is enantiomerically enriched and it can be further purified using polar organic solvents. Further, a pharmaceutically acceptable salt of the compound of formula I can be formed. For example, the citrate salt can be prepared by dissolving the amine of formula I in ethanol and treating the solution with citric acid monohydrate. The preparation of other salts will be readily apparent to the person skilled in the art. The following examples will further illustrate the invention, they should not be interpreted as limiting the scope of the invention.
EXAMPLES General Methods and Materials. a) Reactions in autoclave
The substrate and the components of the chiral ruthenium (II) catalyst system used in the process of the present invention: bidentate phosphorous-containing ligand, amine and base (if the base is a solid) are weighed (not necessarily anaerobic) in a schlenk flask. With larger quantities of substrate (more than 1.5 mmol) the substrate is filled directly into the autoclave. The schlenk flask is securated and the solvent (stock solution) is added under anaerobic conditions. The formed suspension is stirred up to the dissolution of the chiral ruthenium (II) catalyst system (ca. 5 min). Then the base solution is added with a securated Hamilton glass syringe and stirred again 5 min if it was not already added as a solid at the beginning. Afterwards the solution is transferred into the securated autoclave standing under vacuum (via capillary and argon pressure). The reaction solution is then heated up to the desired temperature. The desired hydrogen pressure is adjusted.
b) Reactions at normal pressure
The substrate and the components of the chiral ruthenium (II) catalyst system used in the process of the present invention: bidentate phosphorous-containing ligand, amine and base (if the base is a solid) are weighed (not necessarily anaerobic) and given in a temperaturable two neck reaction vessel. This is connected to a dropping funnel containing the solvent (stock solution, anaerobic conditions) and the normal pressure registration equipment. Afterwards this complete system is carefully securated. Furthermore the solution in the dropping funnel is added to the solids in the reaction vessel and the base solution is added to the suspension. Then the argon is replaced with hydrogen (3 x securation with hydrogen). Normal pressure is adjusted by deflating the overpressure over a bubble counter and the measurement is started. Example 1. Preparation of the enantiomerically enriched phenyl l-methylpirazoyl carbiiiol
Table 1: Preparation of the enantiomeπcally enriched phenyl l-methylpirazoyl carbinol (variation of standard condition*)
Figure imgf000014_0001
* Standard conditionb 0 01 mmol R /U-Ru(BiNAP), 0 01 mol amine, 0 5 or 1 mmol 1-methylpirazoyl carbinol, 0 04 mmol /-BuOK1 20 ml solvent, 1 - 100 bar H2, 10 - 45 0C
Entries 1 and 2 according to method a)
The compound was prepared from 0 5 mmol phenyl 1 -methylpyrazoyl ketone 0.01 mmol Λ-Ru(BINAP); 0.01 mmol R1R-DPEN
0.04 mmol /-BuOK (40 μl, /-BuOK 1.0 M solution in /-BuOH);
20 ml methanol, at 250C or 300C and 100 bar H2. Conversion: 100 % after 2 h with 42 %ee for 30 0C and 100 % after 18 h with 53 %ee for 25 0C.
Entries 3, 4 and 5 according to method a)
The compound was prepared from 1 mmol phenyl 1-methylpyrazoyl ketone 0.01 mmol /2-Ru(BINAP); 0.01 mmol R1R-DPEN
0.04 mmol /-BuOK (40 μl, /-BuOK 1.0 M solution in /-BuOH);
20 ml isopropanol, at 250C, 300C or 35 0C and 8 bar H2.
Conversion: 100 % after 3.5 h with 73 %ee for 35 0C, 100 % after 2 h with 19 %ee for 30 0C and
100 % after 5 h with 81 %ee for 25 0C.
Entries 6 and 7 according to method a)
The compound was prepared from 1 mmol phenyl 1 -methylpyrazoyl ketone 0.01 mmol ^-Ru(BiNAP); 0.01 mmol R1R-DPEN
0.04 mmol /-BuOK (40 μl, /-BuOK 1.0 M solution in /-BuOH);
20 ml /-butanol or 19 ml /-butanol and 1 ml isopropanol; at 30°C and 8 bar H2.
Conversion: 100 % after 3.5 h with 82 %ee for 20 ml /-butanol and 100 % after 1 h with 80 %ee for 19 ml /-butanol and 1 ml isopropanol. Entries 8 and 9 according to method a)
The compound was prepared from 1 mmol phenyl 1-methylpyrazoyl ketone
0.01 mmol 7?-Ru(BINAP); 0.01 mmol tf-DAIPEN or ethylendiamine; 0.04 mmol /-BuOK (40 μl, /-BuOK 1.0 M solution in /-BuOH);
20 ml isopropanol; at 25°C and 8 bar H2.
Conversion: 100 % after 3 h with 73 %ee for DAIPEN and
100 % after 4 h with 33 %ee for ethyl endiamin. Entries 10 and 11 according to method b)
The compound was prepared from 1 mmol phenyl 1 -methylpyrazoyl ketone
0.01 mmol /J-Ru(BINAP); 0.01 mmol Λ,i?-DPEN
0.04 mmol /-BuOK (40 μl, /-BuOK 1.0 M solution in /-BuOH); 20 ml isopropanol or 19 ml /-butanol and 1 ml isopropanol; at 25°C and 1 bar H2.
Conversion: 98 % after 20 h with 75 %ee for 20 ml isopropanol and
100 % after 20 h with 75 %ee for 19 ml /-butanol and 1 ml isopropanol.
The best results where obtained with the 19 to 1 mixture of /-butanol and isopropanol at 8 bar and 30 0C, see example 7.
Example 2. Preparation of the enantiomerically enriched phenyl 1-methylpirazoyl carbinol
Table 2: Preparation of the enantiomerically enπched phenyl 1-methylpirazoyl carbinol (variation of standard condition*)
Figure imgf000017_0001
* Standard conditions 0 01 mmol Λ,Λ-Ru(BINAP), 0 01 mol amine, 2 or 50 mmol 1-methylpirazoyl carbinol, 0 04 mmol /-BuOK, 20 ml solvent, 50 bar H2, 30 0C * 0 20 mmol /-BuOK
Entries 12 and 13 according to method a)
The compound was prepared from 2 mmol phenyl 1 -methylpirazoyl ketone
0.01 mmol Λ,Λ-Ru(BINAP) or Λ,Λ-Ru(TolBINAP); 0.01 mmol R, R-OPEN;
0 04 mmol /-BuOK (80 μl, /-BuOK 0.5 M solution in /-BuOH);
19 ml /-butanol and 1 ml isopropanol; at 30 0C and 50 bar H2.
Conversion: 100 % after 0,25 h with 82 %ee with R1R-Ru(B INAP) and 100 % after 0,25 h with 86 %ee with /?,^-Ru(TolBINAP).
Entry 14 according to method a)
The compound was prepared from 50 mmol phenyl 1-methylpyrazoyl ketone
0 01 mmol R, R-Ru(BW AP); 0.01 mmol R.R-OPEN;
0.20 mmol /-BuOK (400 μl, /-BuOK 0 5 M solution in /-BuOH); 190 ml Mπitanol and 10 ml isopropanol; at 30 0C and 50 bar H2.
Conversion: 86 % after 1 ,5 h with 83 %ee and 100 % after 3 h.
The best results concerning the selectivity where obtained with Λ,i?-Ru(TolBINAP) entry 13 and concerning the activity with the s/c of 5000 (TOF = 1650 h~') entry 14.

Claims

1. A process for the preparation of an enantiomerically enriched compound of formula (II):
Figure imgf000019_0001
(II) which comprises the asymmetric hydrogenation of a prochiral ketone of formula (III)
Figure imgf000019_0002
(III) in the presence of a base and a chiral ruthenium (II) catalyst system comprising at least a bidentate phosphorous-containing ligand and a diamine ligand.
2. A process according to claim 1 , wherein the bidentate phosphorous-containing ligand is a bisphosphine ligand comprising a binaphthyl group, preferably selected from the group formed by the stereoisomers of 2,2'-bis(diphenyl-phosphino)-l ,l '-binaphtyl (BINAP), ToIBINAP and XyIBINAP.
3. A process according to claim 1 wherein the diamine is an enantiomerically-enriched 1 ,2 diamine, preferably selected from the group consisting of l,l-bis(4- methoxyphenyl)-3 -methyl- 1 ,2-butanediamine (DAIPEN), 1,2-diphenylethylendiamine (DPEN) or 1 ,2-diaminocyclohexane (DACH).
4. A process according to claim 3 wherein the diamine is DPEN.
5. A process according to claim 1 wherein the base is selected from alkali metal alcoholates, preferably /-butanolate.
6. A process according to claim 1 wherein the base is selected from /-BuOK, KOH, K2CO3, NEt3 and AgCF3SO3, preferably /-BuOK.
7. A process according to claim 1 wherein the mole ratio base : ruthenium (II) component of the catalyst system is comprised between 10:1 and 1 :1, preferably between 4: 1 and 1 :1, more preferably between about 4: 1 and 2:1.
8. A process according to claim 1 wherein the solvent is an alcohol, preferably selected from methanol, isopropanol, Z-butanol and their mixtures, more preferably is Z-butanol.
9. A process according to claim 1 which further comprises an O-alkylation of the enantiomerically enriched compound of formula II to prepare respectively (+)- Cizolirtine and (-)-Cizolirtine.
10. A process according to claim 9 wherein the O-alkylation is carried out on the product of the process as defined in anyone of claims 1-8, without an intermediate separation or purification step.
1 1. A process for the preparation of an enantiomerically enriched compound of formula (II):
Figure imgf000020_0001
(H) which comprises the asymmetric hydrogenation of a prochiral ketone of formula (III)
Figure imgf000021_0001
(III) in the presence of a base and a chiral ruthenium (II) catalyst system comprising at least a bidentate phosphorous-containing ligand selected from ToIBINAP and BINAP and a diamine ligand selected DAIPEN and DPEN.
PCT/EP2005/014023 2004-12-27 2005-12-26 Process for obtaining enantiomers of cizolirtine Ceased WO2006069766A1 (en)

Applications Claiming Priority (4)

Application Number Priority Date Filing Date Title
EP04380274A EP1674458A1 (en) 2004-12-27 2004-12-27 Process for obtaining enantiomers of cizolirtine
EP04380274.3 2004-12-27
US11/041,667 2005-01-24
US11/041,667 US20060142589A1 (en) 2004-12-27 2005-01-24 Process for obtaining enantiomers of Cizolirtine

Publications (1)

Publication Number Publication Date
WO2006069766A1 true WO2006069766A1 (en) 2006-07-06

Family

ID=35999570

Family Applications (1)

Application Number Title Priority Date Filing Date
PCT/EP2005/014023 Ceased WO2006069766A1 (en) 2004-12-27 2005-12-26 Process for obtaining enantiomers of cizolirtine

Country Status (1)

Country Link
WO (1) WO2006069766A1 (en)

Non-Patent Citations (3)

* Cited by examiner, † Cited by third party
Title
ANTONI TORRENS, JOSE A CASTRILLO, ALEX XLAPAROLS, JORDI REDONDO: "Enantioselective Synthesis of (R)- and (S)-Cizolirtine; Application of Oxazaborolidine-Catalysed Asymmetric Borane Reduction to Azolyl Phenyl Ketones", SYNLETT, no. 6, 1999, pages 765 - 767, XP001205886 *
CHENG-YI CHEN, ROBERT A REAMER, JENNIFER R CHILENSKI AND CHRIS J MCWILLIAMS: "Highly Enantioselective hydrogenation of Aromatic-Heteroaromatic ketones", ORGANIC LETTERS, vol. 5, no. 2, 2003, pages 5039 - 5042, XP002327203 *
RYOJI NOYORI AND TAKESHI OHKUMA: "Asymetric Catalysis by Architectural and Functional Molecular Engineering : Practical Chemo- and Stereoselective Hydrogenation of Ketones", ANGEWANDTE CHEMIE INT ED, vol. 40, 2001, pages 40 - 73, XP000998801 *

Similar Documents

Publication Publication Date Title
US8563739B2 (en) Ruthenium complexes having hybrid amine ligands, their preparation and use
JP2710632B2 (en) Method for producing optically active secondary amine
JPH11189600A (en) Ruthenium complex and method for producing alcohol compound using the same as catalyst
EP1305278B1 (en) Ruthenium complexes and their use in asymmetric hydrogenation
HU221381B1 (en) Heteroaromatic chiral diphosphines, their complexes with transition metals, preparation and use thereof
EP1276745B1 (en) Ruthenium-diphosphine complexes and their use as catalysts
JP2007536338A (en) Ruthenium complex with 2- (aminomethyl) pyridine and phosphine, process for its preparation and use as catalyst
CN106831550A (en) A kind of optical activity two(It is miscellaneous)Aryl methyl alcohol and its method of asymmetric synthesis
EP1323724B1 (en) Ruthenium complexes and process for preparing alcoholic compounds using these
CN103889995A (en) New metal ruthenium complex having nitrogen ligand, preparation method therefor, and uses thereof
US6979742B1 (en) Process for obtaining enantiomers of thienylazolylalcoxyethanamines
KR101579992B1 (en) Trisubstituted 3,4-dihydro-1h-isoquinolin compound, process for its preparation, and its use
WO2006069766A1 (en) Process for obtaining enantiomers of cizolirtine
US20060142589A1 (en) Process for obtaining enantiomers of Cizolirtine
WO2006069767A1 (en) Process for obtaining enantiomers of thienylazolylalcoxyethanamines
EP3016961B1 (en) Novel ruthenium catalysts and their use for asymmetric reduction of ketones
ES2303796B1 (en) PROCEDURE TO OBTAIN CIZOLIRTINE ENANTIOMERS.
JP4519913B2 (en) Process for the preparation of asymmetrically substituted biaryldiphosphines
US7109349B2 (en) Process for obtaining Cizolirtine and its enantiomers
JP2015024975A (en) Production method of optically active secondary alcohol
EP1792887A1 (en) Process for the homogeneous hydrogenation of ketones using ruthenium catalytic systems
ES2303795B1 (en) PROCEDURE TO OBTAIN TIENILAZOLILALCOXIETANAMIN ENANTIOMERS.
EP1757571A1 (en) Process for the homogeneous hydrogenation of ketones using ruthenium catalytic systems.
JP2012031119A (en) Axially chiral isoquinoline derivative, its production method, and asymmetric synthesis method
JP4751579B2 (en) Process for producing optically active tetrahydroisoquinolines

Legal Events

Date Code Title Description
121 Ep: the epo has been informed by wipo that ep was designated in this application
DPE1 Request for preliminary examination filed after expiration of 19th month from priority date (pct application filed from 20040101)
ENP Entry into the national phase

Ref document number: 200750039

Country of ref document: ES

Kind code of ref document: A

WWE Wipo information: entry into national phase

Ref document number: P200750039

Country of ref document: ES

NENP Non-entry into the national phase

Ref country code: DE

122 Ep: pct application non-entry in european phase

Ref document number: 05843397

Country of ref document: EP

Kind code of ref document: A1

WWW Wipo information: withdrawn in national office

Ref document number: 5843397

Country of ref document: EP

WWP Wipo information: published in national office

Ref document number: 200750039

Country of ref document: ES

Kind code of ref document: A

WWG Wipo information: grant in national office

Ref document number: 200750039

Country of ref document: ES

Kind code of ref document: A