US20120022102A1 - Method for preparation of pitavastatin and its pharmaceutical acceptable salts thereof - Google Patents

Method for preparation of pitavastatin and its pharmaceutical acceptable salts thereof Download PDF

Info

Publication number
US20120022102A1
US20120022102A1 US13/009,492 US201113009492A US2012022102A1 US 20120022102 A1 US20120022102 A1 US 20120022102A1 US 201113009492 A US201113009492 A US 201113009492A US 2012022102 A1 US2012022102 A1 US 2012022102A1
Authority
US
United States
Prior art keywords
compound
formula
zinc
pitavastatinmagnesium
solvent
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.)
Abandoned
Application number
US13/009,492
Inventor
Shriprakash Dhar Dwivedi
Dhimant Jasubhai Patel
Alpesh Pravinchandra SHAH
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.)
Zydus Lifesciences Ltd
Original Assignee
Cadila Healthcare Ltd
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
Application filed by Cadila Healthcare Ltd filed Critical Cadila Healthcare Ltd
Assigned to CADILA HEALTHCARE LIMITED reassignment CADILA HEALTHCARE LIMITED ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: DWIVEDI, Shriprakash Dhar, PATEL, DHIMANT JASUBHAI, SHAH, ALPESH PRAVINCHANDRA
Publication of US20120022102A1 publication Critical patent/US20120022102A1/en
Priority to US13/665,932 priority Critical patent/US8829186B2/en
Priority to US14/479,575 priority patent/US9139527B2/en
Abandoned legal-status Critical Current

Links

Images

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D215/00Heterocyclic compounds containing quinoline or hydrogenated quinoline ring systems
    • C07D215/02Heterocyclic compounds containing quinoline or hydrogenated quinoline ring systems having no bond between the ring nitrogen atom and a non-ring member or having only hydrogen atoms or carbon atoms directly attached to the ring nitrogen atom
    • C07D215/12Heterocyclic compounds containing quinoline or hydrogenated quinoline ring systems having no bond between the ring nitrogen atom and a non-ring member or having only hydrogen atoms or carbon atoms directly attached to the ring nitrogen atom with substituted hydrocarbon radicals attached to ring carbon atoms
    • C07D215/14Radicals substituted by oxygen atoms
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P3/00Drugs for disorders of the metabolism
    • A61P3/06Antihyperlipidemics
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P43/00Drugs for specific purposes, not provided for in groups A61P1/00-A61P41/00

Definitions

  • the present invention relates to processes for the preparation of pitavastatin and pharmaceutically acceptable salts thereof.
  • the present invention provides processes for the preparation of pitavastatinalkali or alkaline earth metal salts in crystalline and amorphous forms.
  • Pitavastatin is a synthetic lipid-lowering agent that acts as an inhibitor of 3-hydroxy-3-methylglutaryl-coenzyme a (HMG-CoA) reductase (HMG-CoA Reductase inhibitor). This enzyme catalyzes the conversions of HMG-CoA to mevalonate, inhibitors are commonly referred to as “statins”.
  • Statins are therapeutically effective drugs used for reducing low density lipoprotein (LDL) particle concentration in the blood stream of patients at risk for cardiovascular disease.
  • LDL low density lipoprotein
  • Pitavastatin is used in the treatment of hyperchloesterolemia and mixed dyslipidemia.
  • US20090182008 A1 discloses polymorphic form A, B, C, D, E, and F, and the amorphous form of Pitavastatin Calcium salt (2:1).
  • crystalline Form A having water content from about. 5% to about 15% and process for its preparation are disclosed.
  • US20090176987 A1 also discloses polymorphic form crystal form A of Pitavastatin Calcium which contains from 5 to 15% of water and which shows, in its X-ray powder diffraction as measured by using CuKa radiation, a peak having a relative intensity of more than 25% at a diffraction angle (20) of 30.16°.
  • WO2007/132482 A1 discloses a novel process for the preparation of Pitavastatin Calcium by condensing bromide salt of formula-3 with aldehyde compound of formula-4 to obtain olefinic compound of formula-5 and converting olefinic compound to Pitavastatin Calcium via organic amine salt for purification.
  • alkali or alkaline earth salt of quinoline derivatives such as pitavastatin, a HMG-CoA inhibitors
  • the present invention provides a novel process for the preparation of pitavastatinmagnesium it is crystalline and amorphous form.
  • pitavastatin in one embodiment, there is provided a novel process for the preparation of pitavastatin and its pharmaceutically acceptable salts.
  • pitavastatinalkali or alkaline earth metal comprises one or more of magnesium, zinc, potassium, strontium, barium and the like.
  • Pitavastatin which is chemically known as (3R,5S)-7-[2-cyclopropyl-4-(4-fluorophenyl)quinolin-3-yl]-3,5-dihydroxy-6(E)-heptenoic acid and its pharmaceutically acceptable salts having the general formula I
  • M is K + , Mg +2 , Sr +2 , Zn +2 , Ba +2 .
  • pitavastatin and its pharmaceutically acceptable salts particularlypitavastatinmagnesium which is chemically known as (3R,5S)-7-[2-cyclopropyl-4-(4-fluorophenyl)quinolin-3-yl]-3,5-dihydroxy-6(E)-heptenoic acid Magnesium salt having the formula IB.
  • pitavastatinmagnesium it its crystalline form having X-ray powder diffraction peaks at 10.1, 13.2, 19.3 and 27.2 ⁇ 0.2 (2 ⁇ ).
  • the process for the preparation of pitavastatinmagnesium according to the present inventions provides crystalline form of pitavastatinmagnesium having water content in the range of from about 7% to about 12% wt/wt.
  • the process comprising: (a) providing pitavastatinmagnesium in crystalline form having water content in the range of about 8% to about 12% wt/wt; (b) contacting the pitavastatinmagnesium with humid air in a fluidized bed drier, or maintaining the pitavastatinmagnesium at a temperature of from about 5 to about 60° C., under pressure of less than 30 mm/Hg for a period of from about 1 to 5 days; and (c) recoveringthe pitavastatinmagnesium in the amorphous form having water content less than about 2% wt/wt.
  • substantially pure pitavastatinmagnesium in stable crystalline form there is provided substantially pure pitavastatinmagnesium in stable crystalline form.
  • FIG. 1 X-ray diffraction pattern of crystalline pitavastatinmagnesium having about 8% to about 12% water content prepared as per the process of Example-2
  • FIG. 2 X-ray diffraction pattern of amorphous pitavastatin magnesium prepared as per the process of Example-3
  • FIG. 3 X-ray diffraction pattern of crystalline (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)-quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound (II).
  • FIG. 4 DSC thermogram of crystalline (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)-quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound (II) having endothermic peak at about 116.04° C.
  • the prior art discloses the use of organic amine salts of Pitavastatin for obtaining better purity.
  • the present inventors have found that pitavastatinalkali or alkaline earth metal salt prepared by using the process provided herein provides better yield and purity and avoids the use of amine salt formation. This significantly improves the process economics and commercial viability.
  • isolation may include filtration, filtration under vacuum, centrifugation, and decantation.
  • the product obtained may be further or additionally dried to achieve the desired moisture values.
  • the product may be dried in a tray drier, dried under vacuum and/or in a Fluid Bed Drier.
  • the solution prior to any solids formation, can be filtered to remove any undissolved solids, solid impurities and the like prior to removal of the solvent.
  • Any filtration system and filtration techniques known in the art can be used.
  • Suitable organic solvent means a single or a combination of two or more solvents.
  • Substantially pure means pitavastatinalkali or alkaline earth metal prepared by the process of the present invention is substantially free from any single individual impurities like desfluoro impurity, cis-isomer impurity, Pitavastatin 5-oxo impurity, pitavastatinlactone impurity, pitavastatin t-butyl diol ester impurity, and pitavastatincondensed impurity.
  • substantially pure means pitavastatinalkali or alkaline earth having purity greater than 99%. In particular, it may be greater than 99.5% by area percentage of HPLC. In particular, containing less than about 0.1% of single individual impurity as herein described above and total impurities not more than 1.0% by area percentage of HPLC.
  • pitavastatindiastereomeric impurity and pitavastatinenantiomeric impurity are present less than about 0.3% by area percentage of HPLC.
  • pitavastatinalkali or alkaline earth metal salts includes the following which were determined from an HPLC analysis of different batches of pitavastatinalkali or alkaline earth metal salts produced by the method described in the specification herein after:
  • alkali or alkaline earth metal salts of pitavastatin wherein the alkali or alkaline earth metal comprises one or more of magnesium, zinc, potassium, strontium, barium and the like. In particular, it may comprises one or more of magnesium, zinc and potassium.
  • the pitavastatin magnesium may be a hydrate having water content in the range of from about 7% to about 12% wt/wt.
  • the water content may be about 9% to about 12% wt/wt. More particularly, the water content may be about 10% to about 12% wt/wt as measured by the known techniques in the art like Karl-Fisher method.
  • pitavastatin magnesium in crystalline form having x-ray powder diffraction peaks at 10.1, 13.2, 19.3 and 27.2 ⁇ 0.2 (2 ⁇ ).
  • the pitavastatin magnesium crystalline form is having an x-ray powder diffraction pattern as shown in FIG. 1 .
  • Further embodiment includes pitavastatin magnesium having optical rotation of about +22.0 to +22.5 in 1% DMSO at 20 ⁇ 0.5° C.
  • an amorphous form of the pitavastatin magnesium having x-ray powder diffraction peaks as shown in FIG. 2 .
  • the amorphous form of pitavastatin magnesium is having the water content less than about 5% wt/wt. In particular, it may have the water content less than about 2% wt/wt.
  • pitavastatin alkali or alkaline earth metal comprises one or more of magnesium, potassium, zinc and the like.
  • the pitavastatinalkali metal salts is chemically known as (3R,5S)-7-[2-cyclopropyl-4-(4-fluorophenyl)quinolin-3-yl]-3,5-dihydroxy-6(E)-heptenoic acid salt having the general Formula (I)
  • M is Na + , K + , Li + .
  • step (b) hydrolyzing the compound of Formula-II under the acidic conditions to remove acetonide protection to form diol compound; (c) treating the diol compound of step (b) in-situ with an alkali metal hydroxide to form the corresponding alkali metal salt of Pitavastatin (I);
  • M is Na + , K + , Li + ; (d) treating the alkali metal salt of pitavastatin (I) with a magnesium source to obtain pitavastatinmagnesium; and (e) isolating the pitavastatin magnesium.
  • the phosphonium bromide compound of Formula-IV and aldehyde compound of Formula-III can be reacted in the presence of alkali or alkaline earth metal bases.
  • the alkali or alkaline earth metal bases comprises one or more of sodium hydroxide, potassium hydroxide, lithium hydroxide, potassium carbonate, sodium carbonate, lithium carbonate, cesium carbonate and the like. In particular, it may be potassium carbonate.
  • Embodiments includes that the reaction may be performed in a suitable polar aprotic solvent comprises one or more dimethylformamide, dimethylsulfoxide, dimethylacetamide, tetrahydrofuran, N-methylpyrrolidone or mixtures thereof. In particular, it may be dimethylsulfoxide.
  • the reaction may be performed at an ambient temperature i.e. at about 15° C. to about 40° C. In particular, it may be from about 20° C. to about 35° C.
  • the reaction mixture may be stirred for about 5 to 15 hours till completion of the reaction, in particular for 10 hours.
  • the reaction mixture may be further treated with suitable organic solvents like toluene, xylene, methylene dichloride, ethyl acetate for extracting the compound of Formula-II.
  • suitable organic solvents like toluene, xylene, methylene dichloride, ethyl acetate for extracting the compound of Formula-II.
  • the compound of Formula-II is extracted by using toluene.
  • the compound of Formula-II may be isolated by removal of toluene followed by addition of isopropanol. After the addition of isopropanol, the reaction mixture can be heated to 40° C. to 80° C., preferably 60° C. to 70° C. and cooling to 15° C. to obtain olefin compound of Formula (II).
  • the compound of Formula (II) may optionally be purified in suitable polar solvent like methanol, ethanol, Isopropanol, acetone, DMF, ethyl acetate, butyl acetate and the like. In particular, the compound of Formula (II) may be purified using methanol.
  • hydrolysis of compound of Formula (II) includes, hydrolysis of compound of Formula (II).
  • the hydrolysis of olefin compound is done under the acidic conditions to remove the acetonideprotection and to form diol compound.
  • the suitable acids comprise one or more of hydrochloric acid, acetic acid, sulfuric acid, nitric acid, phosphoric acid and the like. In particular it may be hydrochloric acid.
  • the diol compound obtained is in-situ treated with an alkali metal hydroxide selected from sodium hydroxide, potassium hydroxide, lithium hydroxide and the like.
  • M is Na + .
  • Embodiments of the process includes treating alkali metal salt of formula (I) of pitavastatin, in particular it may be pitavastatinsodium with magnesium source.
  • Preferred magnesium source comprises one or more of magnesium chloride, magnesium methoxide, magnesium acetate and hydrates thereof. In particular, it may be magnesium chloride hexahydrate.
  • the pitavastatinmagnesium prepared by the method as described above can be dried in hot air oven at 40° C. to 45° C. for at least about 4 to 24 hours having water content in the range of about 8% to 12% wt/wt to obtain pitavastatinmagnesium in crystalline form.
  • Embodiments further includes, drying pitavastatin magnesium having water content in the range of about 8% to about 12% wt/wt for about 8 hours or more; in particular, for at least about 24 hours so as obtain substantially anhydrous pitavastatin magnesium having water content less than about 2% wt/wt.
  • the phosphonium bromide compound of Formula-IV and aldehyde compound of Formula-III can be reacted in the presence of alkali or alkaline earth metal base.
  • the alkali or alkaline earth metal base comprises one or more of sodium hydroxide, potassium hydroxide, lithium hydroxide, potassium carbonate, sodium carbonate, lithium carbonate, cesium carbonate and the like. In particular, it may be potassium carbonate.
  • Embodiments includes that the reaction can be performed in one or more of suitable polar aprotic solvent selected from dimethylformamide, dimethylsulfoxide, dimethylacetamide, tetrahydrofuran, N-methylpyrrolidone or mixtures thereof.
  • suitable polar aprotic solvent selected from dimethylformamide, dimethylsulfoxide, dimethylacetamide, tetrahydrofuran, N-methylpyrrolidone or mixtures thereof.
  • suitable polar aprotic solvent selected from dimethylformamide, dimethylsulfoxide, dimethylacetamide, tetrahydrofuran, N-methylpyrrolidone or mixtures thereof.
  • suitable polar aprotic solvent selected from dimethylformamide, dimethylsulfoxide, dimethylacetamide, tetrahydrofuran, N-methylpyrrolidone or mixtures thereof.
  • it may bedimethylsulfoxide at an ambient temperature i.e. at about 15° C. to about 40° C.
  • the reaction mixture can be stirred for about 5 to 15 hours till completion of the reaction. In particular, it may be for 10 hours.
  • the reaction mixture can be further treated with suitable organic solvents like toluene, xylene, methylene dichloride, ethyl acetate for extracting compound of Formula-II.
  • suitable organic solvents like toluene, xylene, methylene dichloride, ethyl acetate for extracting compound of Formula-II.
  • the compound of Formula (II) may be extracted with toluene.
  • the compound of Formula-II can be isolated by removal of toluene followed by addition of isopropanol. After the addition of isopropanol, the reaction mixture can be heated to 40° C. to 80° C., particularly at about 60° C. to 70° C. and cooling to 15° C. to obtain compound of formula (II).
  • the compound of formula (II) can be purified in suitable polar solvent like methanol, ethanol, Isopropanol, acetone, DMF, ethyl acetate, butyl acetate and the like. In particular, it may be methanol.
  • the term “elevated temperature” includes heating the compound II in a polar solvent at about 50° C. to about 100° C.
  • the compound II may be heated at about 50° C. to about 70° C., most particularly, at about 60° C. to 65° C.
  • the term “ambient temperature” includes cooling the reaction mixture comprising the compound II in a polar solvent at about 0° C. to about 30° C. In particular, it may be at about 0° C. to about 15° C., most particularly, at about 0° C. to 10° C.
  • the compound (II) i.e. (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester is obtain in crystalline form after purification in polar solvent.
  • the crystalline form of compound (II) is characterized by an X-ray powder diffraction pattern having characteristics peaks expressed in degrees 2 ⁇ ( ⁇ 0.2° 2 ⁇ ) at 7.86°, 9.94°, 11.48°, 12.71°, 14.80°, 15.88°, 17.44°, 18.16°, 19.17°, 19.97°, 20.77°, 22.71°, 23.41°, 24.68°, 26.02°, 27.63° and 29.36° ⁇ 0.2°.
  • the X-ray powder diffraction pattern is characterized substantially the same that shown in FIG. 3 .
  • the crystalline form of compound (II) is characterized by an IR spectrum having peaks at about 2999, 2976, 1720, 1600, 1512, 1487, 1379, 1342, 1288, 1197, 1134, 1066, 1035, 931 and 842 cm ⁇ 1 and DSC endotherm at about 116.04° C.
  • the DSC thermogram is substantially the same that shown in FIG. 4 .
  • the preferable zinc source comprises one or more of zinc formate, zinc acetate, zinc propionate, zinc maleate, zinc fumarate, zinc tartrate, zinc lactate, zinc malate, zinc citrate, Zinc ascorbate, zinc malonate, zinc oxalate, zinc glycolate, zinc methanesulfonate, zinc ethanesulfonate, a salt of zinc with amino acid, zinc sulfate, zinc chloride, zinc carbonate or zinc nitrate.
  • it comprises one or more of zinc sulfate, zinc chloride or zinc acetate.
  • the process comprising: (a) reacting phosphonium bromide compound of Formula-IV with an aldehyde compound of Formula-III in the presence of an alkali or alkaline earth metal bases in one or more suitable polar aprotic solvent to provide (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of Formula-II, (b) hydrolyzing the compound of Formula-II by subjecting under the acidic conditions to remove the acetonideprotection to form diol compound; (c) treating the diol compound of step (b) in-situwith a potassium source to obtain pitavastatinpotassium.
  • the preferable potassium source comprises one or more of potassium hydroxide, potassium carbonate, potassium bicarbonate, potassium acetate, potassium chloride and the like.
  • the amorphous form can be generally prepared by addition of anti-solvent to a concentrated solution of pitavastatinmagnesium in an organic solvent.
  • Embodiments of the process includes preparing the solution of pitavastatinmagnesium in suitable organic solvent selected from the group consisting of a chlorinated solvent, alcoholic solvent, ketonic solvent, ester solvents and mixtures thereof.
  • suitable organic solvent selected from the group consisting of a chlorinated solvent, alcoholic solvent, ketonic solvent, ester solvents and mixtures thereof.
  • the preferred solvent comprises one or more of methylene dichloride, ethylene dichloride, chlorobenzene, methanol, ethanol, isopropanol, butanol, acetone, methylethyl ketone, ethyl acetate, butyl acetate, isopropyl acetate, and mixtures thereof or mixture thereof with water.
  • the suitable solvent comprises one or more of methanol, acetone, ethyl acetate.
  • the embodiment of the process includes adding suitable antisolvent to the solution of pitavastatinmagnesium in suitable organic solvent.
  • the suitable anti-solvent comprises one or more of hexane, heptane, cyclohexane, toluene, xylene, diisopropyl ether, methyl tert-butyl ether, 1,4-dioxane, tetrahydrofuranand the like.
  • the suitable anti-solvent comprises one or more of heptane or cyclohexane or methyl tert-butyl ether.
  • the suitable solvents and anti-solvents comprises from the same as listed herein above.
  • the reaction mixture can be heated to an elevated temperature in step (b).
  • the elevated temperature is from about 50° C. to about 100° C. In particularly, it may be from about 70° C. to about 90° C.
  • the reaction mixture is then cooled to an ambient temperature, preferably from about 15° C. to about 35° C., preferably from about 25° C. to 35° C.
  • the anti-solvent and solvent are miscible.
  • the amorphous form can also be prepared by lyophilization of or removal of solvent from the solution of pitavastatinmagnesium in a suitable solvent.
  • amorphous form of pitavastatinmagnesium having water content less than about 2% wt/wt is prepared by contacting pitavastatinmagnesium containing about 8% to about 12% of water content with humid air in a fluidized bed apparatus.
  • the temperature is of about 25° C. to about 50° C., more particularly at about 30° C. to about 40° C.
  • the contacting may be carried out, in particularly at about 6 hours to 2 days.
  • the term “humid” refers to a relative humidity of at least 30%. In particular, it may be at least about 50% and most particularly at least about 70%.
  • substantially pure pitavastatinmagnesium in stable crystalline form there is provided substantially pure pitavastatinmagnesium in stable crystalline form.
  • a pharmaceutical composition comprising a therapeutically effective amount of crystalline pitavastatinmagnesium characterized by X-ray diffraction pattern having characteristic peaks at 2-theta values 10.1°, 13.2°, 19.3° and 27.2° ⁇ 0.2°, and one or more pharmaceutically acceptable carriers, excipients or diluents.
  • a pharmaceutical composition comprising a therapeutically effective amount of amorphouspitavastatinmagnesium characterized by x-ray diffraction pattern substantially as depicted in FIG. 2 , and one or more pharmaceutically acceptable carriers, excipients or diluents.
  • the starting material, phosphonium bromide compound of Formula-IV, can be prepared from alcoholic compound of formula (VI)
  • the alcoholic compound of formula (VI) is converted o phosphonium compound of Formula (IV) via formation of 3-(bromomethyl)-2-cyclopropyl-4(4′-fluorophenyl)quinoline of Formula (V) by the known process reported in the prior art.
  • bromo compound of formula (V) 3-(bromomethyl)-2-cyclopropyl-4-(4′-fluorophenyl)quinoline with wittig reagent like triphenyl phosphine in suitable non-polar solvents like toluene, o-xylene, chlorobenzeneetc to obtain phosphonium bromide compound of formula (IV).
  • the starting reagent, alcohol compound of formula (VI) can be prepared from the known process reported in the art like Tetrahedron Letters , Vol. 34, No. 51, p.p. 8271-8274 (1993); Heterocycles , Vol. 50, No. 1, 1999 ; Drugs of Future 1998 23 (8) or Tetrahedron Asymmetry 1993, Vol. 4, pp. 201-204 are reported herein as reference in its entirety.
  • the pitavastatin magnesium can be prepared by as shown bellow:
  • the reaction mixture was stirred for 4 hours at 25° C. and quenched in water.
  • the reaction mass was treated with 92 mL 1 N HCl solution to adjust the pH of about 8.0 and treated with methylene dichloride for washing.
  • the separated aqueous layer is treated with 100 g of magnesium chloride hexahydrate and stirred for 30 min at 25° C.
  • the solution is cooled to 15° C., filtered and washed with water.
  • the product is dried in hot air oven for 4 hours to obtain 82 g of crystalline Pitavastatin Magnesium having water content of 11.0%. (XRD as shown in FIG. 1 )
  • the reaction mass was treated with 92 mL 1 N HCl solution to adjust the pH of about 8.0 and treated with methylene dichloride for washing.
  • the separated aqueous layer is treated with 100 g of zinc sulfate and stirred for 30 min at 25° C.
  • the solution is cooled to 15° C., filtered and washed with water.
  • the product is dried in hot air oven for 4 hours to obtain 75 g of crystalline Pitavastatin zinc.
  • the reaction mass was treated with 92 mL 1 N HCl solution to adjust the pH of about 8.0 and treated with methylene dichloride for washing.
  • the separated aqueous layer is treated with 80 g of Potassium hydroxide and stirred for 30 min at 25° C.
  • the solution is cooled to 15° C., filtered and washed with water.
  • the product is dried in hot air oven for 4 hours to obtain 72 g of crystalline Pitavastatin Potassium.
  • the present invention provides novel pharmaceutically acceptable salt of alkali metal salts of Pitavastatin. 2.
  • the present invention provides an improved process for the preparation of pitavastatinalkali metal salts.
  • the present invention provides crystalline form of pitavastatinmagnesium having 8% to 12% water content.
  • the present invention also provides amorphous form of pitavastatinmagnesium and process for preparation thereof.
  • the present invention provides amorphous form of pitavastatinmagnesium containing less than about 2% of water content. 6.
  • the process provided is eco-friendly, economically viable and easily scalable on large scale production.

Landscapes

  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Health & Medical Sciences (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • General Health & Medical Sciences (AREA)
  • General Chemical & Material Sciences (AREA)
  • Medicinal Chemistry (AREA)
  • Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
  • Bioinformatics & Cheminformatics (AREA)
  • Pharmacology & Pharmacy (AREA)
  • Engineering & Computer Science (AREA)
  • Animal Behavior & Ethology (AREA)
  • Chemical Kinetics & Catalysis (AREA)
  • Public Health (AREA)
  • Veterinary Medicine (AREA)
  • Diabetes (AREA)
  • Hematology (AREA)
  • Obesity (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Quinoline Compounds (AREA)
  • Plural Heterocyclic Compounds (AREA)
  • Organic Low-Molecular-Weight Compounds And Preparation Thereof (AREA)

Abstract

The present invention discloses a compound, which is alkali or alkaline earth metal salts of pitavastatin, wherein the alkali or earth metal comprise one or more of magnesium, zinc, potassium, strontium and barium.

Description

    FIELD OF THE INVENTION
  • The present invention relates to processes for the preparation of pitavastatin and pharmaceutically acceptable salts thereof. In particular, the present invention provides processes for the preparation of pitavastatinalkali or alkaline earth metal salts in crystalline and amorphous forms.
    • BACKGROUND OF THE INVENTION
  • Pitavastatin calcium is chemically known as (3R,5S)-7-[2-cyclopropyl-4-(4-fluorophenyl)quinolin-3-yl]-3,5-dihydroxy-6(E)-heptenoic acid calcium salt having the formula IA is known in the literature.
  • Figure US20120022102A1-20120126-C00001
  • Pitavastatin is a synthetic lipid-lowering agent that acts as an inhibitor of 3-hydroxy-3-methylglutaryl-coenzyme a (HMG-CoA) reductase (HMG-CoA Reductase inhibitor). This enzyme catalyzes the conversions of HMG-CoA to mevalonate, inhibitors are commonly referred to as “statins”. Statins are therapeutically effective drugs used for reducing low density lipoprotein (LDL) particle concentration in the blood stream of patients at risk for cardiovascular disease. Pitavastatin is used in the treatment of hyperchloesterolemia and mixed dyslipidemia.
  • Pitavastatin calcium has recently been developed as a new chemically synthesized and powerful statin by Kowa Company Ltd, Japan. On the basis of reported data, the potency of Pitavastatin is dose-dependent and appears to be equivalent to that of Atorvastatin. This new statin is safe and well tolerated in the treatment of patients with hypercholesterolaemia. Significant interactions with a number of other commonly used drugs can be considered to be extremely low.
  • Processes for the preparation of Pitavastatin are described in EP-A-0304063 and EP-A-1099694 and in the publications by N. Miyachi et al. in Tetrahedron Letters (1993) vol. 34, pages 8267-8270 and by K. Takahashi et al. in Bull. Chem. Soc. Japan (1995) Vol. 68, 2649-2656. These publications describe the synthesis of Pitavastatin in great detail but do not describe the hemi-calcium salt of Pitavastatin. The publications by L A. Sorbera et al. in Drugs of the Future (1998) vol. 23, pages 847-859 and by M. Suzuki at al. in Bioorganic & Medicinal Chemistry Letters (1999) vol. 9, pages 2977-2982 describe Pitavastatin calcium, however, a precise procedure for its preparation is not given. A full synthetic procedure for the preparation of Pitavastatin calcium is described in EP-A-0520406. In the process described in this patent Pitavastatin calcium is obtained by precipitation from an aqueous solution as a white crystalline material with a melting point of 190-192° C.
  • US20090182008 A1 discloses polymorphic form A, B, C, D, E, and F, and the amorphous form of Pitavastatin Calcium salt (2:1). In particular, crystalline Form A having water content from about. 5% to about 15% and process for its preparation are disclosed.
  • US20090176987 A1 also discloses polymorphic form crystal form A of Pitavastatin Calcium which contains from 5 to 15% of water and which shows, in its X-ray powder diffraction as measured by using CuKa radiation, a peak having a relative intensity of more than 25% at a diffraction angle (20) of 30.16°.
  • WO2007/132482 A1 discloses a novel process for the preparation of Pitavastatin Calcium by condensing bromide salt of formula-3 with aldehyde compound of formula-4 to obtain olefinic compound of formula-5 and converting olefinic compound to Pitavastatin Calcium via organic amine salt for purification.
  • There are no reports available in the prior art for the preparation of Pitavastatin Magnesium. Thus, the inventors of the present inventions provide a novel pharmaceutically acceptable salt of Pitavastatin, preferably magnesium salt.
    • SUMMARY OF THE INVENTION
  • In accordance with the present invention, there is provided alkali or alkaline earth salt of quinoline derivatives such as pitavastatin, a HMG-CoA inhibitors, more specially, the present invention provides a novel process for the preparation of pitavastatinmagnesium it is crystalline and amorphous form.
  • In one embodiment, there is provided a novel process for the preparation of pitavastatin and its pharmaceutically acceptable salts. In particular, pitavastatinalkali or alkaline earth metalcomprises one or more of magnesium, zinc, potassium, strontium, barium and the like. Pitavastatin, which is chemically known as (3R,5S)-7-[2-cyclopropyl-4-(4-fluorophenyl)quinolin-3-yl]-3,5-dihydroxy-6(E)-heptenoic acid and its pharmaceutically acceptable salts having the general formula I
  • Figure US20120022102A1-20120126-C00002
  • wherein, M is K+, Mg+2, Sr+2, Zn+2, Ba+2.
  • In one preferred embodiment, there is provided a novel process for the preparation of pitavastatin and its pharmaceutically acceptable salts, particularlypitavastatinmagnesium which is chemically known as (3R,5S)-7-[2-cyclopropyl-4-(4-fluorophenyl)quinolin-3-yl]-3,5-dihydroxy-6(E)-heptenoic acid Magnesium salt having the formula IB.
  • In second embodiment, there is provided a novel salt, pitavastatinmagnesium of Formula (IB)
  • Figure US20120022102A1-20120126-C00003
  • In yet another embodiment, there is provided pitavastatinmagnesium it its crystalline form having X-ray powder diffraction peaks at 10.1, 13.2, 19.3 and 27.2±0.2 (2θ).
  • In further embodiment, there is provided a process for the preparation of pitavastatinmagnesium of formula (1B), the process comprising:
  • (a) reacting phosphonium bromide compound of Formula-IV with an aldehyde compound of Formula-III in the presence of an alkali or alkaline earth metal base in one or more suitable polar aprotic solvent to provide (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of formula-II;
    (b) hydrolyzing the compound of Formula-II under the acidic conditions to remove the acetonideprotection to form a diol compound;
    (c) treating the diol compound of step (b) in-situ with an alkali metal hydroxide to form the corresponding alkali metal salt of pitavastatin (I);
    (d) treating alkali metal salt of pitavastatin with a magnesium source to obtain pitavastatinmagnesium; and
    (e) isolating the pitavastatinmagnesium.
  • According to the embodiments, the process for the preparation of pitavastatinmagnesium according to the present inventions provides crystalline form of pitavastatinmagnesium having water content in the range of from about 7% to about 12% wt/wt.
  • According to another embodiment, the compound (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester of formula (II) in crystalline form.
  • According to another embodiment, there is provided an improved process for the purification of (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester of formula (II) to obtain in crystalline form.
  • According to the further embodiments, there is provided a process for the preparation of pitavastatinmagnesium in amorphous form, the process comprising:
  • (a) providing a solution comprising pitavastatinmagnesium in a suitable organic solvent wherein the organic solvent is one or more of a chlorinated solvent, alcoholic solvent, ketonic solvent, aliphatic or cyclic ether and mixtures thereof;
    (b) adding suitable antisolvent to the solution; and
    (c) recovering the amorphous form of the pitavastatinmagnesium.
  • According to the further embodiments, there is provided a process for the preparation of an amorphous form of the pitavastatinmagnesium having water content less than about 2% wt/wt,
  • the process comprising:
    (a) providing pitavastatinmagnesium in crystalline form having water content in the range of about 8% to about 12% wt/wt;
    (b) contacting the pitavastatinmagnesium with humid air in a fluidized bed drier, or maintaining the pitavastatinmagnesium at a temperature of from about 5 to about 60° C., under pressure of less than 30 mm/Hg for a period of from about 1 to 5 days; and
    (c) recoveringthe pitavastatinmagnesium in the amorphous form having water content less than about 2% wt/wt.
  • According to the further embodiment, there is provided substantially pure pitavastatinmagnesium in stable crystalline form.
    • DETAILED DESCRIPTION OF DRAWINGS
  • FIG. 1: X-ray diffraction pattern of crystalline pitavastatinmagnesium having about 8% to about 12% water content prepared as per the process of Example-2
  • FIG. 2: X-ray diffraction pattern of amorphous pitavastatin magnesium prepared as per the process of Example-3
  • FIG. 3: X-ray diffraction pattern of crystalline (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)-quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound (II).
  • FIG. 4. DSC thermogram of crystalline (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)-quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound (II) having endothermic peak at about 116.04° C.
    •
  • The details of one or more embodiments of the inventions are set forth in the description below.
  • Other features, objects and advantages of the inventions will be apparent from the description and claims.
    • DETAILED DESCRIPTION OF THE INVENTION
  • The prior art discloses the use of organic amine salts of Pitavastatin for obtaining better purity. The present inventors have found that pitavastatinalkali or alkaline earth metal salt prepared by using the process provided herein provides better yield and purity and avoids the use of amine salt formation. This significantly improves the process economics and commercial viability.
  • As used here in the term “isolation” may include filtration, filtration under vacuum, centrifugation, and decantation. The product obtained may be further or additionally dried to achieve the desired moisture values. For example, the product may be dried in a tray drier, dried under vacuum and/or in a Fluid Bed Drier.
  • Optionally, the solution, prior to any solids formation, can be filtered to remove any undissolved solids, solid impurities and the like prior to removal of the solvent. Any filtration system and filtration techniques known in the art can be used.
  • The term “Suitable organic solvent” means a single or a combination of two or more solvents.
  • The term “Substantially pure” means pitavastatinalkali or alkaline earth metal prepared by the process of the present invention is substantially free from any single individual impurities like desfluoro impurity, cis-isomer impurity, Pitavastatin 5-oxo impurity, pitavastatinlactone impurity, pitavastatin t-butyl diol ester impurity, and pitavastatincondensed impurity.
  • Further the term “substantially pure” means pitavastatinalkali or alkaline earth having purity greater than 99%. In particular, it may be greater than 99.5% by area percentage of HPLC. In particular, containing less than about 0.1% of single individual impurity as herein described above and total impurities not more than 1.0% by area percentage of HPLC.
  • Particularly, pitavastatindiastereomeric impurity and pitavastatinenantiomeric impurity are present less than about 0.3% by area percentage of HPLC.
  • The above impurities are present in the preparation of pitavastatinalkali or alkaline earth metal salts includes the following which were determined from an HPLC analysis of different batches of pitavastatinalkali or alkaline earth metal salts produced by the method described in the specification herein after:
  • Figure US20120022102A1-20120126-C00004
    Figure US20120022102A1-20120126-C00005
  • In first embodiment, there is provided alkali or alkaline earth metal salts of pitavastatin, wherein the alkali or alkaline earth metal comprises one or more of magnesium, zinc, potassium, strontium, barium and the like. In particular, it may comprises one or more of magnesium, zinc and potassium.
  • In second embodiment of the present invention, there is provided a novel salt pitavastatin magnesium of Formula (IB)
  • Figure US20120022102A1-20120126-C00006
  • In particular, the pitavastatin magnesium may be a hydrate having water content in the range of from about 7% to about 12% wt/wt. In particular, the water content may be about 9% to about 12% wt/wt. More particularly, the water content may be about 10% to about 12% wt/wt as measured by the known techniques in the art like Karl-Fisher method.
  • In yet another embodiment, there is provided pitavastatin magnesium in crystalline form having x-ray powder diffraction peaks at 10.1, 13.2, 19.3 and 27.2±0.2 (2θ). In particular, the pitavastatin magnesium crystalline form is having an x-ray powder diffraction pattern as shown in FIG. 1. Further embodiment includes pitavastatin magnesium having optical rotation of about +22.0 to +22.5 in 1% DMSO at 20±0.5° C.
  • In yet another embodiment, there is provided an amorphous form of the pitavastatin magnesium having x-ray powder diffraction peaks as shown in FIG. 2. According to further embodiment, the amorphous form of pitavastatin magnesium is having the water content less than about 5% wt/wt. In particular, it may have the water content less than about 2% wt/wt.
  • In a third embodiment, there is provided a process for the preparation of pitavastatin and its pharmaceutically acceptable salts, in particular pitavastatin alkali or alkaline earth metal comprises one or more of magnesium, potassium, zinc and the like.
  • The pitavastatinalkali metal salts is chemically known as (3R,5S)-7-[2-cyclopropyl-4-(4-fluorophenyl)quinolin-3-yl]-3,5-dihydroxy-6(E)-heptenoic acid salt having the general Formula (I)
  • Figure US20120022102A1-20120126-C00007
  • wherein, M is Na+, K+, Li+.
  • In a further embodiment of the present invention, there is provided a pitavastatinzinc of Formula (IC)
  • Figure US20120022102A1-20120126-C00008
  • In yet another aspect of the present invention, there is provided a pitavastatinpotassium of formula (ID)
  • Figure US20120022102A1-20120126-C00009
  • According to a further embodiment, there is provided a process for the preparation of pitavastatinmagnesium of formula (IB),
  • Figure US20120022102A1-20120126-C00010
  • the process comprising:
    (a) reacting phosphonium bromide compound of Formula-IV
  • Figure US20120022102A1-20120126-C00011
  • with an aldehyde compound of Formula-III
  • Figure US20120022102A1-20120126-C00012
  • in the presence of an alkali or alkaline earth metal base in one or more suitable polar aprotic solvent to provide (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of formula-II,
  • Figure US20120022102A1-20120126-C00013
  • (b) hydrolyzing the compound of Formula-II under the acidic conditions to remove acetonide protection to form diol compound;
    (c) treating the diol compound of step (b) in-situ with an alkali metal hydroxide to form the corresponding alkali metal salt of Pitavastatin (I);
  • Figure US20120022102A1-20120126-C00014
  • wherein, M is Na+, K+, Li+;
    (d) treating the alkali metal salt of pitavastatin (I) with a magnesium source to obtain pitavastatinmagnesium; and
    (e) isolating the pitavastatin magnesium.
  • The phosphonium bromide compound of Formula-IV and aldehyde compound of Formula-III can be reacted in the presence of alkali or alkaline earth metal bases. The alkali or alkaline earth metal bases comprises one or more of sodium hydroxide, potassium hydroxide, lithium hydroxide, potassium carbonate, sodium carbonate, lithium carbonate, cesium carbonate and the like. In particular, it may be potassium carbonate.
  • Embodiments includes that the reaction may be performed in a suitable polar aprotic solvent comprises one or more dimethylformamide, dimethylsulfoxide, dimethylacetamide, tetrahydrofuran, N-methylpyrrolidone or mixtures thereof. In particular, it may be dimethylsulfoxide. The reaction may be performed at an ambient temperature i.e. at about 15° C. to about 40° C. In particular, it may be from about 20° C. to about 35° C.
  • The reaction mixture may be stirred for about 5 to 15 hours till completion of the reaction, in particular for 10 hours. The reaction mixture may be further treated with suitable organic solvents like toluene, xylene, methylene dichloride, ethyl acetate for extracting the compound of Formula-II. Particularly, the compound of Formula-II is extracted by using toluene.
  • In general, the compound of Formula-II may be isolated by removal of toluene followed by addition of isopropanol. After the addition of isopropanol, the reaction mixture can be heated to 40° C. to 80° C., preferably 60° C. to 70° C. and cooling to 15° C. to obtain olefin compound of Formula (II). The compound of Formula (II) may optionally be purified in suitable polar solvent like methanol, ethanol, Isopropanol, acetone, DMF, ethyl acetate, butyl acetate and the like. In particular, the compound of Formula (II) may be purified using methanol.
  • Further embodiments of the process include, hydrolysis of compound of Formula (II). The hydrolysis of olefin compound is done under the acidic conditions to remove the acetonideprotection and to form diol compound. The suitable acids comprise one or more of hydrochloric acid, acetic acid, sulfuric acid, nitric acid, phosphoric acid and the like. In particular it may be hydrochloric acid.
  • The diol compound obtained is in-situ treated with an alkali metal hydroxide selected from sodium hydroxide, potassium hydroxide, lithium hydroxide and the like.
  • In particular it may be sodium hydroxide to obtain corresponding alkali metal salt of pitavastatin (I)
  • Figure US20120022102A1-20120126-C00015
  • herein M is Na+.
  • Embodiments of the process includes treating alkali metal salt of formula (I) of pitavastatin, in particular it may be pitavastatinsodium with magnesium source. Preferred magnesium source comprises one or more of magnesium chloride, magnesium methoxide, magnesium acetate and hydrates thereof. In particular, it may be magnesium chloride hexahydrate.
  • In general, the pitavastatinmagnesium prepared by the method as described above, can be dried in hot air oven at 40° C. to 45° C. for at least about 4 to 24 hours having water content in the range of about 8% to 12% wt/wt to obtain pitavastatinmagnesium in crystalline form.
  • Embodiments further includes, drying pitavastatin magnesium having water content in the range of about 8% to about 12% wt/wt for about 8 hours or more; in particular, for at least about 24 hours so as obtain substantially anhydrous pitavastatin magnesium having water content less than about 2% wt/wt.
  • According to the preferred embodiment, there is provided an improved process for the preparation of (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester of Formula (II),
  • Figure US20120022102A1-20120126-C00016
  • the process comprising:
    (a) reacting phosphonium bromide compound of Formula-IV with an aldehyde compound of Formula-III in the presence of an alkali or alkaline earth metal base in one or more suitable polar aprotic solvent to provide (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of Formula-II,
    (b) treating compound of Formula-II with one or more suitable polar solvent to form reaction mixture;
    (c) heating the reaction mixture at an elevated temperature;
    (d) cooling the reaction mixture to ambient temperature; and
    (e) isolating the (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester in crystalline form.
  • The phosphonium bromide compound of Formula-IV and aldehyde compound of Formula-III can be reacted in the presence of alkali or alkaline earth metal base. The alkali or alkaline earth metal base comprises one or more of sodium hydroxide, potassium hydroxide, lithium hydroxide, potassium carbonate, sodium carbonate, lithium carbonate, cesium carbonate and the like. In particular, it may be potassium carbonate.
  • Embodiments includes that the reaction can be performed in one or more of suitable polar aprotic solvent selected from dimethylformamide, dimethylsulfoxide, dimethylacetamide, tetrahydrofuran, N-methylpyrrolidone or mixtures thereof. In particular it may bedimethylsulfoxide at an ambient temperature i.e. at about 15° C. to about 40° C. In particularly, it may be from about 20° C. to about 35° C.
  • The reaction mixture can be stirred for about 5 to 15 hours till completion of the reaction. In particular, it may be for 10 hours. The reaction mixture can be further treated with suitable organic solvents like toluene, xylene, methylene dichloride, ethyl acetate for extracting compound of Formula-II. In particular, the compound of Formula (II) may be extracted with toluene.
  • The compound of Formula-II can be isolated by removal of toluene followed by addition of isopropanol. After the addition of isopropanol, the reaction mixture can be heated to 40° C. to 80° C., particularly at about 60° C. to 70° C. and cooling to 15° C. to obtain compound of formula (II). The compound of formula (II) can be purified in suitable polar solvent like methanol, ethanol, Isopropanol, acetone, DMF, ethyl acetate, butyl acetate and the like. In particular, it may be methanol.
  • In general, the term “elevated temperature” includes heating the compound II in a polar solvent at about 50° C. to about 100° C. In particular, the compound II may be heated at about 50° C. to about 70° C., most particularly, at about 60° C. to 65° C.
  • In general, the term “ambient temperature” includes cooling the reaction mixture comprising the compound II in a polar solvent at about 0° C. to about 30° C. In particular, it may be at about 0° C. to about 15° C., most particularly, at about 0° C. to 10° C. According to the embodiment, the compound (II) i.e. (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester is obtain in crystalline form after purification in polar solvent.
  • The crystalline form of compound (II) is characterized by an X-ray powder diffraction pattern having characteristics peaks expressed in degrees 2θ (±0.2° 2θ) at 7.86°, 9.94°, 11.48°, 12.71°, 14.80°, 15.88°, 17.44°, 18.16°, 19.17°, 19.97°, 20.77°, 22.71°, 23.41°, 24.68°, 26.02°, 27.63° and 29.36°±0.2°. The X-ray powder diffraction pattern is characterized substantially the same that shown in FIG. 3.
  • The crystalline form of compound (II) is characterized by an IR spectrum having peaks at about 2999, 2976, 1720, 1600, 1512, 1487, 1379, 1342, 1288, 1197, 1134, 1066, 1035, 931 and 842 cm−1 and DSC endotherm at about 116.04° C. The DSC thermogram is substantially the same that shown in FIG. 4.
  • According to the further embodiment, there is provided a process for the preparation of pitavastatinzinc of formula (IC),
  • Figure US20120022102A1-20120126-C00017
  • the process comprising:
    (a) reacting phosphonium bromide compound of Formula-IV with an aldehyde compound of Formula-III in the presence of an alkali or alkaline earth metal base in one or more suitable polar aprotic solvent to provide (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of formula-II;
    (b) hydrolyzing the compound of Formula-II under the acidic conditions to remove the acetonide protection to form diol compound;
    (c) treating the diol compound of step (b) in-situ with an alkali metal hydroxide to form the corresponding alkali metal salt of pitavastatin (I);
    (d) treating the alkali metal salt of pitavastatin (I) with a zinc source to obtain Pitavastatinzinc; and
    (e) isolating the pitavastatinzinc.
  • In general, the process parameters for the preparation of compound (II) and its hydrolysis are similar as discloses herein above. The preferable zinc source comprises one or more of zinc formate, zinc acetate, zinc propionate, zinc maleate, zinc fumarate, zinc tartrate, zinc lactate, zinc malate, zinc citrate, Zinc ascorbate, zinc malonate, zinc oxalate, zinc glycolate, zinc methanesulfonate, zinc ethanesulfonate, a salt of zinc with amino acid, zinc sulfate, zinc chloride, zinc carbonate or zinc nitrate. In particular, it comprises one or more of zinc sulfate, zinc chloride or zinc acetate.
  • According to the further aspect, there is provided a method for the preparation of pitavastatinpotassium of formula (ID),
  • Figure US20120022102A1-20120126-C00018
  • the process comprising:
    (a) reacting phosphonium bromide compound of Formula-IV with an aldehyde compound of Formula-III in the presence of an alkali or alkaline earth metal bases in one or more suitable polar aprotic solvent to provide (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of Formula-II,
    (b) hydrolyzing the compound of Formula-II by subjecting under the acidic conditions to remove the acetonideprotection to form diol compound;
    (c) treating the diol compound of step (b) in-situwith a potassium source to obtain pitavastatinpotassium.
  • In general, the process parameters for the preparation of compound (II) and its hydrolysis are similar as discloses herein above. The preferable potassium source comprises one or more of potassium hydroxide, potassium carbonate, potassium bicarbonate, potassium acetate, potassium chloride and the like.
  • According to the further embodiment, there is provided a process for the preparation of amorphous form of pitavastatinmagnesium, the process comprising:
  • (a) providing a solution comprising pitavastatinmagnesium in a suitable organic solvent wherein the organic solvent is selected from the group consisting of a chlorinated solvent, alcoholic solvent, ketonic solvent, esters solvent and mixtures thereof;
    (b) removing the organic solvent to obtain residue;
    (c) adding a suitable anti-solvent to the residue; and
    (d) recovering the amorphous form of the pitavastatinmagnesium.
  • The amorphous form can be generally prepared by addition of anti-solvent to a concentrated solution of pitavastatinmagnesium in an organic solvent.
  • Embodiments of the process includes preparing the solution of pitavastatinmagnesium in suitable organic solvent selected from the group consisting of a chlorinated solvent, alcoholic solvent, ketonic solvent, ester solvents and mixtures thereof. The preferred solvent comprises one or more of methylene dichloride, ethylene dichloride, chlorobenzene, methanol, ethanol, isopropanol, butanol, acetone, methylethyl ketone, ethyl acetate, butyl acetate, isopropyl acetate, and mixtures thereof or mixture thereof with water. In particular, the suitable solvent comprises one or more of methanol, acetone, ethyl acetate.
  • In general, the embodiment of the process includes adding suitable antisolvent to the solution of pitavastatinmagnesium in suitable organic solvent. The suitable anti-solvent comprises one or more of hexane, heptane, cyclohexane, toluene, xylene, diisopropyl ether, methyl tert-butyl ether, 1,4-dioxane, tetrahydrofuranand the like. In particular, the suitable anti-solvent comprises one or more of heptane or cyclohexane or methyl tert-butyl ether.
  • According to the embodiment, there is provided a process for the preparation of amorphous form of pitavastatinmagnesium, the process comprising:
  • (a) providing a solution comprising pitavastatinmagnesium in a suitable organic solvent wherein the organic solvent is one or more of a chlorinated solvent, alcoholic solvent, ketonic solvent, esters solvent and mixtures thereof;
    (b) heating reaction mixture at an elevated temperature followed by cooling to ambient temperature;
    (c) adding a suitable anti-solvent to the solution; and
    (d) recovering the amorphous form of pitavastatinmagnesium.
  • In general, the suitable solvents and anti-solvents comprises from the same as listed herein above. However, the reaction mixture can be heated to an elevated temperature in step (b). The elevated temperature is from about 50° C. to about 100° C. In particularly, it may be from about 70° C. to about 90° C.
  • The reaction mixture is then cooled to an ambient temperature, preferably from about 15° C. to about 35° C., preferably from about 25° C. to 35° C.
  • It is preferable that the anti-solvent and solvent are miscible. The amorphous form can also be prepared by lyophilization of or removal of solvent from the solution of pitavastatinmagnesium in a suitable solvent.
  • According to the further embodiments, there is provided a process for the preparation of amorphous form of pitavastatinmagnesium having water content less than about 2% wt/wt, the process comprising:
  • (a) providing pitavastatinmagnesium in crystalline form having water content in the range of about 8% to about 12% wt/wt;
    (b) contacting the pitavastatinmagnesium with humid air in a fluidized bed drier, or maintaining the pitavastatinmagnesium at a temperature of from about 5 to about 60° C., under pressure of less than 30 mm/Hg for a period of from about 1 to 5 days; and
    (c) recovering the pitavastatin magnesium in the amorphous form having water content less than about 2% wt/wt.
  • According to the process, amorphous form of pitavastatinmagnesium having water content less than about 2% wt/wt is prepared by contacting pitavastatinmagnesium containing about 8% to about 12% of water content with humid air in a fluidized bed apparatus.
  • In particular, the temperature is of about 25° C. to about 50° C., more particularly at about 30° C. to about 40° C. The contacting may be carried out, in particularly at about 6 hours to 2 days. As used herein, the term “humid” refers to a relative humidity of at least 30%. In particular, it may be at least about 50% and most particularly at least about 70%.
  • According to the further embodiment, there is provided substantially pure pitavastatinmagnesium in stable crystalline form.
  • In another embodiment, there is provided pitavastatinmagnesium substantially free desfluoro impurity, cis-isomer impurity, pitavastatin 5-oxo impurity, pitavastatinlactone impurity, pitavastatin t-butyl diol ester impurity and pitavastatincondensed impurity when measured by area percentage of HPLC. Also, pitavastatindiastereomeric impurity less than 0.3% by area percentage of HPLC.
  • According to the further embodiment, there is provided a pharmaceutical composition comprising a therapeutically effective amount of crystalline pitavastatinmagnesium characterized by X-ray diffraction pattern having characteristic peaks at 2-theta values 10.1°, 13.2°, 19.3° and 27.2°±0.2°, and one or more pharmaceutically acceptable carriers, excipients or diluents.
  • According to the further embodiment, there is provided a pharmaceutical composition comprising a therapeutically effective amount of amorphouspitavastatinmagnesium characterized by x-ray diffraction pattern substantially as depicted in FIG. 2, and one or more pharmaceutically acceptable carriers, excipients or diluents.
  • The starting material, phosphonium bromide compound of Formula-IV, can be prepared from alcoholic compound of formula (VI)
  • Figure US20120022102A1-20120126-C00019
  • The alcoholic compound of formula (VI) is converted o phosphonium compound of Formula (IV) via formation of 3-(bromomethyl)-2-cyclopropyl-4(4′-fluorophenyl)quinoline of Formula (V) by the known process reported in the prior art. WO 95/11898 A1 in its reference example-7 and Example-1 or as per the process disclosed in U.S. Pat. No. 6,627,636 and U.S. Pat. No. 5,763,675.
  • Figure US20120022102A1-20120126-C00020
  • The bromo compound of formula (V) 3-(bromomethyl)-2-cyclopropyl-4-(4′-fluorophenyl)quinoline with wittig reagent like triphenyl phosphine in suitable non-polar solvents like toluene, o-xylene, chlorobenzeneetc to obtain phosphonium bromide compound of formula (IV).
  • The starting reagent, alcohol compound of formula (VI) can be prepared from the known process reported in the art like Tetrahedron Letters, Vol. 34, No. 51, p.p. 8271-8274 (1993); Heterocycles, Vol. 50, No. 1, 1999; Drugs of Future 1998 23 (8) or Tetrahedron Asymmetry 1993, Vol. 4, pp. 201-204 are reported herein as reference in its entirety.
  • As set forth in the following schemes, the pitavastatin magnesium can be prepared by as shown bellow:
  • Figure US20120022102A1-20120126-C00021
  • The present invention is further illustrated by the following examples which are provided merely to be exemplary of the invention and do not limit the scope of the invention. Certain modifications and equivalents will be apparent to those skilled in the art and are intended to be included within the scope of the present invention.
    • Preparation-1 Preparation of 3-(bromomethyl)-2-cyclopropyl-4-(4′-fluorophenyl)quinoline (V)
  • Figure US20120022102A1-20120126-C00022
  • 1 Kg of alcohol compound of formula (VI) and 8 L of methylene dichloride were taken in reactor at 0° C. 0.462 Kg of freshly prepared phosphonium bromide solution in 2 L methylene dichloride was added slowly and stirred at 25° C. for 2 hours. After the completion of the reaction as monitored by TLC, the reaction mixture was quenched with 5% sodium bicarbonate solution to adjust the pH from 7-8. The organic layer was separated and washed with 5 L water followed by removal of solvent under vacuum at 45° C. The residue was treated with 2.5 L heptane at 60° C. and cooled to 15° C. The product was filtered at 15° C. and dried under vacuum at 55° C. for 8 hours to obtain 3-(bromomethyl)-2-cyclopropyl-4-(4′-fluorophenyl)quinoline.
    • Preparation-2 Preparation of Phosphonium Bromide Compound of Formula (IV)
  • Figure US20120022102A1-20120126-C00023
  • 1 Kg of 3-(bromomethyl)-2-cyclopropyl-4-(4′-fluorophenyl)quinoline, 10 L of toluene and 300 mL of isopropanol were taken in reactor and heated at 50° C. 0.874 Kg of triphenyl phosphine solution in 2 L toluene was added slowly and stirred for 3 hours. The reaction mixture was cooled to 25° C. and stirred for 1 hour. The product was filtered and washed with toluene. The product was dried in tray dryer at 55° C. for 8 hours to obtain phosphonium bromide compound of formula (IV).
    • Example-1 Preparation of (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of formula II
  • Figure US20120022102A1-20120126-C00024
  • To the solution of 0.751 Kg of tert-butyl-2-((4R,6S)-6-formul-2,2-dimethyl-1,3-dioxan-4-yl)acetate (III) in 7 L of dimethylsulphoxide was added 1 Kg of phosphonium bromide compound of formula (IV) and 0.67 Kg of potassium carbonate. The reaction mixture was stirred at 25° C. for 10 hours. The reaction mixture was quenched with water and extracted with toluene. The organic layer was concentrated and the title compound was isolated using isopropanol as crude solid. The crude product thus obtained was recrystallized in methanol as shown below.
    • Purification of Olefin Compound of Formula II
  • Pitavastatin Olefin compound (II) (100 g) and methanol (600 mL) were heated to 60° C. to 65° C. to obtain the clear solution and stirred for 10 mins. Activated Carbon (10 g) were added at 60° C. to 65° C. and stirred for 10 min. The reaction mixture was filtered and washed with methanol (100 mL). The filtrate was cooled to 25° C. and gradually to 10° C. followed by stirring for 2 hours at 10° C. The resulting slurry was filtered and washed with chilled methanol (100 mL). The wet-cake was heated in methanol (480 mL) at 60° C. to 65° C. to obtain the clear solution. Activated Carbon (10 g) were added at 60° C. to 65° C. and stirred for 10 min. The reaction mixture was filtered and washed with methanol (100 mL). The filtrate was cooled to 25° C. and gradually to 10° C. followed by stirring for 2 hours at 10° C. The resulting slurry was filtered and washed with chilled methanol (100 mL). The wet-cake was dried under vacuum for 30 minutes followed by drying in hot air oven at 50° C. to 55° C. for 12 hours to obtain crystalline olefin compound (II) characterized by X-ray powder diffraction substantially as same as shown in FIG. 3 and DSC thermogram having endothermic peak at about 116.04° C. as shown in FIG. 4.
    • Example-2 Preparation of Pitavastatin Magnesium of Formula (IB)
  • Figure US20120022102A1-20120126-C00025
  • To the solution of 100 g of (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of formula II (crystalline) in 1 L methanol was added 272.8 mL 1N HCl solution at 25° C. The reaction mixture was stirred for 8 hours. The reaction mixture was cooled to 15° C. and treated with 23.2 g 10% sodium hydroxide solution.
  • The reaction mixture was stirred for 4 hours at 25° C. and quenched in water. The reaction mass was treated with 92 mL 1 N HCl solution to adjust the pH of about 8.0 and treated with methylene dichloride for washing. The separated aqueous layer is treated with 100 g of magnesium chloride hexahydrate and stirred for 30 min at 25° C. The solution is cooled to 15° C., filtered and washed with water. The product is dried in hot air oven for 4 hours to obtain 82 g of crystalline Pitavastatin Magnesium having water content of 11.0%. (XRD as shown in FIG. 1)
    • Example-3 Preparation of Pitavastatin Zinc of Formula (IC)
  • Figure US20120022102A1-20120126-C00026
  • To the solution of 100 g of (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of formula II (crystalline) in 1 L methanol was added 272.8 mL 1N HCl solution at 25° C. The reaction mixture was stirred for 8 hours. The reaction mixture was cooled to 15° C. and treated with 23.2 g 10% sodium hydroxide solution. The reaction mixture was stirred for 4 hours at 25° C. and quenched in water. The reaction mass was treated with 92 mL 1 N HCl solution to adjust the pH of about 8.0 and treated with methylene dichloride for washing. The separated aqueous layer is treated with 100 g of zinc sulfate and stirred for 30 min at 25° C. The solution is cooled to 15° C., filtered and washed with water. The product is dried in hot air oven for 4 hours to obtain 75 g of crystalline Pitavastatin zinc.
    • Example-4 Preparation of Pitavastatin Potassium of Formula (ID)
  • Figure US20120022102A1-20120126-C00027
  • To the solution of 100 g of (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of formula II (crystalline) in 1 L methanol was added 272.8 mL 1N HCl solution at 25° C. The reaction mixture was stirred for 8 hours. The reaction mixture was cooled to 15° C. and treated with 23.2 g 10% sodium hydroxide solution. The reaction mixture was stirred for 4 hours at 25° C. and quenched in water. The reaction mass was treated with 92 mL 1 N HCl solution to adjust the pH of about 8.0 and treated with methylene dichloride for washing. The separated aqueous layer is treated with 80 g of Potassium hydroxide and stirred for 30 min at 25° C. The solution is cooled to 15° C., filtered and washed with water. The product is dried in hot air oven for 4 hours to obtain 72 g of crystalline Pitavastatin Potassium.
    • Example 5 Preparation of the Amorphous Form of Pitavastatin Magnesium
  • 100 g of crystalline Pitavastatin Magnesium was dissolved in 800 ml Ethyl Acetate by heating at 75° C. to 80° C. The slightly turbid solution was filtered through hyflow bed at 75° C. to 80° C. The filtrate was cooled to 25° C. and added to cyclohexane (3300 mL). The reaction mixture was stirred for 2 hours. The reaction mixture was filtered and wet-cake was washed with cyclohexane (100 mL). The product was dried in hot air oven for 12 hours to get 83.0 g amorphous Pitavastatin Magnesium. The obtained solid was amorphous as is shown by the X-ray diffraction pattern given in FIG. 2.
    • Example 6 Preparation of the Amorphous Form of Pitavastatin Magnesium
  • 100 g of crystalline Pitavastatin Magnesium was dissolved in 800 ml Ethyl Acetate by heating at 75° C. to 80° C. The slightly turbid solution was filtered through hyflow bed at 75° C. to 80° C. The filtrate was distilled under vacuum till dry powder obtained at 45° C. to 50° C. The solid was cooled to 25° C. and cyclohexane (500 mL) was added to the filtrate and stirred for 30 min. The reaction mixture was filtered and wet-cake was washed with cyclohexane (100 mL). The product was dried in hot air oven for 12 hours to get 83.0 g amorphous Pitavastatin Magnesium. The obtained solid was amorphous as is shown by the X-ray diffraction pattern given in FIG. 2.
    • Example 7 Preparation of the Amorphous Form of Pitavastatin Magnesium
  • 100 g of crystalline Pitavastatin Magnesium and Methanol (500 mL) were stirred in RBF for 30 minutes. The reaction mixture was distilled at 45° C. to 50° C. under vacuum to obtain dry product. The filtrate was distilled under vacuum till dry powder obtained at 45° C. to 50° C. The solid was cooled to 25° C. and cyclohexane (500 mL) was added to the filtrate and stirred for 30 min. The reaction mixture was filtered and wet-cake was washed with cyclohexane (100 mL). The product was dried in hot air oven for 12 hours to get 83.0 g amorphous Pitavastatin Magnesium.
    • Example 8 Preparation of the Amorphous Form of Pitavastatin Magnesium
  • 100 g of crystalline Pitavastatin Magnesium was dissolved in 800 ml Acetone by heating at 55° C. to 60° C. The slightly turbid solution was filtered through hyflow bed at 55° C. to 60° C. The filtrate was cooled to 25° C. and added to diisopropyl ether (3000 mL). The reaction mixture was stirred for 3-min. The reaction mixture was filtered and wet-cake was washed with diisopropyl ether (100 mL). The product was dried in hot air oven for 12 hours to get 45.0 g amorphous Pitavastatin Magnesium.
    • Example 9 Preparation of the Amorphous Form of Pitavastatin Magnesium
  • 10 g of Pitavastatin Magnesium having water content 11% was dried in fluid bed dried at 45° C. for 2 days to obtain amorphous Pitavastatin Magnesium having water content less than 2% wt/wt. An X-ray diffraction study on the product showed it to be amorphous.
    • Example 10 Preparation of the Amorphous Form of Pitavastatin Magnesium
  • 10 g of Pitavastatin Magnesium having water content 11% was dried in vacuum tray dryer at about 5 to about 60° C., under pressure of less than 30 mm/Hg for a period of 24 hours to obtain amorphous Pitavastatin Magnesium having water content less than 2% wt/wt. An X-ray diffraction study on the product showed it to be amorphous, see FIG. 2.
  • While the present invention has been described in terms of its specific embodiments, certainmodifications and equivalents will be apparent to those skilled in the art and are intended to beincluded within the scope of the present invention.
    • ADVANTAGES OF THE INVENTION
  • 1. The present invention provides novel pharmaceutically acceptable salt of alkali metal salts of Pitavastatin.
    2. The present invention provides an improved process for the preparation of pitavastatinalkali metal salts.
    3. The present invention provides crystalline form of pitavastatinmagnesium having 8% to 12% water content.
    4. The present invention also provides amorphous form of pitavastatinmagnesium and process for preparation thereof.
    5. The present invention provides amorphous form of pitavastatinmagnesium containing less than about 2% of water content.
    6. The process provided is eco-friendly, economically viable and easily scalable on large scale production.

Claims (46)

1. A compound, which is alkali or alkaline earth metal salts of pitavastatin, wherein the alkali or earth metal comprise one or more of magnesium, zinc, potassium, strontium and barium.
2. The compound as claimed in claim 1, which is pitavastatinmagnesium.
3. The compound as claimed in claim 2, wherein the compound is a hydrate.
4. The compound as claimed in claim 3, wherein thecompound has water content in the range of from about 7% to about 12% wt/wt.
5. The compound as claimed in claim 2, wherein the compound is crystalline.
6. The compound as claimed in claim 5, wherein the crystalline form is characterized by an X-ray powder diffraction pattern having characteristics peaks expressed in degrees 2θ (±0.2° 2θ) at 10.1°, 13.2°, 19.3° and 27.2°±0.2°.
7. The compound as claimed in claim 6 having an x-ray powder diffraction pattern substantially same as that shown in FIG. 1.
8. The compound as claimed in claim 2, wherein the compound is amorphous.
9. The compound as claimed in claim 8 having x-ray powder diffraction pattern substantially same that shown in FIG. 2.
10. The compound as claimed in claim 8, wherein the compound has water content less than about 5% wt/wt.
11. The compound as claimed in claim 2 having a specific optical rotation of about +22.0 to +22.5 in 1% DMSO at 20±0.5° C.
12. A pharmaceutical composition comprising pitavastatinmagnesium and one or more pharmaceutically acceptable carriers or excipients.
13. The compound as claimed in claim 2, wherein the pitavastatinmagnesium is substantially pure having a purity greater than about 99% by area percentage of HPLC.
14. The compound as claimed in claim 2, wherein the pitavastatinmagnesium is substantially pure having less than about 0.3% of diastereomeric impurity by area percentage of HPLC.
15. A process for the preparation of pitavastatinmagnesium of Formula (1B),
Figure US20120022102A1-20120126-C00028
the process comprising:
(a) reacting phosphonium bromide compound of Formula-IV
Figure US20120022102A1-20120126-C00029
with an aldehyde compound of Formula-III
Figure US20120022102A1-20120126-C00030
in the presence of an alkali or alkaline earth metal base in one or more suitable polar aprotic solvents to provide (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of Formula-II;
Figure US20120022102A1-20120126-C00031
(b) hydrolyzing the compound of Formula-II under acidic conditions to remove acetonideprotection to form a diol compound;
(c) treating the diol compound of step (b) in situ with an alkali metal hydroxide to form corresponding alkali metal salt of pitavastatin (I);
Figure US20120022102A1-20120126-C00032
wherein, M is Na+, K+, Li+;
(d) treating alkali metal salt of pitavastatin (I) with a magnesium source to obtain pitavastatinmagnesium; and
(e) isolating the pitavastatinmagnesium.
16. The process as claimed in claim 15 (a), wherein the alkali or alkaline earth metal base comprises one or more of sodium hydroxide, potassium hydroxide, lithium hydroxide, potassium carbonate, sodium carbonate, lithium carbonate, cesium carbonate, and the like.
17. The process as claimed in claim 15 (a), wherein the suitable polar aprotic solvent comprises one or more of dimethylformamide, dimethylsulfoxide, dimethylacetamide, tetrahydrofuran, N-methylpyrrolidone, or mixtures thereof.
18. The process as claimed in claim 15, wherein the compound (II) can optionally be isolated by removal of the solvent.
19. The process as claimed in claim 15, wherein the compound (II) can optionally be purified in suitable polar solvent like methanol, ethanol, isopropanol, acetone, DMF, ethyl acetate, butyl acetate, and the like.
20. The process as claimed in claim 15 (b), wherein the hydrolysis of compound (II) under acidic conditions can be done by selecting suitable acids from hydrochloric acid, acetic acid, sulfuric acid, nitric acid, phosphoric acid, and the like.
21. The process as claimed in claim 15 (c), wherein the suitable alkali metal hydroxide comprises one or more of sodium hydroxide, potassium hydroxide, lithium hydroxide, and the like.
22. The process as claimed in claim 15 (c), wherein the alkali metal salt of pitavastatin is pitavastatinsodium.
23. The process as claimed in claim 15 (d), wherein the suitable magnesium source comprises one or more of magnesium chloride, magnesium methoxide, magnesium acetate and hydrates thereof.
24. The process as claimed in claim 15 (e), wherein the pitavastatin magnesium is isolated in a crystalline form.
25. A compound (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester of Formula (II) in crystalline form.
26. The compound as claimed in claim 25, wherein the crystalline form is characterized by an X-ray powder diffraction pattern having characteristics peaks expressed in degrees 20 at 7.86°, 9.94°, 11.48°, 12.71°, 14.80°, 15.88°, 17.44°, 18.16°, 19.17°, 19.97°, 20.77°, 22.71°, 23.41°, 24.68°, 26.02°, 27.63° and 29.36°±0.2°.
27. The compound as claimed in claim 25, wherein the crystalline form is characterized by an IR spectrum having peaks at about 2999, 2976, 1720, 1600, 1512, 1487, 1379, 1342, 1288, 1197, 1134, 1066, 1035, 931 and 842 cm.
28. The compound as claimed in claim 25, wherein the crystalline form is having DSC endotherm at about 116.04° C.
29. An improved process for the preparation of (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)-quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester of Formula (II),
Figure US20120022102A1-20120126-C00033
the process comprising:
(a) reacting phosphonium bromide compound of Formula-IV with an aldehyde compound of Formula-III in the presence of an alkali or alkaline earth metal base in one or more suitable polar aprotic solvents to provide an (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of Formula-II;
(b) treating compound of Formula-II with one or more suitable polar solvents to form a reaction mixture;
(c) heating the reaction mixture at an elevated temperature;
(d) cooling the reaction mixture to ambient temperature; and
(e) isolating the (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester in crystalline form.
30. The process as claimed in claim 29, wherein the suitable polar solvent comprises one or more of methanol, ethanol, isopropanol, acetone, DMF, ethyl acetate, butyl acetate, and the like.
31. The process as claimed in claim 29, wherein the elevated temperature is from about 50° C. to about 100° C.
32. The process as claimed in claim 29, wherein the ambient temperature is from about 0° C. to about 30° C.
33. A process for the preparation of amorphous form of pitavastatinmagnesium, the process comprising:
(a) providing a solution comprising pitavastatinmagnesium in a suitable organic solvent wherein the organic solvent is one or more of a chlorinated solvent, alcoholic solvent, ketonic solvent, esters solvent and mixtures thereof;
(b) removing the organic solvent to obtain a residue;
(c) adding a suitable anti-solvent to the residue; and
(d) recovering the amorphous form of the pitavastatinmagnesium.
34. The process as claimed in claim 33 (a), wherein the suitable organic solvent comprises one or more of methylene dichloride, ethylene dichloride, chlorobenzene, methanol, ethanol, isopropanol, butanol, acetone, methylethyl ketone, ethyl acetate, butyl acetate, isopropyl acetate, and mixtures thereof or mixture thereof with water.
35. The process as claimed in claim 33 (c), wherein the suitable anti-solvent comprises one or more of hexane, heptane, cyclohexane, toluene, xylene, diisopropyl ether, methyl tert-butyl ether, 1,4-dioxane, tetrahydrofuran, and the like.
36. A process for the preparation of amorphous form of pitavastatinmagnesium, the process comprising:
(a) providing a solution comprising pitavastatinmagnesium in a suitable organic solvent wherein the organic solvent is one or more of a chlorinated solvent, alcoholic solvent, ketonic solvent, esters solvent and mixtures thereof;
(b) heating reaction mixture at an elevated temperature followed by cooling to ambient temperature;
(c) adding a suitable anti-solvent to the solution; and
(d) recovering the amorphous form of the pitavastatinmagnesium.
37. The process as claimed in claim 36 (a), wherein the suitable organic solvent comprises one or more of methylene dichloride, ethylene dichloride, chlorobenzene, methanol, ethanol, isopropanol, butanol, acetone, methylethyl ketone, ethyl acetate, butyl acetate, isopropyl acetate, and mixtures thereof or mixture thereof with water.
38. The process as claimed in claim 36 (b), wherein the elevated temperature is from about 50° C. to about 100° C.
39. The process as claimed in claim 36 (b), wherein the ambient temperature is from about 15° C. to about 35° C.
40. The process as claimed in claim 36 (c), wherein the suitable anti-solvent comprises one or more of hexane, heptane, cyclohexane, toluene, xylene, diisopropyl ether, methyl tert-butyl ether, 1,4-dioxane, tetrahydrofuran, and the like.
41. A process for the preparation of an amorphous form of pitavastatinmagnesium having water content less than 2% wt/wt, the process comprising:
(a) providing pitavastatinmagnesium in crystalline form having water content in the range of about 8% to about 12% wt/wt;
(b) contacting the pitavastatinmagnesium with humid air in a fluidized bed drier, or maintaining the pitavastatinmagnesium at a temperature of from about 5 to about 60° C., under pressure of less than 30 mm/Hg for a period of from about 1 to 5 days; and
(c) recovering the pitavastatinmagnesium in the amorphous form having water content less than 2% wt/wt.
42. The process as claimed in claim 41, wherein the humid air refers to a relative humidity of at least 30%.
43. A process for the preparation of pitavastatinzinc of Formula (1C),
Figure US20120022102A1-20120126-C00034
the process comprising:
(a) reacting phosphonium bromide compound of Formula-IV with an aldehyde compound of Formula-III in the presence of an alkali or alkaline earth metal base in a suitable polar aprotic solvent to provide (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of Formula-II;
(b) hydrolyzing the compound of Formula-II under acidic conditions to remove the acetonide protection to form a diol compound;
(c) treating the diol compound of step (b) in situ with an alkali metal hydroxide to form corresponding alkali metal salt of pitavastatin (I);
(d) treating the alkali metal salt of pitavastatin (I) with a zinc source to obtain pitavastatin zinc; and
(e) isolating the pitavastatin zinc.
44. The process as claimed in claim 43, wherein the zinc source comprises one or more of zinc formate, zinc acetate, zinc propionate, zinc maleate, zinc fumarate, zinc tartrate, zinc lactate, zinc malate, zinc citrate, zinc ascorbate, zinc malonate, zinc oxalate, zinc glycolate, Zinc methanesulfonate, zinc ethanesulfonate, a salt of zinc with amino acid, zinc sulfate, zinc chloride, zinc carbonate or zinc nitrate.
45. A process for the preparation of pitavastatinpotassium of Formula (1D),
Figure US20120022102A1-20120126-C00035
the process comprising:
(a) reacting phosphonium bromide compound of Formula-IV with an aldehyde compound of Formula-III in the presence of an alkali or alkaline earth metal base in a suitable polar aprotic solvent to provide an (4R,6S)-(E)-6-[2-(2-cyclopropyl-4-(4-fluorophenyl)quinoline-3-yl)-vinyl-2,2-dimethyl-1,3-dioxane-4-yl]acetic acid tertiary butyl ester compound of Formula-II;
(b) hydrolyzing the compound of Formula-II by subjecting under the acidic conditions to remove the acetonideprotection to form a diol compound; and
(c) treating the diol compound of step (b) in situ with a potassium source to obtain pitavastatinpotassium.
46. The process as claimed in claim 45, wherein the potassium source comprises one or more of potassium hydroxide, potassium carbonate, potassium bicarbonate, potassium acetate, potassium chloride, and the like.
US13/009,492 2010-01-20 2011-01-19 Method for preparation of pitavastatin and its pharmaceutical acceptable salts thereof Abandoned US20120022102A1 (en)

Priority Applications (2)

Application Number Priority Date Filing Date Title
US13/665,932 US8829186B2 (en) 2010-01-20 2012-11-01 Method for preparation of pitavastatin and pharmaceutical acceptable salts thereof
US14/479,575 US9139527B2 (en) 2010-01-20 2014-09-08 Method of preparation of pitavastatin and pharmaceutical acceptable salts thereof

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
IN159/MUM/2010 2010-01-20
IN159MU2010 2010-01-20

Related Child Applications (1)

Application Number Title Priority Date Filing Date
US13/665,932 Division US8829186B2 (en) 2010-01-20 2012-11-01 Method for preparation of pitavastatin and pharmaceutical acceptable salts thereof

Publications (1)

Publication Number Publication Date
US20120022102A1 true US20120022102A1 (en) 2012-01-26

Family

ID=44169119

Family Applications (3)

Application Number Title Priority Date Filing Date
US13/009,492 Abandoned US20120022102A1 (en) 2010-01-20 2011-01-19 Method for preparation of pitavastatin and its pharmaceutical acceptable salts thereof
US13/665,932 Active US8829186B2 (en) 2010-01-20 2012-11-01 Method for preparation of pitavastatin and pharmaceutical acceptable salts thereof
US14/479,575 Expired - Fee Related US9139527B2 (en) 2010-01-20 2014-09-08 Method of preparation of pitavastatin and pharmaceutical acceptable salts thereof

Family Applications After (2)

Application Number Title Priority Date Filing Date
US13/665,932 Active US8829186B2 (en) 2010-01-20 2012-11-01 Method for preparation of pitavastatin and pharmaceutical acceptable salts thereof
US14/479,575 Expired - Fee Related US9139527B2 (en) 2010-01-20 2014-09-08 Method of preparation of pitavastatin and pharmaceutical acceptable salts thereof

Country Status (3)

Country Link
US (3) US20120022102A1 (en)
JP (1) JP2013516459A (en)
WO (1) WO2011089623A2 (en)

Cited By (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2014203045A1 (en) 2013-06-20 2014-12-24 Lupin Limited A novel, green and cost effective process for synthesis of tert-butyl (3r,5s)-6-oxo-3,5-dihydroxy-3,5-o-isopropylidene-hexanoate

Families Citing this family (7)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2012025939A1 (en) 2010-08-25 2012-03-01 Cadila Healthcare Limited Pitavastatin calcium and process for its preparation
SI2751081T1 (en) 2011-09-12 2017-05-31 Farma Grs, D.O.O. Polymorphic form of pitavastatin calcium
JP2013103884A (en) * 2011-11-10 2013-05-30 Daito Kk Industrial production method of pitavastatin calcium salt
CN102898367B (en) * 2012-11-15 2014-04-30 江苏阿尔法药业有限公司 Preparation method of pitavastatin calcium crude drug midbody
CN103508948A (en) * 2013-10-17 2014-01-15 凯莱英医药集团(天津)股份有限公司 Method for preparing pitavastatin calcium
CN109867695B (en) * 2017-12-01 2021-09-17 上虞京新药业有限公司 Novel preparation method of pitavastatin calcium intermediate
CN111875538B (en) * 2020-08-06 2022-05-17 安徽省庆云医药股份有限公司 Synthetic method of pitavastatin tert-butyl ester

Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO1995011898A1 (en) * 1992-05-12 1995-05-04 Nissan Chemical Industries Ltd. Condensed pyridine type mevalonolactone intermediate and process for its production

Family Cites Families (14)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CA1336714C (en) 1987-08-20 1995-08-15 Yoshihiro Fujikawa Quinoline type mevalonolactone inhibitors of cholesterol biosynthesis
JP3528186B2 (en) 1991-06-24 2004-05-17 日産化学工業株式会社 Diastereomeric salts of optically active quinoline mevalonic acid
JPH05310700A (en) * 1992-05-12 1993-11-22 Sagami Chem Res Center Condensed pyridine-based mevalonolactone intermediate and its production
GB9314159D0 (en) 1993-07-08 1993-08-18 Zeneca Ltd Chemical process
FR2731706B1 (en) * 1995-03-14 1997-04-11 Cird Galderma AROMATIC HETEROCYCLIC COMPOUNDS, PHARMACEUTICAL AND COSMETIC COMPOSITIONS CONTAINING THEM AND USES
MXPA01000890A (en) 1998-07-23 2002-06-04 Nissan Chemical Ind Ltd Process for the preparation of quinoline derivative and intermediate therefor.
US6627636B2 (en) 2000-06-15 2003-09-30 Bristol-Myers Squibb Company HMG-CoA reductase inhibitors and method
CN102285916B (en) 2003-02-12 2015-02-25 日产化学工业株式会社 Crystalline forms of pitavastatin calcium
TWI328006B (en) 2003-12-26 2010-08-01 Nissan Chemical Ind Ltd Crystal form of quinoline compound and process for its production
SE0400235D0 (en) * 2004-02-06 2004-02-06 Active Biotech Ab New composition containing quinoline compounds
US8455640B2 (en) * 2006-05-03 2013-06-04 Msn Laboratories Limited Process for statins and its pharmaceutically acceptable salts thereof
WO2007132482A2 (en) 2006-05-17 2007-11-22 Manne Satyanarayana Reddy Novel process for the preparation of pitavastatin and its pharmaceutically acceptable salts
ES2763703T3 (en) * 2008-04-15 2020-05-29 Sarcode Bioscience Inc Topical LFA-1 antagonists used in the localized treatment of immune disorders
EP2387561A4 (en) * 2009-01-19 2012-07-25 Msn Lab Ltd Improved process for the preparation of highly pure (3r,5s)-7-ý2-cyclopropyl-4-(4-fluorophenyl) quinolin-3-yl¨-3,5-dihydroxy-6(e)-heptenoic acid and pharmaceutically acceptable salts thereof

Patent Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO1995011898A1 (en) * 1992-05-12 1995-05-04 Nissan Chemical Industries Ltd. Condensed pyridine type mevalonolactone intermediate and process for its production

Cited By (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2014203045A1 (en) 2013-06-20 2014-12-24 Lupin Limited A novel, green and cost effective process for synthesis of tert-butyl (3r,5s)-6-oxo-3,5-dihydroxy-3,5-o-isopropylidene-hexanoate

Also Published As

Publication number Publication date
WO2011089623A3 (en) 2011-12-22
US9139527B2 (en) 2015-09-22
WO2011089623A2 (en) 2011-07-28
JP2013516459A (en) 2013-05-13
US8829186B2 (en) 2014-09-09
US20130059885A1 (en) 2013-03-07
US20150152061A1 (en) 2015-06-04

Similar Documents

Publication Publication Date Title
US9139527B2 (en) Method of preparation of pitavastatin and pharmaceutical acceptable salts thereof
US8487105B2 (en) Process for preparing pitavastatin, intermediates and pharmaceuctically acceptable salts thereof
US20080234302A1 (en) Novel Processes for Preparing Amorphous Rosuvastatin Calcium and a Novel Polymorphic Form of Rosuvastatin Sodium
US8912333B2 (en) Polymorphs of pitavastatin calcium
CA2711043A1 (en) Method of synthesis of bosentan, its polymorphic forms and its salts
US9034901B2 (en) Pitavastatin calcium and process for its preparation
US9518020B2 (en) Process for Regorafenib
AU2007208965A1 (en) A process for manufacturing Rosuvastatin Potassium and crystalline and amorphous forms thereof
CA2632954A1 (en) An improved process for the manufacture of montelukast sodium
US10259790B2 (en) Polymorphic forms of pitavastatin sodium
JP5745050B2 (en) Novel Montelukast 4-halobenzylamine salt and method for producing Montelukast sodium salt using the same
US20100292251A1 (en) Montelukast benzhydryl piperazine salts and process for preparation thereof
US20130072688A1 (en) Method for preparing an intermediate of pitavastatin or of the salt thereof
WO2014086073A1 (en) New crystal form of pitavastatin ester and method of preparing same
JP6059157B2 (en) Montelukast Intermediate Camphorsulfonate
WO2011004298A1 (en) Montelukast hexamethylenediamine salt and its use for the preparation of montelukast sodium

Legal Events

Date Code Title Description
AS Assignment

Owner name: CADILA HEALTHCARE LIMITED, INDIA

Free format text: ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNORS:DWIVEDI, SHRIPRAKASH DHAR;PATEL, DHIMANT JASUBHAI;SHAH, ALPESH PRAVINCHANDRA;REEL/FRAME:026069/0912

Effective date: 20110317

STCB Information on status: application discontinuation

Free format text: ABANDONED -- FAILURE TO RESPOND TO AN OFFICE ACTION