WO2004050618A2 - Crystalline form f of atorvastatin hemi-calcium salt - Google Patents

Crystalline form f of atorvastatin hemi-calcium salt Download PDF

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WO2004050618A2
WO2004050618A2 PCT/US2003/038090 US0338090W WO2004050618A2 WO 2004050618 A2 WO2004050618 A2 WO 2004050618A2 US 0338090 W US0338090 W US 0338090W WO 2004050618 A2 WO2004050618 A2 WO 2004050618A2
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phenylamino
fluorophenyl
dihydroxy
delta
beta
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PCT/US2003/038090
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French (fr)
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WO2004050618A3 (en
WO2004050618A8 (en
Inventor
Fritz Blatter
Martin Szelagiewicz
Paul Adriaan Van Der Schaaf
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Teva Pharmaceutical Industries Ltd.
Teva Pharmaceuticals Usa Inc.
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Priority claimed from EP02406037A external-priority patent/EP1424324A1/en
Application filed by Teva Pharmaceutical Industries Ltd., Teva Pharmaceuticals Usa Inc. filed Critical Teva Pharmaceutical Industries Ltd.
Priority to EP03812471A priority Critical patent/EP1572643A2/en
Priority to AU2003297594A priority patent/AU2003297594A1/en
Priority to CA002508871A priority patent/CA2508871C/en
Publication of WO2004050618A2 publication Critical patent/WO2004050618A2/en
Publication of WO2004050618A3 publication Critical patent/WO2004050618A3/en
Publication of WO2004050618A8 publication Critical patent/WO2004050618A8/en

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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D207/00Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom
    • C07D207/02Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom
    • C07D207/30Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having two double bonds between ring members or between ring members and non-ring members
    • C07D207/34Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having two double bonds between ring members or between ring members and non-ring members with hetero atoms or with carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals, directly attached to ring carbon 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

Definitions

  • the present invention is directed to a crystalline form of Atorvastatin calcium, processes for the preparation thereof and pharmaceutical compositions comprising this crystalline form.
  • Atorvastatin calcium is known by the chemical name, [R-(R * ,R * )J-2-(4-fluorophenyl)-beta,delta-dihydroxy- 5-(1 -methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrroIe-1 -heptanoic acid calcium salt (2:1).
  • Atorvastatin has the following formula:
  • Atorvastatin calcium is an orally-active hypocholesterolaemic, a liver-selective HMG-CoA reductase inhibitor.
  • Processes for the preparation of Atorvastatin calcium are described in US-A-5,273,995, US-A-5,298,627, US-A-6,087,511 , US-A-6,274,740, WO-A-97/03960, WO- A-02/059087, WO-A-02/072073, and in the publications by P.L. Brower et al. in Tetrahedron Letters (1992), vol. 33, pages 2279-2282, K.L. Baumann et al. in Tetrahedron Letters (1992), vol. 33, pages 2283-2284 and A. Graul et al. in Drugs of the Future (1997), vol. 22, pages 956-968.
  • This calcium salt (2:1) is desirable since it enables Atorvastatin calcium to be conveniently formulated.
  • the processes in the above mentioned patents and publications result in the preparation of amorphous Atorvastatin calcium.
  • Atorvastatin calcium in a reproducible, pure and crystalline form to enable formulations to meet exacting pharmaceutical requirements and specifications. Furthermore, it is economically desirable that the product is stable for extended periods of time without the need for specialized storage conditions.
  • Atorvastatin calcium salt (2:1) herein designated as Form F.
  • This novel form of the present invention can be prepared in ecological friendly solvents and has a good thermal stability combined with good solubility characteristics.
  • the present invention is directed to the polymorphic Form F of Atorvastatin calcium salt (2:1 ).
  • the crystalline polymorph F exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d-values (A) at
  • Table 1 d-spacings and 2 ⁇ angles for Form F.
  • the polymorphic Form F of Atorvastatin calcium is especially characterized by a powder X- ray diffraction pattern substantially as depicted in Figure 1.
  • the crystalline polymorph F exhibits a characteristic 13 C CP-MAS solid state NMR spectrum with chemical shifts (in parts per million, with peak intensity in arbitrary units in brackets) at 188.2 (2.5), 184.3 (2.2), 177.4 (2.8), 167.5 (2.9), 162.6 (2.4), 161.0 (3.9), 139.8 (6.5), 138.2 (4.3), 135.8 (5.1), 134.1 (4.0), 132.0 (8.4), 131.2 (7.3), 130.5 (14.0), 129.0 (9.5), 128.0 (6.6), 127.2 (4.6), 125.5 (2.9), 124.0 (4.9), 123.5 (4.7), 122.8 (4.8), 122.1 (6.2), 120.7 (5.4), 117.6 (4.1), 116.6 (4.1), 115.2 (3.6), 112.8 (1.6), 72.9 (4.8), 71.7 (5.2), 69.4 (6.5), 67.1 (4.9), 63.2 (0.7), 46.3 (10.4), 44.1 (12.6), 40.6 (7.6), 36.4 (0.7), 32.1 (3.8), 31.1 (1.3), 28.2 (5.3
  • the polymorphic Form F of Atorvastatin calcium is especially characterized by a 13 C CP- MAS solid state NMR spectrum as depicted in Figure 2. Furthermore, the present invention is directed to processes for the preparation of Form F of Atorvastatin calcium.
  • Form F can generally be prepared by adding Form A to a ketone solvent, especially acetone. It is preferred that the ketone solvent contains as a further solvent some water. The amount of water is preferably about 1 to 30%, more preferably about 5 to 20%, especially about 10 to 20% by volume of the suspension. It is preferred that the suspension is treated at temperatures between 10 and 60°C, preferably at temperatures of 20 to 40°C, especially for a longer periods of time, like 10 to 40 hours. It is further preferred that nucleation of Form F is induced at a temperature of 40 to 60°C, especially at about 60°C, and subsequent ripening and equilibration is performed at temperatures between 20 and 40°C. If desired, during the preparation process seeding with Form F can be carried out.
  • Form F can, for example, be isolated by filtration and dried in air or in vacuum.
  • the above mentioned process can also be carried out using another crystalline form or the amorphous form of atorvastatin calcium.
  • Examples of other crystalline forms are Forms I, II, III, IV, V, VI, VII, VIII, IX, X, XI, XII, A, B1 , B2, C, D and E, which are disclosed and characterized in the references given hereinbefore.
  • Preferred forms for this purpose are Form A (see for example WO-A-02/051804; last but one paragraph of page 2; page 4, last but one paragraph to page 5, first paragraph; Examples 2, 8 and 9; Fig.
  • Form B1 see for example WO-A-02/051804; the paragraph bridging pages 2 and 3; page 5, second paragraph; Example 3; and Fig. 3).
  • Form B2 see for example WO-A-02/051804; page 3, second paragraph; page 5, third paragraph; Example 4; and Fig. 3.
  • Form F can also be prepared from Atorvastatin lactone upon subsequent reaction with NaOH to form Atorvastatin sodium followed by reaction with CaCI 2 in a ketone solvent, especially in acetone. It is preferred that the ketone solvent contains as a further solvent some water. The amount of water is preferably about 1 to 30%. If desired, during the preparation process seeding with Form F can be carried out.
  • Form F can also be prepared directly from Atorvastatin lactone upon reaction with a calcium(ll) salt, like Ca(OH) 2 or Ca(OAc) 2 , in a ketone solvent, especially in acetone. It is preferred that the ketone solution contains as a further solvent some water. The amount of water is preferably about 1 to 30%. If desired, during the preparation process seeding with Form F can be carried out.
  • Form F can also be prepared by adding a concentrated solution of Atorvastatin calcium in an organic solvent, like tetrahydrofuran, to a ketone solvent, especially acetone. It is preferred that the ketone solution contains as a further solvent some water. The amount of water is preferably about 1 to 30%. If desired, during the preparation process seeding with Form F can be carried out.
  • ketone solvent of the preparation processes given above it is preferred to use C 3 - C 8 ketones, especially acetone.
  • Another object of the present invention are crystalline forms of atorvastatin calcium which are essentially free of residual organic solvent.
  • Preferred are Forms I to XII and A, B1 , B2, C, D, E and F which are essentially free of residual organic solvent.
  • Highly preferred are Forms B1 , B2 and F, especially Form F.
  • Forms I to XII and A, B1 , B2, C, D, E are disclosed in the references given above.
  • the following preparations of forms which are essentially free of residual organic solvents can be applied to any form of Atorvastatin calcium. It is preferred that the crystalline forms contain less than 0.5% by weight of residual organic solvent. Highly preferred are amounts of residual organic solvents of less than 5000 ppm, especially less than 2000 ppm.
  • residual organic solvents of less than 400 ppm, especially less than 200 ppm.
  • residual organic solvents are aceton, ethylacetate, tetrahydrofuran, ethanol, methanol, acetonitrile and hexane.
  • the crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta- dihydroxy-5-(1 -methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) which is essentially free of residual organic solvents exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d- values (A) at 31.9 (w), 24.3 (s), 16.3 (w), 13.1 (vw), 12.1 (w), 11.4 (m), 10.2 (s), 8.7 (s), 8.1 (vw), 7.1 (w), 6.9 (w), 6.5 (m), 5.98 (vw), 5.60 (vw), 5.21 (m), 5.00 (m), 4.80 (m), 4.56 (vs), 4.32 (w), 4.23 (m), 4.00 (m), 3.72 (m), 3.48 (m); wherein
  • the crystalline polymorph F of [R-(R * ,R * )]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1- methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) which is essentially free of residual organic solvents is especially characterized by an X-ray powder diffraction pattern substantially as depicted in figure 3.
  • the crystalline polymorphs F have a water content of up to 5% by weight (independently whether the polymorphs are essentially free of residual organic solvents or not).
  • Another object of the present invention are processes for the preparation of crystalline forms of atorvastatin calcium which are essentially free of residual organic solvent.
  • Preferred are processes for the preparation of Forms I to XII and A, B1 , B2, C, D, E and F which are essentially free of residual organic solvent.
  • Highly preferred are processes for the preparation of Forms B1 , B2 and F, especially Form F, which are essentially free of residual organic solvent.
  • Forms I to XII and A, B1 , B2, C, D, E are disclosed in the references given above. The following preparations of forms which are essentially free of residual organic solvents can be applied to any form of Atorvastatin calcium.
  • the present invention is related to processes for the preparation of crystalline forms of atorvastatin calcium essentially free of residual organic solvent by exposing the crystalline form of atorvastatin calcium to an atmosphere with a defined relative air humidity.
  • a corresponding process for the preparation of Form F is preferred.
  • atorvastatin calcium essentially free of residual organic solvent can be prepared by exposure to an inert gas flow with a defined relative air humidity (to exchange residual organic solvent with water).
  • a corresponding process for the preparation of Form F is preferred.
  • Form F can be generally prepared essentially free of residual organic solvent by storage of this form in an atmosphere with a relative air humidity of 5 to 100%, preferably 40 to 80%, or by treating this form with a gas stream with a relative air humidity of 5 to 100%, preferably 40 to 80%.
  • compositions comprising an effective amount of crystalline polymorphic Form F, and a pharmaceutically acceptable carrier.
  • the polymorphic Form F may be used as single component or as mixtures with other polymorphic forms or the amorphous form of atorvastatin calcium.
  • Atorvastatin calcium it is preferred that it contains 25-100% by weight, especially 50- 100% by weight of the novel form, based on the total amount of Atorvastatin calcium.
  • an amount of the novel polymorphic form of Atorvastatin calcium is 75- 100% by weight, especially 90-100% by weight. Highly preferred is an amount of 95-100% by weight.
  • compositions of the present invention include powders, granulates, aggregates and other solid compositions comprising polymorphic Form F.
  • compositions that are contemplated by the present invention may further include diluents, such as cellulose-derived materials like powdered cellulose, microcrystalline cellulose, microfine cellulose, methyl cellulose, ethyl cellulose, hydroxyethyl cellulose, hydroxypropyl cellulose, hydroxypropylmethyl cellulose, carboxymethyl cellulose salts and other substituted and unsubstituted celluloses; starch; pregelatinized starch; inorganic diluents like calcium carbonate and calcium diphosphate and other diluents known to the pharmaceutical industry.
  • suitable diluents include waxes, sugars and sugar alcohols like mannitol and sorbitol, acrylate polymers and copolymers, as well as pectin, dextrin and gelatin.
  • excipients that are within the contemplation of the present invention include binders, such as acacia gum, pregelatinized starch, sodium alginate, glucose and other binders used in wet and dry granulation and direct compression tableting processes.
  • binders such as acacia gum, pregelatinized starch, sodium alginate, glucose and other binders used in wet and dry granulation and direct compression tableting processes.
  • Excipients that also may be present in the solid compositions further include disintegrants like sodium starch glycolate, crospovidone, low-substituted hydroxypropyl cellulose and others.
  • excipients may include tableting lubricants like magnesium and calcium stearate and sodium stearyl fumarate; flavorings; sweeteners; preservatives; pharmaceutically acceptable dyes and glidants such as silicon dioxide.
  • the dosages include dosages suitable for oral, buccal, rectal, parenteral (including subcutaneous, intramuscular, and intravenous), inhalant and ophthalmic administration.
  • parenteral including subcutaneous, intramuscular, and intravenous
  • inhalant and ophthalmic administration are examples of the most suitable route in any given case.
  • oral the most preferred route of the present invention is oral.
  • the dosages may be conveniently presented in unit dosage form and prepared by any of the methods well-known in the art of pharmacy.
  • Dosage forms include solid dosage forms, like tablets, powders, capsules, suppositories, sachets, troches and losenges as well as liquid suspensions and elixirs. While the description is not intended to be limiting, the invention is also not intended to pertain to true solutions of Atorvastatin calcium whereupon the properties that distinguish the solid form of Atorvastatin calcium are lost. However, the use of the novel form to prepare such solutions is considered to be within the contemplation of the invention.
  • Capsule dosages will contain the solid composition within a capsule which may be made of gelatin or other conventional encapsulating material.
  • Tablets and powders may be coated. Tablets and powders may be coated with an enteric coating.
  • the enteric coated powder forms may have coatings comprising phthalic acid cellulose acetate, hydroxypropylmethyl-cellulose phthalate, polyvinyl alcohol phthalate, carboxymethylethylcellulose, a copolymer of styrene and maleic acid, a copolymer of methacrylic acid and methyl methacrylate, and like materials, and if desired, they may be employed with suitable plasticizers and/or extending agents.
  • a coated tablet may have a coating on the surface of the tablet or may be a tablet comprising a powder or granules with an enteric coating.
  • Preferred unit dosages of the pharmaceutical compositions of this invention typically contain from 1 to 100 mg of the novel Atorvastatin calcium form or mixtures with other forms of Atorvastatin calcium (including the amorphous form). More usually, the combined weight of the Atorvastatin calcium forms of a unit dosage are from 5 mg to 80 mg, for example 10, 20 or 40 mg.
  • Atorvastatin calcium Form A 277 mg are added to 11 ml of a mixture of acetone and water (80:20 v/v). This suspension is stirred at ambient temperature for about ten minutes, leading to almost complete dissolution of Form A. When the resulting slightly turbid, opalescent solution is stirred at 40°C for about 14 hours, a white precipitate is formed. This precipitate is separated by filtration and dried at 60°C for 2 hours. Yield: 153 mg (55%). Analysis by powder X-ray diffraction shows that the obtained sample is Atorvastatin calcium Form F as shown in Figure 1. Karl Fischer titration of the sample after X-ray diffraction reveals a water content of 2.0 %.
  • Atorvastatin calcium Form A 303 mg are added to a mixture of 10 ml acetone and 1 ml of water. This mixture is stirred at ambient temperature for about 15 minutes which leads to almost complete dissolution of the solid. The slightly turbid, opalescent solution/suspension is stirred at 40°C for 22 hours. Within this time a thick precipitate is formed. This suspension is thoroughly stirred at 50°C for about 15 minutes, then the mixture is cooled to 20°C while stirring is continued for another 4 hours. Then the suspension is filtrated and dried at 80°C for 3 hours (300 mbar). An X-ray powder diffraction study shows the product to be polymorphic Form F.
  • Atorvastatin calcium Form I 500 mg are suspended in 15 ml of acetone and water mixture (80:20 v/v). This suspension is shortly stirred at 60°C giving a clear solution which becomes immediately turbid. This turbid suspension is stirred for an additional 16 hours at 40°C. The resulting precipitate is filtered, washed with 2 ml of the acetone/water mixture and dried for 1 hour at 50°C/800 mbar. Yield 400 mg (80%). An X-ray powder diffraction study shows the product to be polymorphic Form F.
  • Atorvastatin calcium Form F as obtained in example 4 was placed in a U-shaped glass tube in a oven at 60°C. This glass tube was purged with a nitrogen flow with a relative air humidity of ca. 50% for a period of 16 hours. Analysis by Karl Fischer titration reveals a water content of 2.5%, and analysis by GC-head space chromatography reveals an acetone content of less than 0.05%.
  • Atorvastatin calcium Form F as obtained in example 4 was placed in a desiccator over a saturated NaCI solution at room temperature, i.e. in an atmosphere with a relative air humidity of 75%, for 44 hours.
  • Analysis by Karl Fischer titration reveals a water content of 2.7%
  • analysis by GC-head space chromatography reveals an acetone content of less than 0.05%.
  • Further analysis by X-ray powder diffraction and i3 C CP-MAS solid state NMR spectroscopy shows that the crystal structure of Atorvastatin Form F was essentially retained under the given conditions, see Figures 3 and 4, respectively.
  • the X-ray source is operated at 45 kV and 45 mA. Spectra are recorded at a step size of 0.02° with a counting time of 2.4 seconds per step.
  • the accuracy of the 2 theta values of conventionally recorded powder X-ray diffraction patterns is generally +/- 0.2°.
  • about 40 mg of substance was prepared into circular shaped quartz sample holders of 0.5 mm depth and 10 mm width.
  • the 13 C CP-MAS solid state NMR spectra were recorded on a Bruker Avance-600 NMR spectrometer operating at 600 MHz proton resonance frequency. Samples were filled into 4 mm rotors without further pretreatment. Bruker xwinnmr version 3.1 was used to acquire the spectra. All spectra were recorded with variable-amplitude (linear ramp) cross polarization from the protons and using high-power proton decoupling (100 KHz field strength using the XiX decoupling scheme). The MAS frequency was set to 15 KHz and stabilized to within 5 Hz. 3072 transients with 4096 complex data points each (acquisition time 41 ms) were added.
  • the recycle delay was set to 3 sec leading to a measurement time of about 3 hours.
  • the data analysis was carried out using MATLAB version 6.5.
  • the first 200 complex data points of the acquired signal (FID) were Fourier transformed using a cosine-squared window function and zero filling to 32768 data points leading to an optimized signal-to-noise ratio and spectral resolution.
  • the digital resolution in the frequency domain is 1.53 Hz.
  • the spectra were referenced to an external standard using uniformly 13 C/ 15 N labeled alanine by setting the resonance frequency of the C ⁇ to 51.9 ppm. Under these measurement conditions and above described data evaluation the accuracy of the NMR shifts as presented is +/- 0.05 ppm.
  • Figure 1 is a characteristic X-ray powder diffraction pattern for Form F.
  • Figure 2 is a characteristic 13 C CP-MAS solid state NMR spectrum of Form F.
  • Figure 3 is a characteristic X-ray powder diffraction pattern for Form F essentially free of residual organic solvent.
  • Figure 4 is a characteristic 13 C CP-MAS solid state NMR spectrum of Form F essentially free of residual organic solvent.

Abstract

The present invention is directed to the novel polymorphic Form F of Atorvastatin calcium, processes for the preparation thereof and pharmaceutical compositions comprising this crystalline form.

Description

Crvstalline form
The present invention is directed to a crystalline form of Atorvastatin calcium, processes for the preparation thereof and pharmaceutical compositions comprising this crystalline form.
The present invention relates to a crystalline form of Atorvastatin calcium. Atorvastatin calcium is known by the chemical name, [R-(R*,R*)J-2-(4-fluorophenyl)-beta,delta-dihydroxy- 5-(1 -methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrroIe-1 -heptanoic acid calcium salt (2:1). Atorvastatin has the following formula:
Figure imgf000002_0001
Atorvastatin calcium is an orally-active hypocholesterolaemic, a liver-selective HMG-CoA reductase inhibitor. Processes for the preparation of Atorvastatin calcium are described in US-A-5,273,995, US-A-5,298,627, US-A-6,087,511 , US-A-6,274,740, WO-A-97/03960, WO- A-02/059087, WO-A-02/072073, and in the publications by P.L. Brower et al. in Tetrahedron Letters (1992), vol. 33, pages 2279-2282, K.L. Baumann et al. in Tetrahedron Letters (1992), vol. 33, pages 2283-2284 and A. Graul et al. in Drugs of the Future (1997), vol. 22, pages 956-968.
This calcium salt (2:1) is desirable since it enables Atorvastatin calcium to be conveniently formulated. The processes in the above mentioned patents and publications result in the preparation of amorphous Atorvastatin calcium.
The preparations of Atorvastatin calcium (2:1 ) described in WO-A-97/03958 and WO-A-97/03959 result in the isolation of crystalline Atorvastatin calcium with the polymorphic forms III, and I, II, and IV, respectively. WO-A-01/36384, WO-A-02/41834 and WO-A- 02/43732 claim the preparation of crystalline Atorvastatin calcium with the polymorphic forms V to XII, whereas WO-A-02/051804 claims the polymorphic forms A, B1 , B2, C, D and E. However, there is still a need to produce Atorvastatin calcium in a reproducible, pure and crystalline form to enable formulations to meet exacting pharmaceutical requirements and specifications. Furthermore, it is economically desirable that the product is stable for extended periods of time without the need for specialized storage conditions.
Surprisingly, there has now been found a novel crystalline form of Atorvastatin calcium salt (2:1), herein designated as Form F. This novel form of the present invention can be prepared in ecological friendly solvents and has a good thermal stability combined with good solubility characteristics.
Accordingly, the present invention is directed to the polymorphic Form F of Atorvastatin calcium salt (2:1 ).
Therefore, the present invention is directed to a crystalline polymorph F of [R-(R*,R*)]-2-(4- fluorophenyl)-beta,delta-dihydroxy-5-(1-methylethyl)-3-phenyl-4-[(phenylamino)carbonyI]-1 H- pyrrole-1 -heptanoic acid calcium salt (2:1) which exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d-values (A) at 24.3 (s), 10.2 (s), 8.6 (s), 4.57 (vs), 4.26 (m); wherein (vs) = very strong intensity; (s) = strong intensity; (m) = medium intensity.
More particularly, the crystalline polymorph F exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d-values (A) at
32.3 (w), 24.3 (s), 16.5 (m), 13.0 (w), 11.4 (m), 10.2 (s), 8.6 (s), 7.0 (m), 6.4 (m), 5.16 (m),
4.96 (m), 4.57 (vs), 4.26 (m), 3.95 (m), 3.67 (m), 3.48 (m), 3.20 (w).
The abbreviations in brackets mean: (vs) = very strong intensity; (s) = strong intensity;
(m) = medium intensity; (w) = weak intensity.
Especially, the crystalline polymorph F exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d-values (A) and in 2Θ as given in Table 1 (vs = very strong intensity, s = strong intensity, m = medium intensity, w = weak intensity). Table 1 : d-spacings and 2Θ angles for Form F.
Figure imgf000004_0001
The polymorphic Form F of Atorvastatin calcium is especially characterized by a powder X- ray diffraction pattern substantially as depicted in Figure 1.
Furthermore, the crystalline polymorph F exhibits a characteristic 13C CP-MAS solid state NMR spectrum with chemical shifts (in parts per million, with peak intensity in arbitrary units in brackets) at 188.2 (2.5), 184.3 (2.2), 177.4 (2.8), 167.5 (2.9), 162.6 (2.4), 161.0 (3.9), 139.8 (6.5), 138.2 (4.3), 135.8 (5.1), 134.1 (4.0), 132.0 (8.4), 131.2 (7.3), 130.5 (14.0), 129.0 (9.5), 128.0 (6.6), 127.2 (4.6), 125.5 (2.9), 124.0 (4.9), 123.5 (4.7), 122.8 (4.8), 122.1 (6.2), 120.7 (5.4), 117.6 (4.1), 116.6 (4.1), 115.2 (3.6), 112.8 (1.6), 72.9 (4.8), 71.7 (5.2), 69.4 (6.5), 67.1 (4.9), 63.2 (0.7), 46.3 (10.4), 44.1 (12.6), 40.6 (7.6), 36.4 (0.7), 32.1 (3.8), 31.1 (1.3), 28.2 (5.3), 27.4 (9.0), 25.8 (11.2), 22.5 (3.7), 20.9 (4.2), 20.0 (4.8).
The polymorphic Form F of Atorvastatin calcium is especially characterized by a 13C CP- MAS solid state NMR spectrum as depicted in Figure 2. Furthermore, the present invention is directed to processes for the preparation of Form F of Atorvastatin calcium.
Form F can generally be prepared by adding Form A to a ketone solvent, especially acetone. It is preferred that the ketone solvent contains as a further solvent some water. The amount of water is preferably about 1 to 30%, more preferably about 5 to 20%, especially about 10 to 20% by volume of the suspension. It is preferred that the suspension is treated at temperatures between 10 and 60°C, preferably at temperatures of 20 to 40°C, especially for a longer periods of time, like 10 to 40 hours. It is further preferred that nucleation of Form F is induced at a temperature of 40 to 60°C, especially at about 60°C, and subsequent ripening and equilibration is performed at temperatures between 20 and 40°C. If desired, during the preparation process seeding with Form F can be carried out. Form F can, for example, be isolated by filtration and dried in air or in vacuum. The above mentioned process can also be carried out using another crystalline form or the amorphous form of atorvastatin calcium. Examples of other crystalline forms are Forms I, II, III, IV, V, VI, VII, VIII, IX, X, XI, XII, A, B1 , B2, C, D and E, which are disclosed and characterized in the references given hereinbefore. Preferred forms for this purpose are Form A (see for example WO-A-02/051804; last but one paragraph of page 2; page 4, last but one paragraph to page 5, first paragraph; Examples 2, 8 and 9; Fig. 2) or Form I (see for example WO-A-97/03959; table on page 4; page 20, line 9 to page 22, line 11 ; Example 1 ; Fig. 1 ). As to Form B1 see for example WO-A-02/051804; the paragraph bridging pages 2 and 3; page 5, second paragraph; Example 3; and Fig. 3). As to Form B2 see for example WO-A-02/051804; page 3, second paragraph; page 5, third paragraph; Example 4; and Fig. 3.
Form F can also be prepared from Atorvastatin lactone upon subsequent reaction with NaOH to form Atorvastatin sodium followed by reaction with CaCI2 in a ketone solvent, especially in acetone. It is preferred that the ketone solvent contains as a further solvent some water. The amount of water is preferably about 1 to 30%. If desired, during the preparation process seeding with Form F can be carried out.
Form F can also be prepared directly from Atorvastatin lactone upon reaction with a calcium(ll) salt, like Ca(OH)2 or Ca(OAc)2, in a ketone solvent, especially in acetone. It is preferred that the ketone solution contains as a further solvent some water. The amount of water is preferably about 1 to 30%. If desired, during the preparation process seeding with Form F can be carried out.
Form F can also be prepared by adding a concentrated solution of Atorvastatin calcium in an organic solvent, like tetrahydrofuran, to a ketone solvent, especially acetone. It is preferred that the ketone solution contains as a further solvent some water. The amount of water is preferably about 1 to 30%. If desired, during the preparation process seeding with Form F can be carried out.
As to the ketone solvent of the preparation processes given above it is preferred to use C3- C8ketones, especially acetone.
Another object of the present invention are crystalline forms of atorvastatin calcium which are essentially free of residual organic solvent. Preferred are Forms I to XII and A, B1 , B2, C, D, E and F which are essentially free of residual organic solvent. Highly preferred are Forms B1 , B2 and F, especially Form F. Forms I to XII and A, B1 , B2, C, D, E are disclosed in the references given above. The following preparations of forms which are essentially free of residual organic solvents can be applied to any form of Atorvastatin calcium. It is preferred that the crystalline forms contain less than 0.5% by weight of residual organic solvent. Highly preferred are amounts of residual organic solvents of less than 5000 ppm, especially less than 2000 ppm. Most preferred are amounts of residual organic solvents of less than 400 ppm, especially less than 200 ppm. Examples of such residual organic solvents are aceton, ethylacetate, tetrahydrofuran, ethanol, methanol, acetonitrile and hexane.
Therefore, the present invention is directed to a crystalline polymorph F of [R-(R*,R*)]-2-(4- fluorophenyl)-beta,delta-dihydroxy-5-(1-methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H- pyrrole-1-heptanoic acid calcium salt (2:1) which is essentially free of residual organic solvents and which exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d-values (A) at 24.3 (s), 10.2 (s), 8.7 (s), 4.80 (m), 4.56 (vs), 4.00 (m), 3.72 (m); wherein (vs) = very strong intensity; (s) = strong intensity; (m) = medium intensity.
More particularly, the crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta- dihydroxy-5-(1 -methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) which is essentially free of residual organic solvents exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d- values (A) at 31.9 (w), 24.3 (s), 16.3 (w), 13.1 (vw), 12.1 (w), 11.4 (m), 10.2 (s), 8.7 (s), 8.1 (vw), 7.1 (w), 6.9 (w), 6.5 (m), 5.98 (vw), 5.60 (vw), 5.21 (m), 5.00 (m), 4.80 (m), 4.56 (vs), 4.32 (w), 4.23 (m), 4.00 (m), 3.72 (m), 3.48 (m); wherein (vs) = very strong intensity; (s) = strong intensity; (m) = medium intensity; (w) = weak intensity; (vw) = very weak intensity.
The crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1- methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) which is essentially free of residual organic solvents is especially characterized by an X-ray powder diffraction pattern substantially as depicted in figure 3.
Furthermore, the crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta- dihydroxy-5-(1 -methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1 ) which is essentially free of residual organic solvents exhibits a characteristic 13C CP-MAS solid state NMR spectrum with chemical shifts (in parts per million, with peak intensity in arbitrary units in brackets) at 187.7 (1.3), 184.6 (1.7), 177.7 (2.5), 167.5 (3.4), 162.8 (1.7), 161.1 (3.0), 143.6 (1.3), 140.0 (3.3), 139.3 (3.7), 138.0 (4.0), 137.1 (3.4), 136.0 (5.7), 134.1 (8.8), 132.0 (8.7), 131.3 (8.5), 130.2 (13.3), 129.5 (14.0), 127.9 (9.6), 126.8 (3.6), 125.3 (4.4), 123.1 (8.5), 120.5 (3.8), 117.5 (4.5), 115.3 (4.9), 112.8 (1.1 ), 72.7 (3.9), 71.5 (6.2), 69.3 (9.3), 67.2 (5.8), 46.3 (11.3), 44.4 (12.4), 41.3 (6.2), 40.6 (7.2), 34.7 (0.9), 32.0 (1.4), 30.8 (1.4), 28.2 (6.5), 27.3 (9.5), 25.9 (7.8), 21.1 (4.2), 20.3 (4.3).
The crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1- methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) which is essentially free of residual organic solvents is especially characterized by a 13C CP-MAS solid state NMR spectrum substantially as depicted in figure 4.
It is preferred that the crystalline polymorphs F have a water content of up to 5% by weight (independently whether the polymorphs are essentially free of residual organic solvents or not). Another object of the present invention are processes for the preparation of crystalline forms of atorvastatin calcium which are essentially free of residual organic solvent. Preferred are processes for the preparation of Forms I to XII and A, B1 , B2, C, D, E and F which are essentially free of residual organic solvent. Highly preferred are processes for the preparation of Forms B1 , B2 and F, especially Form F, which are essentially free of residual organic solvent. Forms I to XII and A, B1 , B2, C, D, E are disclosed in the references given above. The following preparations of forms which are essentially free of residual organic solvents can be applied to any form of Atorvastatin calcium.
Particularly, the present invention is related to processes for the preparation of crystalline forms of atorvastatin calcium essentially free of residual organic solvent by exposing the crystalline form of atorvastatin calcium to an atmosphere with a defined relative air humidity. A relative air humidity of 5 to 100%, especially 40 to 80%, is preferred. A corresponding process for the preparation of Form F is preferred.
More particularly, atorvastatin calcium essentially free of residual organic solvent can be prepared by exposure to an inert gas flow with a defined relative air humidity (to exchange residual organic solvent with water). A relative air humidity of 5 to 100%, especially 40 to 80%, is preferred. A corresponding process for the preparation of Form F is preferred.
For example, Form F can be generally prepared essentially free of residual organic solvent by storage of this form in an atmosphere with a relative air humidity of 5 to 100%, preferably 40 to 80%, or by treating this form with a gas stream with a relative air humidity of 5 to 100%, preferably 40 to 80%.
The powder X-ray diffraction pattern as well as the 13C CP-MAS solid state NMR spectrum of Form F essentially free of residual organic solvent may appear with slight deviations as compared to Form F containing residual organic solvent, compare Figure 3 and Figure 4 with Figure 1 and Figure 2, respectively.
Another object of the present invention are pharmaceutical compositions comprising an effective amount of crystalline polymorphic Form F, and a pharmaceutically acceptable carrier. The polymorphic Form F may be used as single component or as mixtures with other polymorphic forms or the amorphous form of atorvastatin calcium.
As to Atorvastatin calcium it is preferred that it contains 25-100% by weight, especially 50- 100% by weight of the novel form, based on the total amount of Atorvastatin calcium. Preferably, such an amount of the novel polymorphic form of Atorvastatin calcium is 75- 100% by weight, especially 90-100% by weight. Highly preferred is an amount of 95-100% by weight.
The compositions of the present invention include powders, granulates, aggregates and other solid compositions comprising polymorphic Form F. In addition, the compositions that are contemplated by the present invention may further include diluents, such as cellulose-derived materials like powdered cellulose, microcrystalline cellulose, microfine cellulose, methyl cellulose, ethyl cellulose, hydroxyethyl cellulose, hydroxypropyl cellulose, hydroxypropylmethyl cellulose, carboxymethyl cellulose salts and other substituted and unsubstituted celluloses; starch; pregelatinized starch; inorganic diluents like calcium carbonate and calcium diphosphate and other diluents known to the pharmaceutical industry. Yet other suitable diluents include waxes, sugars and sugar alcohols like mannitol and sorbitol, acrylate polymers and copolymers, as well as pectin, dextrin and gelatin.
Further excipients that are within the contemplation of the present invention include binders, such as acacia gum, pregelatinized starch, sodium alginate, glucose and other binders used in wet and dry granulation and direct compression tableting processes. Excipients that also may be present in the solid compositions further include disintegrants like sodium starch glycolate, crospovidone, low-substituted hydroxypropyl cellulose and others. In addition, excipients may include tableting lubricants like magnesium and calcium stearate and sodium stearyl fumarate; flavorings; sweeteners; preservatives; pharmaceutically acceptable dyes and glidants such as silicon dioxide.
The dosages include dosages suitable for oral, buccal, rectal, parenteral (including subcutaneous, intramuscular, and intravenous), inhalant and ophthalmic administration. Although the most suitable route in any given case will depend on the nature and severity of the condition being treated, the most preferred route of the present invention is oral. The dosages may be conveniently presented in unit dosage form and prepared by any of the methods well-known in the art of pharmacy.
Dosage forms include solid dosage forms, like tablets, powders, capsules, suppositories, sachets, troches and losenges as well as liquid suspensions and elixirs. While the description is not intended to be limiting, the invention is also not intended to pertain to true solutions of Atorvastatin calcium whereupon the properties that distinguish the solid form of Atorvastatin calcium are lost. However, the use of the novel form to prepare such solutions is considered to be within the contemplation of the invention.
Capsule dosages, of course, will contain the solid composition within a capsule which may be made of gelatin or other conventional encapsulating material. Tablets and powders may be coated. Tablets and powders may be coated with an enteric coating. The enteric coated powder forms may have coatings comprising phthalic acid cellulose acetate, hydroxypropylmethyl-cellulose phthalate, polyvinyl alcohol phthalate, carboxymethylethylcellulose, a copolymer of styrene and maleic acid, a copolymer of methacrylic acid and methyl methacrylate, and like materials, and if desired, they may be employed with suitable plasticizers and/or extending agents. A coated tablet may have a coating on the surface of the tablet or may be a tablet comprising a powder or granules with an enteric coating.
Preferred unit dosages of the pharmaceutical compositions of this invention typically contain from 1 to 100 mg of the novel Atorvastatin calcium form or mixtures with other forms of Atorvastatin calcium (including the amorphous form). More usually, the combined weight of the Atorvastatin calcium forms of a unit dosage are from 5 mg to 80 mg, for example 10, 20 or 40 mg.
The following Examples illustrate the invention in more detail. Temperatures are given in degrees Celsius.
Example 1 :
277 mg of Atorvastatin calcium Form A are added to 11 ml of a mixture of acetone and water (80:20 v/v). This suspension is stirred at ambient temperature for about ten minutes, leading to almost complete dissolution of Form A. When the resulting slightly turbid, opalescent solution is stirred at 40°C for about 14 hours, a white precipitate is formed. This precipitate is separated by filtration and dried at 60°C for 2 hours. Yield: 153 mg (55%). Analysis by powder X-ray diffraction shows that the obtained sample is Atorvastatin calcium Form F as shown in Figure 1. Karl Fischer titration of the sample after X-ray diffraction reveals a water content of 2.0 %.
Example 2:
303 mg of Atorvastatin calcium Form A are added to a mixture of 10 ml acetone and 1 ml of water. This mixture is stirred at ambient temperature for about 15 minutes which leads to almost complete dissolution of the solid. The slightly turbid, opalescent solution/suspension is stirred at 40°C for 22 hours. Within this time a thick precipitate is formed. This suspension is thoroughly stirred at 50°C for about 15 minutes, then the mixture is cooled to 20°C while stirring is continued for another 4 hours. Then the suspension is filtrated and dried at 80°C for 3 hours (300 mbar). An X-ray powder diffraction study shows the product to be polymorphic Form F.
Example 3:
500 mg of Atorvastatin calcium Form I are suspended in 15 ml of acetone and water mixture (80:20 v/v). This suspension is shortly stirred at 60°C giving a clear solution which becomes immediately turbid. This turbid suspension is stirred for an additional 16 hours at 40°C. The resulting precipitate is filtered, washed with 2 ml of the acetone/water mixture and dried for 1 hour at 50°C/800 mbar. Yield 400 mg (80%). An X-ray powder diffraction study shows the product to be polymorphic Form F.
Example 4:
1.58 g of Atorvastatin calcium Form A are suspended in 44.2 g of a mixture of acetone and water (80:20), heated to 60°C and stirred for 3 hours. The white suspension formed is slowly cooled to 40°C, stirred for an additional 18 hours, slowly cooled to 20°C and stirred for an additional 2 hours. The suspension was filtered and dried at ambient temperatures with dry nitrogen. Yield 1.192 g. An X-ray powder diffraction study shows the product to be polymorphic Form F. Further analysis by 13C CP-MAS solid state NMR spectroscopy reveals a solid state NMR spectrum as shown in Figure 2. analysis by Karl Fischer titration reveals a water content of 1.3%, and analysis by GC-head space chromatography reveals an acetone content of 0.7%. Example 5:
250 mg of Atorvastatin calcium Form F as obtained in example 4 was placed in a U-shaped glass tube in a oven at 60°C. This glass tube was purged with a nitrogen flow with a relative air humidity of ca. 50% for a period of 16 hours. Analysis by Karl Fischer titration reveals a water content of 2.5%, and analysis by GC-head space chromatography reveals an acetone content of less than 0.05%.
Example 6:
250 mg of Atorvastatin calcium Form F as obtained in example 4 was placed in a desiccator over a saturated NaCI solution at room temperature, i.e. in an atmosphere with a relative air humidity of 75%, for 44 hours. Analysis by Karl Fischer titration reveals a water content of 2.7%, and analysis by GC-head space chromatography reveals an acetone content of less than 0.05%. Further analysis by X-ray powder diffraction and i3C CP-MAS solid state NMR spectroscopy shows that the crystal structure of Atorvastatin Form F was essentially retained under the given conditions, see Figures 3 and 4, respectively.
X-ray powder diffraction measurements were performed on a Philips 1710 powder X-ray diffractometer using Cu Kα radiation (Cu Kc^ and Cu K 2 at a ratio of 2, λ of Cu Kα! = 1.54060, and λ of Cu K 2 = 1.54447). The X-ray source is operated at 45 kV and 45 mA. Spectra are recorded at a step size of 0.02° with a counting time of 2.4 seconds per step. The accuracy of the 2 theta values of conventionally recorded powder X-ray diffraction patterns is generally +/- 0.2°. For sample preparation, about 40 mg of substance was prepared into circular shaped quartz sample holders of 0.5 mm depth and 10 mm width. The 13C CP-MAS solid state NMR spectra were recorded on a Bruker Avance-600 NMR spectrometer operating at 600 MHz proton resonance frequency. Samples were filled into 4 mm rotors without further pretreatment. Bruker xwinnmr version 3.1 was used to acquire the spectra. All spectra were recorded with variable-amplitude (linear ramp) cross polarization from the protons and using high-power proton decoupling (100 KHz field strength using the XiX decoupling scheme). The MAS frequency was set to 15 KHz and stabilized to within 5 Hz. 3072 transients with 4096 complex data points each (acquisition time 41 ms) were added. The recycle delay was set to 3 sec leading to a measurement time of about 3 hours. The data analysis was carried out using MATLAB version 6.5. The first 200 complex data points of the acquired signal (FID) were Fourier transformed using a cosine-squared window function and zero filling to 32768 data points leading to an optimized signal-to-noise ratio and spectral resolution. The digital resolution in the frequency domain is 1.53 Hz. The spectra were referenced to an external standard using uniformly 13C/15N labeled alanine by setting the resonance frequency of the Cα to 51.9 ppm. Under these measurement conditions and above described data evaluation the accuracy of the NMR shifts as presented is +/- 0.05 ppm.
Brief description of the drawing
Figure 1 is a characteristic X-ray powder diffraction pattern for Form F.
Figure 2 is a characteristic 13C CP-MAS solid state NMR spectrum of Form F.
Figure 3 is a characteristic X-ray powder diffraction pattern for Form F essentially free of residual organic solvent.
Figure 4 is a characteristic 13C CP-MAS solid state NMR spectrum of Form F essentially free of residual organic solvent.

Claims

Claims
1. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1 - methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) which exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d-values (A) at 24.3 (s), 10.2 (s), 8.6 (s), 4.57 (vs), 4.26 (m); wherein (vs) = very strong intensity; (s) = strong intensity; (m) = medium intensity.
2. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1 - methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) which exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d-values (A) at 32.3 (w), 24.3 (s), 16.5 (m), 13.0 (w), 11.4 (m), 10.2 (s), 8.6 (s), 7.0 (m), 6.4 (m), 5.16 (m), 4.96 (m), 4.57 (vs), 4.26 (m), 3.95 (m), 3.67 (m), 3.48 (m), 3.20 (w); wherein (vs) = very strong intensity; (s) = strong intensity; (m) = medium intensity; (w) = weak intensity.
3. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1 - methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1 ) having an X-ray powder diffraction pattern substantially as depicted in figure 1.
4. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1- methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1 ) which exhibits a characteristic 13C CP-MAS solid state NMR spectrum with chemical shifts (in parts per million, with peak intensity in arbitrary units in brackets) at 188.2 (2.5), 184.3 (2.2), 177.4 (2.8), 167.5 (2.9), 162.6 (2.4), 161.0 (3.9), 139.8 (6.5), 138.2 (4.3), 135.8 (5.1), 134.1 (4.0), 132.0 (8.4), 131.2 (7.3), 130.5 (14.0), 129.0 (9.5), 128.0 (6.6), 127.2 (4.6), 125.5 (2.9), 124.0 (4.9), 123.5 (4.7), 122.8 (4.8), 122.1 (6.2), 120.7 (5.4), 117.6 (4.1), 116.6 (4.1 ), 115.2 (3.6), 112.8 (1.6), 72.9 (4.8), 71.7 (5.2), 69.4 (6.5), 67.1 (4.9), 63.2 (0.7), 46.3 (10.4), 44.1 (12.6), 40.6 (7.6), 36.4 (0.7), 32.1 (3.8), 31.1 (1.3), 28.2 (5.3), 27.4 (9.0), 25.8 (11.2), 22.5 (3.7), 20.9 (4.2), 20.0 (4.8).
5. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1- methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) having a 13C CP-MAS solid state NMR spectrum substantially as depicted in figure 2.
6. A crystalline polymorph of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1- methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) which is essentially free of residual organic solvents.
7. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1- methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1 ) which is essentially free of residual organic solvents.
8. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1 - methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) essentially free of residual organic solvents which exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d-values (A) at 24.3 (s),
10.2 (s), 8.7 (s), 4.80 (m), 4.56 (vs), 4.00 (m), 3.72 (m); wherein (vs) = very strong intensity; (s) = strong intensity; (m) = medium intensity.
9. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1 - methyIethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) essentially free of residual organic solvents which exhibits a characteristic X-ray powder diffraction pattern with characteristic peaks expressed in d-values (A) at 31.9 (w),
24.3 (s), 16.3 (w), 13.1 (vw), 12.1 (w), 11.4 (m), 10.2 (s), 8.7 (s), 8.1 (vw), 7.1 (w), 6.9 (w), 6.5 (m), 5.98 (vw), 5.60 (vw), 5.21 (m), 5.00 (m), 4.80 (m), 4.56 (vs), 4.32 (w), 4.23 (m), 4.00 (m), 3.72 (m), 3.48 (m); wherein (vs) = very strong intensity; (s) = strong intensity; (m) = medium intensity; (w) = weak intensity; (vw) = very weak intensity.
10. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1- methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1 ) essentially free of residual organic solvents having an X-ray powder diffraction pattern substantially as depicted in figure 3.
11. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1 - methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) essentially free or residual organic solvents which exhibits a characteristic 13C CP-MAS solid state NMR spectrum with chemical shifts (in parts per million, with peak intensity in arbitrary units in brackets) at 187.7 (1.3), 184.6 (1.7), 177.7 (2.5), 167.5 (3.4), 162.8 (1.7), 161.1 (3.0), 143.6 (1.3), 140.0 (3.3), 139.3 (3.7), 138.0 (4.0), 137.1 (3.4), 136.0 (5.7), 134.1 (8.8), 132.0 (8.7), 131.3 (8.5), 130.2 (13.3), 129.5 (14.0), 127.9 (9.6), 126.8 (3.6), 125.3 (4.4), 123.1 (8.5), 120.5 (3.8), 117.5 (4.5), 115.3 (4.9), 112.8 (1.1), 72.7 (3.9), 71.5 (6.2), 69.3 (9.3), 67.2 (5.8), 46.3 (11.3), 44.4 (12.4), 41.3 (6.2), 40.6 (7.2), 34.7 (0.9), 32.0 (1.4), 30.8 (1.4), 28.2 (6.5), 27.3 (9.5), 25.9 (7.8), 21.1 (4.2), 20.3 (4.3).
12. A crystalline polymorph F of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1- methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) essentially free of residual organic solvents having a 13C CP-MAS solid state NMR spectrum substantially as depicted in figure 4.
13. A crystalline polymorph of [R-(R*,R*)]-2-(4-fluorophenyl)-beta,delta-dihydroxy-5-(1- methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 -heptanoic acid calcium salt (2:1) according to any of claims 6 to 12 having a water content up to 5%.
14. A process for the preparation of a crystalline polymorph according to any of claims 1 to 13, wherein Atorvastatin calcium is added to a ketone solvent at temperatures between 10 and 60°C.
15. A process according to claim 14 in which Atorvastatin calcium Form A is used.
16. A process according to claim 14 in which the ketone is acetone.
17. A process according to claim 14 in which the ketone contains 1 to 30% water.
18. A process according to any of claims 14 to 17, wherein seeding is carried out with crystals of the crystalline polymorph according to any of claims 1 to 13.
19. A process for the preparation of a crystalline polymorph according to any of claims 1 to 13, wherein Atorvastatin lactone in a ketone solvent is subsequently reacted with NaOH to form Atorvastatin sodium and then with CaCI2.
20. A process according to claim 19 in which the ketone is acetone.
21. A process according to claim 19 in which the ketone contains 1 to 30% water.
22. A process according to any of claims 19 to 21 , wherein seeding is carried out with crystals of the crystalline polymorph according to any of claims 1 to 13.
23. A process for the preparation of a crystalline polymorph according to any of claims 1 to 13, wherein Atorvastatin lactone in a ketone solvent is reacted with a calcium(ll) salt, preferably Ca(OH)2 or Ca(OAc)2.
24. A process according to claim 23 in which the ketone is acetone.
25. A process according to claim 23 in which the ketone contains 1 to 30% water.
26. A process according to any of claims 23 to 25, wherein seeding is carried out with crystals of the crystalline polymorph according to any of claims 1 to 13.
27. A process for the preparation of a crystalline polymorph according to any of claims 1 to 13, wherein a concentrated solution of Atorvastatin calcium in an organic solvent is added to a ketone solvent.
28. A process according to claim 27 in which the ketone is acetone, and the organic solvent is tetrahydrofuran.
29. A process according to claim 27 in which the ketone contains 1 to 30% water.
30. A process according to any of claims 27 to 29, wherein seeding is carried out with crystals of the crystalline polymorph according to any of claims 1 to 13.
31. A process for the preparation of any crystalline form of [R-(R*,R*)]-2-(4-fluorophenyl)- beta,delta-dihydroxy-5-(1 -methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 - heptanoic acid calcium salt (2:1) essentially free of residual organic solvents by exposing the organic solvent containing crystalline form to an atmosphere with a relative air humidity of 5 to 100%.
32. A process for the preparation of any crystalline form of [R-(R*,R*)]-2-(4-fluorophenyl)- beta,delta-dihydroxy-5-(1 -methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 - heptanoic acid calcium salt (2:1) essentially free of residual organic solvents by equilibrating the organic solvent containing crystalline form in an inert gas flow with a relative air humidity of 5 to 100%.
33. A process according to claim 31 or 32 in which the relative air humidity is 40 to 80%.
34. A process for the preparation of crystalline form F of [R-(R*,R*)]-2-(4-fluorophenyl)- beta,delta-dihydroxy-5-(1 -methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 - heptanoic acid calcium salt (2:1) essentially free of residual organic by exposing the organic solvent containing crystalline form F to an atmosphere with a relative air humidity of 5 to 100%.
35. A process for the preparation of crystalline form F of [R-(R*,R*)]-2-(4-fluorophenyl)- beta,delta-dihydroxy-5-(1 -methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 - heptanoic acid calcium salt (2:1) essentially free of residual organic solvents by equilibrating the organic solvent containing form F in an inert gas flow with a relative air humidity of 5 to 100%.
36. A process for the preparation of crystalline form F of [R-(R*,R*)]-2-(4-fluorophenyl)- beta,delta-dihydroxy-5-(1 -methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1 H-pyrrole-1 - heptanoic acid calcium salt (2:1) essentially free of residual organic solvents by equilibrating the organic solvent containing form F in a closed system under an atmosphere with a relative air humidity of 5 to 100%.
37. A process according to any of claims 34 to 36 in which the relative air humidity is 40 to 80%.
8. A pharmaceutical composition comprising an effective amount of a crystalline polymorphic form according to any of claims 1 to 13, and a pharmaceutically acceptable carrier.
PCT/US2003/038090 2002-11-28 2003-11-26 Crystalline form f of atorvastatin hemi-calcium salt WO2004050618A2 (en)

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EP1465865A2 (en) * 2002-11-12 2004-10-13 Teva Pharmaceutical Industries Limited Novel crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
EP1480950A1 (en) * 2002-02-15 2004-12-01 Teva Pharmaceutical Industries Ltd. Novel crystal forms of atorvastatin hemi-calcium and processes for their preparation, as well as novel processes for preparing atorvastatin hemi-calcium forms i, viii and ix
US6992194B2 (en) 2000-11-30 2006-01-31 Teva Pharmaceutical Industries, Ltd. Crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
WO2006011041A2 (en) * 2004-07-20 2006-02-02 Warner-Lambert Company Llc Crystalline forms of (r-(r*))-2-(4-fluorophenyl)-beta, gamma-dihydroxy-5-(1-methylethyl)-3-phenyl-4-((phenylamino)carbonyl)-1h-pyrrole-1-hept anoic acid calcium salt (2:1)
WO2006012499A2 (en) * 2004-07-22 2006-02-02 Teva Pharmaceutical Industries Ltd. Novel crystal forms of atorvastatin hemi-calcium and processes for their preparation
WO2006037125A1 (en) * 2004-09-28 2006-04-06 Teva Pharmaceutical Industries Ltd. Process for preparing forms of atorvastatin calcium substantially free of impurities
WO2006048894A1 (en) * 2004-11-05 2006-05-11 Morepen Laboratories Limited Novel crystalline forms of atorvastatin calcium and processes for preparing them.
WO2008002655A2 (en) * 2006-06-28 2008-01-03 Teva Pharmaceutical Industries Ltd. Crystalline forms of atorvastatin
US7411075B1 (en) 2000-11-16 2008-08-12 Teva Pharmaceutical Industries Ltd. Polymorphic form of atorvastatin calcium
WO2009007856A2 (en) * 2007-07-11 2009-01-15 Actavis Group Ptc Ehf Novel polymorph of atorvastatin calcium and use thereof for the preparation of amorphous atorvastatin calcium
EP2132171A1 (en) * 2007-03-02 2009-12-16 Dong-A Pharm.Co., Ltd. Novel crystal forms of pyrrolylheptanoic acid derivatives
US20100056605A1 (en) * 2004-07-16 2010-03-04 Lek Pharmaceuticals D.D. Oxidative degradation products of atorvastatin calcium
US8080672B2 (en) 2005-12-13 2011-12-20 Teva Pharmaceutical Industries Ltd. Crystal form of atorvastatin hemi-calcium and processes for preparation thereof
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US7732623B2 (en) 1999-11-17 2010-06-08 Teva Pharmaceutical Industries Ltd. Polymorphic form of atorvastatin calcium
US7411075B1 (en) 2000-11-16 2008-08-12 Teva Pharmaceutical Industries Ltd. Polymorphic form of atorvastatin calcium
US7456297B2 (en) 2000-11-30 2008-11-25 Teva Pharmaceutical Industries Ltd. Crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
US7161012B2 (en) 2000-11-30 2007-01-09 Teva Pharmaceutical Industries Ltd. Processes for preparing amorphous atorvastatin hemi-calcium
US7256212B2 (en) 2000-11-30 2007-08-14 Teva Pharmaceutical Industries Ltd. Crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
US6992194B2 (en) 2000-11-30 2006-01-31 Teva Pharmaceutical Industries, Ltd. Crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
US7189861B2 (en) 2000-11-30 2007-03-13 Teva Pharmaceutical Industries, Ltd. Processes for preparing amorphous atorvastatin hemi-calcium
US7488750B2 (en) 2000-11-30 2009-02-10 Teva Pharmaceutical Industries Ltd. Crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
US7501450B2 (en) 2000-11-30 2009-03-10 Teva Pharaceutical Industries Ltd. Crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
US7468444B2 (en) 2000-11-30 2008-12-23 Teva Pharmaceutical Industries Ltd. Crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
US7144916B2 (en) 2000-11-30 2006-12-05 Teva Pharmaceutical Industries Ltd. Crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
US7151183B2 (en) 2000-11-30 2006-12-19 Teva Pharmaceutical Industries Ltd. Processes for preparing amorphous atorvastatin hemi-calcium
US7342120B2 (en) 2000-11-30 2008-03-11 Teva Pharmaceutical Industries, Ltd. Crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
EP1480950A1 (en) * 2002-02-15 2004-12-01 Teva Pharmaceutical Industries Ltd. Novel crystal forms of atorvastatin hemi-calcium and processes for their preparation, as well as novel processes for preparing atorvastatin hemi-calcium forms i, viii and ix
EP1480950A4 (en) * 2002-02-15 2005-05-18 Teva Pharma Novel crystal forms of atorvastatin hemi-calcium and processes for their preparation, as well as novel processes for preparing atorvastatin hemi-calcium forms i, viii and ix
EP1465865A2 (en) * 2002-11-12 2004-10-13 Teva Pharmaceutical Industries Limited Novel crystal forms of atorvastatin hemi-calcium and processes for their preparation as well as novel processes for preparing other forms
US20100056605A1 (en) * 2004-07-16 2010-03-04 Lek Pharmaceuticals D.D. Oxidative degradation products of atorvastatin calcium
WO2006011041A3 (en) * 2004-07-20 2006-06-22 Warner Lambert Co Crystalline forms of (r-(r*))-2-(4-fluorophenyl)-beta, gamma-dihydroxy-5-(1-methylethyl)-3-phenyl-4-((phenylamino)carbonyl)-1h-pyrrole-1-hept anoic acid calcium salt (2:1)
US8026376B2 (en) 2004-07-20 2011-09-27 Pfizer, Inc. Forms of [R-(R*,R*)]-2-(4-fluorophenyl)-β,δ-dihydroxy-5-(1-methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1H-pyrrole-1-heptanoicacid calcium salt (2:1)
US8563750B2 (en) 2004-07-20 2013-10-22 Warner-Lambert Company Llc Forms of [R-(R*,R*)]-2-(4-fluorophenyl)-β,δ-dihydroxy-5-(1-methylethyl)-3-phenyl-4-[(phenylmino)carbonyl]-1H-pyrrole-1-heptanoic acid calcium salt (2:1)
US8895758B2 (en) 2004-07-20 2014-11-25 Warner-Lambert Company Llc Forms of [R-(R*,R*)]-2-(4-fluorophenyl)-β, δ-Dihydroxy-5-(1-methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1H-pyrrole-1-heptanoic acid calcium salt (2:1)
US9199932B2 (en) 2004-07-20 2015-12-01 Warner-Lambert Company Llc Forms of [R-(R*,R*)]-2-(4-fluorophenyl)-β,δ-dihydroxy-5-(1-methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1H-pyrrole-1-heptanoic acid calcium salt (2:1)
US9481647B2 (en) 2004-07-20 2016-11-01 Warner-Lambert Company Llc Forms of [R-(R*,R*)]-2-(4-fluorophenyl)-β, δ-dihydroxy-5-(1-methylethyl)-3-Phenyl-4-[(phenylamino)carbonyl]-1H-pyrrole-1-heptanoic acid calcium salt (2:1)
US9790177B2 (en) 2004-07-20 2017-10-17 Warner-Lambert Company Llc Forms of [R-(R*,R*)]-2-(4-fluorophenyl)-beta, gamma-dihydroxy-5-(1-methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1H-pyrrole-1-heptanoic acid calcium salt (2:1)
WO2006011041A2 (en) * 2004-07-20 2006-02-02 Warner-Lambert Company Llc Crystalline forms of (r-(r*))-2-(4-fluorophenyl)-beta, gamma-dihydroxy-5-(1-methylethyl)-3-phenyl-4-((phenylamino)carbonyl)-1h-pyrrole-1-hept anoic acid calcium salt (2:1)
WO2006012499A3 (en) * 2004-07-22 2006-07-20 Teva Pharma Novel crystal forms of atorvastatin hemi-calcium and processes for their preparation
WO2006012499A2 (en) * 2004-07-22 2006-02-02 Teva Pharmaceutical Industries Ltd. Novel crystal forms of atorvastatin hemi-calcium and processes for their preparation
KR100881103B1 (en) * 2004-09-28 2009-02-02 테바 파마슈티컬 인더스트리즈 리미티드 Process for preparing forms of atorvastatin calcium substantially free of impurities
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US7674923B2 (en) 2004-09-28 2010-03-09 Teva Pharmaceutical Industries Ltd Process for preparing forms of atorvastatin calcium substantially free of impurities
WO2006037125A1 (en) * 2004-09-28 2006-04-06 Teva Pharmaceutical Industries Ltd. Process for preparing forms of atorvastatin calcium substantially free of impurities
WO2006048894A1 (en) * 2004-11-05 2006-05-11 Morepen Laboratories Limited Novel crystalline forms of atorvastatin calcium and processes for preparing them.
US8080672B2 (en) 2005-12-13 2011-12-20 Teva Pharmaceutical Industries Ltd. Crystal form of atorvastatin hemi-calcium and processes for preparation thereof
WO2008002655A2 (en) * 2006-06-28 2008-01-03 Teva Pharmaceutical Industries Ltd. Crystalline forms of atorvastatin
JP2008007507A (en) * 2006-06-28 2008-01-17 Teva Pharmaceutical Industries Ltd Crystalline atorvastatin
WO2008002655A3 (en) * 2006-06-28 2008-03-27 Teva Pharma Crystalline forms of atorvastatin
EP2132171A4 (en) * 2007-03-02 2010-11-17 Dong A Pharm Co Ltd Novel crystal forms of pyrrolylheptanoic acid derivatives
EP2132171A1 (en) * 2007-03-02 2009-12-16 Dong-A Pharm.Co., Ltd. Novel crystal forms of pyrrolylheptanoic acid derivatives
JP2010520273A (en) * 2007-03-02 2010-06-10 ドン・ア・ファーム・カンパニー・リミテッド A novel crystalline form of pyrrolylheptanoic acid derivatives
WO2009007856A3 (en) * 2007-07-11 2009-06-25 Actavis Group Ptc Ehf Novel polymorph of atorvastatin calcium and use thereof for the preparation of amorphous atorvastatin calcium
WO2009007856A2 (en) * 2007-07-11 2009-01-15 Actavis Group Ptc Ehf Novel polymorph of atorvastatin calcium and use thereof for the preparation of amorphous atorvastatin calcium
US11065237B2 (en) 2013-11-15 2021-07-20 Akebia Therapeutics, Inc. Solid forms of {[5-(3-chlorophenyl)-3-hydroxypyridine-2-carbonyl]amino}acetic acid, compositions, and uses thereof
US11690836B2 (en) 2013-11-15 2023-07-04 Akebia Therapeutics, Inc. Solid forms of {[5-(3-chlorophenyl)-3-hydroxypyridine-2-carbonyl]amino}acetic acid, compositions, and uses thereof

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CA2508871A1 (en) 2004-06-17
EP1572643A2 (en) 2005-09-14
WO2004050618A8 (en) 2005-07-14

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