WO2007108604A1 - Pharmaceutical composition containing clopidogrel camphorsulfonate or polymorphic forms thereof - Google Patents

Pharmaceutical composition containing clopidogrel camphorsulfonate or polymorphic forms thereof Download PDF

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Publication number
WO2007108604A1
WO2007108604A1 PCT/KR2007/001278 KR2007001278W WO2007108604A1 WO 2007108604 A1 WO2007108604 A1 WO 2007108604A1 KR 2007001278 W KR2007001278 W KR 2007001278W WO 2007108604 A1 WO2007108604 A1 WO 2007108604A1
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Prior art keywords
clopidogrel
polymorphic form
pharmaceutical composition
polymorphic
camphor
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PCT/KR2007/001278
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French (fr)
Inventor
Won Jeoung Kim
Han Kyong Kim
Kwee Hyun Suh
Gwan Sun Lee
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Hanmi Pharm. Co., Ltd.
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Publication date
Application filed by Hanmi Pharm. Co., Ltd. filed Critical Hanmi Pharm. Co., Ltd.
Priority to US12/293,357 priority Critical patent/US20090209576A1/en
Priority to EP07745581A priority patent/EP1996197A1/en
Priority to AU2007227919A priority patent/AU2007227919B2/en
Publication of WO2007108604A1 publication Critical patent/WO2007108604A1/en

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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/435Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with one nitrogen as the only ring hetero atom
    • A61K31/47Quinolines; Isoquinolines
    • A61K31/4738Quinolines; Isoquinolines ortho- or peri-condensed with heterocyclic ring systems
    • A61K31/4743Quinolines; Isoquinolines ortho- or peri-condensed with heterocyclic ring systems condensed with ring systems having sulfur as a ring hetero atom
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/435Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with one nitrogen as the only ring hetero atom
    • A61K31/47Quinolines; Isoquinolines
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P7/00Drugs for disorders of the blood or the extracellular fluid
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P7/00Drugs for disorders of the blood or the extracellular fluid
    • A61P7/02Antithrombotic agents; Anticoagulants; Platelet aggregation inhibitors
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D495/00Heterocyclic compounds containing in the condensed system at least one hetero ring having sulfur atoms as the only ring hetero atoms
    • C07D495/02Heterocyclic compounds containing in the condensed system at least one hetero ring having sulfur atoms as the only ring hetero atoms in which the condensed system contains two hetero rings
    • C07D495/04Ortho-condensed systems

Definitions

  • the present invention relates to a pharmaceutical composition containing the salt of clopidogrel and camphorsulfonic acid or its polymorphic forms as an active ingredient.
  • Clopidogrel methyl (+)-(S)- ⁇ -(o-chlorophenyl)-6,7-dihydrothieno[3,2- a]pyridine-5(4#)-acetate of formula (II), is a platelet-aggregation inhibitor which is effective in treating and preventing various platelet-associated vascular diseases such as stroke, cerebral arteriosclerosis, myocardial infarction, angina pectoris, arrhythmia, peripheral arteries disease and Burger's disease.
  • various platelet-associated vascular diseases such as stroke, cerebral arteriosclerosis, myocardial infarction, angina pectoris, arrhythmia, peripheral arteries disease and Burger's disease.
  • clopidogrel As a free base form of clopidogrel is an oil which is relatively unstable and is difficult to purify, a stable solid form of clopidogrel suitable for use in the preparation of a pharmaceutical composition has been sought, and there have been reported an acid addition salt of clopidogrel and its polymorphic forms obtained by using a pharmaceutically acceptable inorganic or organic acid.
  • U.S. Patent No. 4,847,265 discloses a number of acid addition salts of clopidogrel including hydrochloride, hydrobromide, hydrogen sulfate and taurocholate.
  • U.S. Patent No. 6,767,913, U.S. Publication Patent No. 2003/225129 and International Publication Patent No. WO 2004/081016 disclose new polymorphic forms of clopidogrel hydrogen sulfate; International Publication Patent Nos. WO 2003/006637, WO 2005/068471 and WO 2005/08089O 5 polymorphic forms of each of clopidogrel hydrochloride and clopidogrel hydrobromide; and International Publication Patent Nos. WO 2004/072084 and WO 2004/106344, solvates and polymorphic forms of each of solid clopidogrel bezenesulfonate and toluenesulfonate.
  • clopidogrel hydrogen sulfate employed in PLAVIXTM (Sanofi-Synthelabo Inc.), a commercial tablet composition, is not sufficiently stable.
  • PLAVIXTM is unstable under an accelerated test condition (40 " C, 75% relative humidity, for 3 months), generating significant amounts of impurities such as hydrolyzed by-products and levorotatory isomers (see [Y Gomez et al., J. Pharm. Biomed. Anal. 34: 341-348, 2004] and [H. Agrawal et al., Talanta, 61: 581-589, 2003]).
  • WO 2004/074215, WO 2004/013147 and WO 2004/106344 disclose the use of camphorsulfonic acid salt of clopidogrel, specifically, (-)-(lR)-camphor-10- sulfonic acid salt in the process of optically resolving racemic clopidogrel.
  • camphorsulfonic acid salt of clopidogrel or some polymorphic forms thereof is more stable toward moisture and heat than conventional acid addition salts.
  • FIGs. 1 to 3 a powder X-ray diffraction spectrum, a differential scanning calorimeter and an FT-IR absorption spectrum of the polymorphic form A 1 of clopidogrel (-)-( 1 R)-camphor- 1 O-sulfonate, respectively;
  • FIGs. 4 to 6 a powder X-ray diffraction spectrum, a differential scanning calorimeter and an FT-IR absorption spectrum of the polymorphic form Bl of clopidogrel (+)-(lS)-camphor-l O-sulfonate, respectively;
  • FIGs. 7 to 9 a powder X-ray diffraction spectrum, a differential scanning calorimeter and an FT-IR absorption spectrum of the polymorphic form B2 of clopidogrel (+)-(lS)-camphor-l O-sulfonate, respectively;
  • FIGs. 10 and 11 a powder X-ray diffraction spectrum and a differential scanning calorimeter of the polymorphic form B3 of clopidogrel (+)-( l$)-eamphor- 1 O-sulfonate, respectively;
  • FIG. 12 time-dependent changes (%) in the assay of four acid addition salts of clopidogrel;
  • FIG. 13 time-dependent changes (%) in the amount of hydro lyzed impurities of four acid addition salts of clopidogrel;
  • FIG. 14 time-dependent changes (%) in the amount of levorotatory isomers of four acid addition salts of clopidogrel.
  • FIG. 15 time-dependent changes (%) in the water content of four acid addition salts of clopidogrel.
  • a pharmaceutical composition for treating or preventing a platelet aggregation-associated disease which comprises clopidogrel camphorsulfonate of formula (I) or its polymorphic forms as an active ingredient:
  • the clopidogrel camphorsulfonate of formula (I) may be (-)-(lR)- camphor-10-sulfonic acid addition salt of clopidogrel of formula (Ia) or (+)- (lS)-camphor-lO-sulfonic acid addition salt of clopidogrel of formula (Ib):
  • the clopidogrel ( ⁇ )-(lR)-camphor-10-sulfonate of formula (Ia) and the clopidogrel (+)-(lS)-camphor-10-sulfonate of formula (Ib) may both have various forms of crystals, i.e., polymorphic forms.
  • the clopidogrel (-)-(lR)-camphor-10-sulfonate of formula (Ia) may have at least two polymorphic forms including polymorphic forms Al and A2, and the clopidogrel (+)-(! S)-camphor-10-sulfonate of formula (Ib), at least three polymorphic forms including polymorphic forms Bl 5 B2 and B3.
  • the inventive pharmaceutical composition may comprise any of the polymorphic forms Al 5 A2 5 Bl 5 B2 and B3 5 or a mixture thereof as an active ingredient.
  • the polymorphic form Al of the clopidogrel (-)-(lR)-camphor-10- sulfonate has the crystal form whose powder X-ray diffraction (XRD) scan shows major peaks having 1/I 0 values greater than 20% (100 ⁇ I/I 0 >20) at 2theta (20) of 8.2, 8.7, 11.2, 16.4, 17.0, 18.6, 19.1, 20.6, 22.7, 23.9, 24.3, 26.2, 27.3 and 36.9 (FIG. 1).
  • Differential scanning calorimeter (DSC) curve of the polymorphic form Al at 10 ° C/min shows an absorption peak of about 75.5 J/g whose heat absorption starts at about 165 °C and reaches its maximum at about 168 ° C (FIG. 2).
  • the actually observed melting point of the polymorphic form Al is 162 to 165 °C .
  • the polymorphic form Al is characterized by having major peaks at 2956, 1756, 1737, 1471, 1454, 1438, 1324, 1304, 1266, 1243, 1226 and 1190 cm “1 in its FT-IR absorption spectrum, as shown in FIG. 3.
  • the polymorphic form Bl of the clopidogrel (+)-(lS)-camphor-10- sulfonate has the crystal form whose powder XRD scan shows major peaks having 1/I 0 values greater than 20% (100 ⁇ I/I 0 >20) at 2 ⁇ of 8.3, 11.5, 13.0, 13.3, 14.1, 15.0, 17.1, 18.3, 18.9, 19.8, 21.4, 22.4, 25.1 and 26.0 (FIG. 4).
  • DSC curve of the polymorphic form Bl at 10 ° C/min shows an absorption peak of about 70 J/g whose heat absorption starts at about 145 0 C and reaches its maximum at about 151 "C (FIG. 5).
  • the actually observed melting point of the polymorphic form Bl is 149 to 150 ° C .
  • the polymorphic form Bl is characterized by having major peaks at 2959, 2936, 1752, 1739, 1452, 1437, 1301, 1241, 1147, 1028, 753, 723 and 613 cnT 1 in its FT-IR absorption spectrum, as shown in FIG. 6.
  • the polymorphic form B2 of the clopidogrel (+)-(! S)-camphor- 10- sulfonate has the crystal form whose powder XRD scan shows major peaks having 1/I 0 values greater than 10% (100 ⁇ I/I 0 >10) at 2 ⁇ of 7.9, 11.9, 14.1, 15.1, 15.7, 17.5, 17.8, 19.2, 19.5, 20.9 and 24.9 (FIG. 7).
  • DSC curve of the polymorphic form B2 at 10 ° C/min shows an absorption peak of about 54 J/g whose heat absorption starts at about 132 ° C and reaches its maximum at about 138 ° C (FIG. 8).
  • the actually observed melting point of the polymorphic form B2 is 135 to 136 ° C .
  • polymorphic form B2 is characterized by having major peaks at 2959, 1748, 1479, 1446, 1322, 1301, 1233, 1201, 1145, 1024, 754, 725 and 614 cm “1 in its FT-IR absorption spectrum, as shown in FIG. 9.
  • the polymorphic forms A2 and B3 are amorphous forms of clopidogrel (-)-(lR)-camphor-10-sulfonate and clopidogrel (+)-(! S)-cam ⁇ hor-10-sulfonate, respectively.
  • These amorphous salts have neither prominent diffraction angles at the powder XRD spectrum nor prominent heat absorption and heat discharge peaks at the DSC, which is confirmed from the curves of FIGs. 10 and 11 which represent the powder XRD spectrum and the DSC of the polymorphic form B3, respectively.
  • (+)-(lS)-Cam ⁇ hor-10-sulfonic acid for the preparation of the clopidogrel camphorsulfonate of formula (I) is frequently employed in the formation of the acid addition salt of alkaline active ingredient, and it is referred to as "camsilate” according to INN and as “camsylate” according to USAN (see [S. M. Berge et al., J. Pharm. Sci 66: 1, 1977], [Handbooks of Pharmaceutical Salts, 'Properties, Selection, and Use', P. H. Stahl] and [C. G. Wermuth Eds., 2002, Verlag Helvetica Chimica Acta, Zurich, pp 275]).
  • the polymorphic forms Al, Bl and B2 may be each prepared by reacting clopidogrel (dextro-rotatory clopidogrel free base) with camphorsulfonic acid, i.e., (-)-(lR)-camphor-10-sulfonic acid or (+)-(lS)- camphor-10-sulfonic acid, in an organic solvent.
  • camphorsulfonic acid i.e., (-)-(lR)-camphor-10-sulfonic acid or (+)-(lS)- camphor-10-sulfonic acid
  • the organic solvent may be employed in an amount ranging from 1 to 50 by ml volume, preferably 3 to 20 by ml volume, based on Ig weight of clopidogrel. It is preferred that when diethyl ether, diisopropyl ether or methyl t-butyl ether is used together with other organic solvents, its volume does not exceed 80% of the total volume of the solvent.
  • camphorsulfonic acid i.e., (-)-(lR)-camphor-10-sulfonic acid or (+)-(lS)- camphor-10-sulfonic acid, may be employed in an amount ranging from 0.9 to 1.2 moles based on 1.0 mole of clopidogrel.
  • the reaction and the crystallization of the salt may be performed at a temperature ranging from -10 °C to the boiling point of the solvent for a period ranging from 0.1 to 24 hours.
  • the resulting reaction mixture may be allowed to be cooled to a temperature ranging from -10 ° C to room temperature and to be stirred for a period ranging from 1 to 24 hours.
  • the precipitates thus formed may be filtered and washed with the solvent used in the reaction or the crystallization.
  • the precipitates are dried using an inert gas such as air and nitrogen under an atmospheric pressure or under a reduced pressure at a temperature ranging from room temperature to 70 °C . If necessary, the polymorphic forms Al, BI and B2 may be each further purified by recrystallization under the organic solvent.
  • the polymorphic form A2 may be prepared by dissolving the polymorphic form Al in at least one organic solvent selected from the group consisting of methanol, ethanol, acetone, acetonitrile, dichloromethane and chloroform, spray drying the solution or removing the solvent therefrom under a reduced pressure, and grinding the resulting residue. So may be prepared the polymorphic form B3 from the polymorphic form Bl or B2.
  • the polymorphic forms Al and Bl When the polymorphic forms Al and Bl are revealed to an accelerated condition of 60 °C and 75% relative humidity for a period of over 28 days, they almost maintain their original water contents, thereby being less hygroscopic, and very stable against moisture and heat.
  • the polymorphic forms Al and Bl show satisfactory water-solubilities of around 4.0 mg/ml when measured in a saturated aqueous solution, which represents their effective dissolution from pharmaceutical compositions containing same. Even though clopidogrel has a relatively low optical purity of 90.0% ee (enantiomeric excess), the desired clopidogrel salt obtained therefrom may have a significantly high optical purity of at least 98.5% ee.
  • the clopidogrel camphorsulfonate of formula (I) and its polymorphic forms may be employed each independently or in a mixed form as an active ingredient in the preparation of a pharmaceutical composition.
  • a pharmaceutical composition comprising the clopidogrel camphorsulfonate or its polymorphic forms can be useful for the treatment and prevention of a platelet aggregation-associated disease.
  • platelet aggregation-associated disease examples include stroke, cerebral arteriosclerosis, myocardial infarction, angina pectoris, arrhythmia, peripheral arteries disease and Burger's disease.
  • inventive pharmaceutical composition comprising the clopidogrel camphorsulfonate or its polymorphic forms as an active ingredient may be administered via the oral route, and, thus, the inventive pharmaceutical composition may be in the form of solutions, suspensions, tablets, pills, capsules, powders and the like.
  • the pharmaceutical composition according to the present invention may be formulated together with pharmaceutically acceptable carriers, if necessary.
  • suitable carriers are excipients such as starch, sugar and mannitol; filling agents or increasing agents such as calcium phosphate and silica derivatives; binding agents such as cellulose derivatives of carboxymethylcellulose or hydroxypropylcellulose, gelatin, arginic acid salt and polyvinylpyrrolidone; lubricating agents such as talc, magnesium or calcium stearate, hydrogenated castor oil and solid polyethylene glycol; disintegrants such as povidone, croscarmellose sodium and crospovidone; and surfactants such as polysorbate, cetyl alcohol and glycerol monostearate.
  • compositions comprising a specific amount of an active ingredient together with or without such additives may be prepared in ' accordance with any of the conventional procedures ⁇ see [Remington 's Pharmaceutical Science, Mack Publishing Company, Easton, PA, 19 th Edition, 1995]).
  • the inventive pharmaceutical composition may contain the clopidogrel camphorsulfonate or its polymorphic forms in an amount ranging from 0.1 to 95% by weight, preferably 1 to 70% by weight, based on the total weight of the composition.
  • the clopidogrel camphorsulfonate of formula (I) may be orally administered to a subject in a dose ranging from 1 to 2,000 mg/60 kg weight, preferably 25 to 600 mg/60 kg weight per day with one portion or divided portions.
  • a dose ranging from 1 to 2,000 mg/60 kg weight, preferably 25 to 600 mg/60 kg weight per day with one portion or divided portions.
  • Condition B For the measurement of the amount of hydrolyzed impurities of acid addition salt of clopidogrel - Column: Capcellpak C18 MQ 5 ⁇ m (250 mm ⁇ 4.6 mm) - Detector: 210 nm - Flow rate: 1.0 m-ft/min.
  • Clopidogrel hydrogen sulfate as a crystalline form II was prepared according to the method similar to that disclosed in U.S. Patent No. 6,429,210 from clopidogrel free base having an optical purity of 98.5% ee.
  • Clopidogrel benzenesulfonate as a crystalline form III was prepared according to the method similar to that disclosed in International Publication Patent No. 2005/0203122 from clopidogrel free base having an optical purity of 98.5% ee. m.p.: 134 ⁇ 136 ° C (calculated value 135-138 0 C) water (Karl-Fisher titrator): below 0.1% optical purity (HPLC): 99.3% ee
  • Example 2 Ig of the polymorphic form Bl of the clopidogrel (+)-(lS)-camphor- 10-sulfonate (clopidogrel camsilate) obtained in Example 2 was dissolved in 12m-£ of acetone under a reflux. The solution was cooled to room temperature and a small quantity of the polymorphic form Bl was added thereto. The mixture was stirred at room temperature for 2 hours, and then, at a temperature ranging from 0 to 5 °C for 12 hours. The precipitates formed were filtered, washed with cool acetone and dried at 50 ° C , to obtain 0.75g of the title compound (yield: 75%) as an white crystal.
  • Example 4 Preparation of clopidogrel (+)-(lS)-cam ⁇ hor ⁇ 10-sulfonate (polymorphic form Bl)
  • Example 8 B2 obtained in Example 8 were added thereto. Then, the mixture was quickly cooled to a temperature ranging from 0 to 5 ° C , and then, it was kept at that temperature for one night while intermittently stirring. The precipitates formed were filtered, washed with cool ethyl acetate and dried at 50 ° C , to obtain 1 ,43g of the title compound (yield: 83%) as an white crystal.
  • Test Example 1 Optical purity measurement of acid addition salt of clopidogrel
  • the optical purities of the acid addition salts obtained were measured under HPLC condition C, and the extents of optical purity improvement are shown in Table 4. ⁇ Table 4>
  • Clopidogrel is liable to be partially racemized to its levorotatory isomer, and thus, a plurality of purification steps is required to achieve a pharmaceutically acceptable optical purity.
  • inventive clopidogrel camphorsulfonate meets the pharmaceutical optical purity requirements without separate purification steps.
  • Test Example 2 Water-solubility measurement of acid addition salt of clopidogrel
  • the water-solubility of the clopidogrel camphorsulfonate according to the present invention was lower than that of hydrogen sulfate or benzenesulfonate, but such water-solubility level is more than sufficient for use in a pharmaceutical composition.
  • Test Example 3 Stability test of acid addition salt of clopidogrel under moist and heated condition
  • the inventive clopidogrel camphorsulfonate and its polymorphic forms were less hygroscopic, and more stable against moisture or heat, as compared to hydrogen sulfate and benzenesulfonate, which suggests that there is no significant decline in the amount of optically pure clopidogrel even after storage under a severe condition for a long period.
  • inventive clopidogrel camphorsulfonate and its polymorphic forms may be formulated alone or in a combination with pharmaceutically acceptable additives, according to any of the conventional methods used to prepare soft or hard capsules and tablets.
  • a tablet was prepared using the following ingredients:
  • inventive clopidogrel camphorsulfonate and its polymorphic forms are very stable against moisture and heat. Accordingly, the inventive pharmaceutical composition comprising same can maintain a high purity of an active ingredient for a prolonged time, and it can be very useful in the prevention and treatment for platelet aggregation-associated diseases. While the invention has been described with respect to the above specific embodiments, it should be recognized that various modifications and changes may be made to the invention by those skilled in the art which also fall within the scope of the invention as defined by the appended claims.

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Abstract

A pharmaceutical composition of the present invention which comprises clopidogrel camphorsulfonate of formula (I) or its polymorphic forms as an active ingredient is useful for treating or preventing a platelet aggregation-associated disease.

Description

PHARMACEUTICAL COMPOSITION CONTAINING CLOPIDOGREL CAMPHORSULFONATE OR POLYMORPHIC FORMS THEREOF
FIELD OF THE INVENTION
The present invention relates to a pharmaceutical composition containing the salt of clopidogrel and camphorsulfonic acid or its polymorphic forms as an active ingredient.
BACKGROUND OF THE INVENTION
Clopidogrel, methyl (+)-(S)-α-(o-chlorophenyl)-6,7-dihydrothieno[3,2- a]pyridine-5(4#)-acetate of formula (II), is a platelet-aggregation inhibitor which is effective in treating and preventing various platelet-associated vascular diseases such as stroke, cerebral arteriosclerosis, myocardial infarction, angina pectoris, arrhythmia, peripheral arteries disease and Burger's disease.
Figure imgf000003_0001
As a free base form of clopidogrel is an oil which is relatively unstable and is difficult to purify, a stable solid form of clopidogrel suitable for use in the preparation of a pharmaceutical composition has been sought, and there have been reported an acid addition salt of clopidogrel and its polymorphic forms obtained by using a pharmaceutically acceptable inorganic or organic acid.
For example, U.S. Patent No. 4,847,265 discloses a number of acid addition salts of clopidogrel including hydrochloride, hydrobromide, hydrogen sulfate and taurocholate. In addition, U.S. Patent No. 6,767,913, U.S. Publication Patent No. 2003/225129 and International Publication Patent No. WO 2004/081016 disclose new polymorphic forms of clopidogrel hydrogen sulfate; International Publication Patent Nos. WO 2003/006637, WO 2005/068471 and WO 2005/08089O5 polymorphic forms of each of clopidogrel hydrochloride and clopidogrel hydrobromide; and International Publication Patent Nos. WO 2004/072084 and WO 2004/106344, solvates and polymorphic forms of each of solid clopidogrel bezenesulfonate and toluenesulfonate.
Among the above acid addition salts of clopidogrel, the most preferred has been crystalline clopidogrel hydrogen sulfate. However, it is known that clopidogrel hydrogen sulfate employed in PLAVIX™ (Sanofi-Synthelabo Inc.), a commercial tablet composition, is not sufficiently stable. For example, it was reported that PLAVIX™ is unstable under an accelerated test condition (40 "C, 75% relative humidity, for 3 months), generating significant amounts of impurities such as hydrolyzed by-products and levorotatory isomers (see [Y Gomez et al., J. Pharm. Biomed. Anal. 34: 341-348, 2004] and [H. Agrawal et al., Talanta, 61: 581-589, 2003]).
As the stability of the active ingredient used in a pharmaceutical composition is very important in terms of shelf storage life, maintenance of its activity and suppressing undesirable side effects, there has been a need to develop an improved salt of clopidogrel. U.S. Patent No. 4,847,265, and International Publication Patent Nos.
WO 2004/074215, WO 2004/013147 and WO 2004/106344 disclose the use of camphorsulfonic acid salt of clopidogrel, specifically, (-)-(lR)-camphor-10- sulfonic acid salt in the process of optically resolving racemic clopidogrel.
The inventors have unexpectedly found that such camphorsulfonic acid salt of clopidogrel or some polymorphic forms thereof is more stable toward moisture and heat than conventional acid addition salts.
SUMMARY OF THE INVENTION
It is an object of the present invention to provide a pharmaceutical composition containing the salt of clopidogrel and camphorsulfonic acid or its polymorphic forms as an active ingredient.
BRIEF DESCRIPTION OF THE DRAWINGS
The above and other objects and features of the present invention will become apparent from the following description of the invention, when taken in conjunction with the accompanying drawings which respectively show:
FIGs. 1 to 3 : a powder X-ray diffraction spectrum, a differential scanning calorimeter and an FT-IR absorption spectrum of the polymorphic form A 1 of clopidogrel (-)-( 1 R)-camphor- 1 O-sulfonate, respectively;
FIGs. 4 to 6 : a powder X-ray diffraction spectrum, a differential scanning calorimeter and an FT-IR absorption spectrum of the polymorphic form Bl of clopidogrel (+)-(lS)-camphor-l O-sulfonate, respectively;
FIGs. 7 to 9 : a powder X-ray diffraction spectrum, a differential scanning calorimeter and an FT-IR absorption spectrum of the polymorphic form B2 of clopidogrel (+)-(lS)-camphor-l O-sulfonate, respectively;
FIGs. 10 and 11 : a powder X-ray diffraction spectrum and a differential scanning calorimeter of the polymorphic form B3 of clopidogrel (+)-( l$)-eamphor- 1 O-sulfonate, respectively; FIG. 12: time-dependent changes (%) in the assay of four acid addition salts of clopidogrel;
FIG. 13: time-dependent changes (%) in the amount of hydro lyzed impurities of four acid addition salts of clopidogrel;
FIG. 14 : time-dependent changes (%) in the amount of levorotatory isomers of four acid addition salts of clopidogrel; and
FIG. 15: time-dependent changes (%) in the water content of four acid addition salts of clopidogrel.
DETAILED DESCRIPTION OF THE INVENTION
In accordance with one aspect of the present invention, there is provided a pharmaceutical composition for treating or preventing a platelet aggregation-associated disease, which comprises clopidogrel camphorsulfonate of formula (I) or its polymorphic forms as an active ingredient:
Figure imgf000006_0001
The clopidogrel camphorsulfonate of formula (I) may be (-)-(lR)- camphor-10-sulfonic acid addition salt of clopidogrel of formula (Ia) or (+)- (lS)-camphor-lO-sulfonic acid addition salt of clopidogrel of formula (Ib):
Figure imgf000006_0002
Figure imgf000006_0003
The clopidogrel (~)-(lR)-camphor-10-sulfonate of formula (Ia) and the clopidogrel (+)-(lS)-camphor-10-sulfonate of formula (Ib) may both have various forms of crystals, i.e., polymorphic forms. Specifically, the clopidogrel (-)-(lR)-camphor-10-sulfonate of formula (Ia) may have at least two polymorphic forms including polymorphic forms Al and A2, and the clopidogrel (+)-(! S)-camphor-10-sulfonate of formula (Ib), at least three polymorphic forms including polymorphic forms Bl5 B2 and B3. Thus, the inventive pharmaceutical composition may comprise any of the polymorphic forms Al5 A25 Bl5 B2 and B35 or a mixture thereof as an active ingredient.
In accordance with the present invention, there are provided polymorphic forms Al and A2 of the clopidogrel (-)-(lR)-camρhor-10- sulfonate of formula (Ia)5 and polymorphic forms Bl5 B2 and B3 of the clopidogrel (+)-(lS)-camphor-10~sulfonate of formula (Ib).
The polymorphic form Al of the clopidogrel (-)-(lR)-camphor-10- sulfonate has the crystal form whose powder X-ray diffraction (XRD) scan shows major peaks having 1/I0 values greater than 20% (100χI/I0>20) at 2theta (20) of 8.2, 8.7, 11.2, 16.4, 17.0, 18.6, 19.1, 20.6, 22.7, 23.9, 24.3, 26.2, 27.3 and 36.9 (FIG. 1). Differential scanning calorimeter (DSC) curve of the polymorphic form Al at 10°C/min shows an absorption peak of about 75.5 J/g whose heat absorption starts at about 165 °C and reaches its maximum at about 168 °C (FIG. 2). The actually observed melting point of the polymorphic form Al is 162 to 165 °C . Further, the polymorphic form Al is characterized by having major peaks at 2956, 1756, 1737, 1471, 1454, 1438, 1324, 1304, 1266, 1243, 1226 and 1190 cm"1 in its FT-IR absorption spectrum, as shown in FIG. 3. The polymorphic form Bl of the clopidogrel (+)-(lS)-camphor-10- sulfonate has the crystal form whose powder XRD scan shows major peaks having 1/I0 values greater than 20% (100χI/I0>20) at 2Θ of 8.3, 11.5, 13.0, 13.3, 14.1, 15.0, 17.1, 18.3, 18.9, 19.8, 21.4, 22.4, 25.1 and 26.0 (FIG. 4). DSC curve of the polymorphic form Bl at 10°C/min shows an absorption peak of about 70 J/g whose heat absorption starts at about 1450C and reaches its maximum at about 151 "C (FIG. 5). The actually observed melting point of the polymorphic form Bl is 149 to 150 °C . Further, the polymorphic form Bl is characterized by having major peaks at 2959, 2936, 1752, 1739, 1452, 1437, 1301, 1241, 1147, 1028, 753, 723 and 613 cnT1 in its FT-IR absorption spectrum, as shown in FIG. 6.
The polymorphic form B2 of the clopidogrel (+)-(! S)-camphor- 10- sulfonate has the crystal form whose powder XRD scan shows major peaks having 1/I0 values greater than 10% (100χI/I0 >10) at 2θ of 7.9, 11.9, 14.1, 15.1, 15.7, 17.5, 17.8, 19.2, 19.5, 20.9 and 24.9 (FIG. 7). DSC curve of the polymorphic form B2 at 10°C/min shows an absorption peak of about 54 J/g whose heat absorption starts at about 132 °C and reaches its maximum at about 138 °C (FIG. 8). The actually observed melting point of the polymorphic form B2 is 135 to 136 °C . Further, the polymorphic form B2 is characterized by having major peaks at 2959, 1748, 1479, 1446, 1322, 1301, 1233, 1201, 1145, 1024, 754, 725 and 614 cm"1 in its FT-IR absorption spectrum, as shown in FIG. 9.
The polymorphic forms A2 and B3 are amorphous forms of clopidogrel (-)-(lR)-camphor-10-sulfonate and clopidogrel (+)-(! S)-camρhor-10-sulfonate, respectively. These amorphous salts have neither prominent diffraction angles at the powder XRD spectrum nor prominent heat absorption and heat discharge peaks at the DSC, which is confirmed from the curves of FIGs. 10 and 11 which represent the powder XRD spectrum and the DSC of the polymorphic form B3, respectively.
(+)-(lS)-Camρhor-10-sulfonic acid for the preparation of the clopidogrel camphorsulfonate of formula (I) is frequently employed in the formation of the acid addition salt of alkaline active ingredient, and it is referred to as "camsilate" according to INN and as "camsylate" according to USAN (see [S. M. Berge et al., J. Pharm. Sci 66: 1, 1977], [Handbooks of Pharmaceutical Salts, 'Properties, Selection, and Use', P. H. Stahl] and [C. G. Wermuth Eds., 2002, Verlag Helvetica Chimica Acta, Zurich, pp 275]). The polymorphic forms Al, Bl and B2 may be each prepared by reacting clopidogrel (dextro-rotatory clopidogrel free base) with camphorsulfonic acid, i.e., (-)-(lR)-camphor-10-sulfonic acid or (+)-(lS)- camphor-10-sulfonic acid, in an organic solvent. Representative examples of the organic solvent which may be used in the present invention include diethyl ether, diisopropyl ether, methyl t-butyl ether, methyl acetate, ethyl acetate, n- propyl acetate, isopropyl acetate, n-butyl acetate, isobutyl acetate, acetone, methyl ethyl ketone, methyl isobutyl ketone, tetrahydrofuran, 1,4-dioxane, isopropanol and a mixture thereof.
The organic solvent may be employed in an amount ranging from 1 to 50 by ml volume, preferably 3 to 20 by ml volume, based on Ig weight of clopidogrel. It is preferred that when diethyl ether, diisopropyl ether or methyl t-butyl ether is used together with other organic solvents, its volume does not exceed 80% of the total volume of the solvent. Further, camphorsulfonic acid, i.e., (-)-(lR)-camphor-10-sulfonic acid or (+)-(lS)- camphor-10-sulfonic acid, may be employed in an amount ranging from 0.9 to 1.2 moles based on 1.0 mole of clopidogrel.
The reaction and the crystallization of the salt may be performed at a temperature ranging from -10 °C to the boiling point of the solvent for a period ranging from 0.1 to 24 hours. Preferably, after precipitation formation, the resulting reaction mixture may be allowed to be cooled to a temperature ranging from -10 °C to room temperature and to be stirred for a period ranging from 1 to 24 hours.
The precipitates thus formed may be filtered and washed with the solvent used in the reaction or the crystallization. The precipitates are dried using an inert gas such as air and nitrogen under an atmospheric pressure or under a reduced pressure at a temperature ranging from room temperature to 70 °C . If necessary, the polymorphic forms Al, BI and B2 may be each further purified by recrystallization under the organic solvent.
The polymorphic form A2 may be prepared by dissolving the polymorphic form Al in at least one organic solvent selected from the group consisting of methanol, ethanol, acetone, acetonitrile, dichloromethane and chloroform, spray drying the solution or removing the solvent therefrom under a reduced pressure, and grinding the resulting residue. So may be prepared the polymorphic form B3 from the polymorphic form Bl or B2.
When the polymorphic forms Al and Bl are revealed to an accelerated condition of 60 °C and 75% relative humidity for a period of over 28 days, they almost maintain their original water contents, thereby being less hygroscopic, and very stable against moisture and heat. In addition, the polymorphic forms Al and Bl show satisfactory water-solubilities of around 4.0 mg/ml when measured in a saturated aqueous solution, which represents their effective dissolution from pharmaceutical compositions containing same. Even though clopidogrel has a relatively low optical purity of 90.0% ee (enantiomeric excess), the desired clopidogrel salt obtained therefrom may have a significantly high optical purity of at least 98.5% ee.
Thus, the clopidogrel camphorsulfonate of formula (I) and its polymorphic forms may be employed each independently or in a mixed form as an active ingredient in the preparation of a pharmaceutical composition. A pharmaceutical composition comprising the clopidogrel camphorsulfonate or its polymorphic forms can be useful for the treatment and prevention of a platelet aggregation-associated disease.
Representative examples of the platelet aggregation-associated disease include stroke, cerebral arteriosclerosis, myocardial infarction, angina pectoris, arrhythmia, peripheral arteries disease and Burger's disease.
The inventive pharmaceutical composition comprising the clopidogrel camphorsulfonate or its polymorphic forms as an active ingredient may be administered via the oral route, and, thus, the inventive pharmaceutical composition may be in the form of solutions, suspensions, tablets, pills, capsules, powders and the like.
The pharmaceutical composition according to the present invention may be formulated together with pharmaceutically acceptable carriers, if necessary. Examples of suitable carriers are excipients such as starch, sugar and mannitol; filling agents or increasing agents such as calcium phosphate and silica derivatives; binding agents such as cellulose derivatives of carboxymethylcellulose or hydroxypropylcellulose, gelatin, arginic acid salt and polyvinylpyrrolidone; lubricating agents such as talc, magnesium or calcium stearate, hydrogenated castor oil and solid polyethylene glycol; disintegrants such as povidone, croscarmellose sodium and crospovidone; and surfactants such as polysorbate, cetyl alcohol and glycerol monostearate. Further, various pharmaceutical compositions comprising a specific amount of an active ingredient together with or without such additives may be prepared in ' accordance with any of the conventional procedures {see [Remington 's Pharmaceutical Science, Mack Publishing Company, Easton, PA, 19th Edition, 1995]).
The inventive pharmaceutical composition may contain the clopidogrel camphorsulfonate or its polymorphic forms in an amount ranging from 0.1 to 95% by weight, preferably 1 to 70% by weight, based on the total weight of the composition.
The clopidogrel camphorsulfonate of formula (I) may be orally administered to a subject in a dose ranging from 1 to 2,000 mg/60 kg weight, preferably 25 to 600 mg/60 kg weight per day with one portion or divided portions. The following Examples are given for the purpose of illustration only, and are not intended to limit the scope of the invention.
The analysis conditions of HPLC employed in Examples are listed below.
Condition A: For the measurement of the assay of acid addition salt of clopidogrel
- Column: Kromasil Cl 8, 5 μm (250 mm χ4.6 mm)
- Detector: 220 nm
- Flow rate: 1.5 m£/min - Mobile phase: Na2HPO4-NaH2PO4 buffer solution : THF : CH3CN = 5 : 2 : 3 (Wv)
Condition B: For the measurement of the amount of hydrolyzed impurities of acid addition salt of clopidogrel - Column: Capcellpak C18 MQ 5 μm (250 mm χ4.6 mm) - Detector: 210 nm - Flow rate: 1.0 m-ft/min.
- Mobile phase: KH2PO4 buffer solution/CH3CN (70/30) : KH2PO4 buffer solution/CH3CN (30/70) = 0 : 100 →IOO : 0 (v/v, gradient elution)
Condition C: For the measurement of the optical purity of acid addition salt of clopidogrel
- Column: Chiralpak AD5 5 μm (250 mm x4.6 mm) - Detector: 210 nm
- Flow rate: 1.0 ml/min. - Mobile phase: n-hexane : isopropanol = 90 : 10 (v/v)
In the following Examples, employed was clopidogrel free base which had been prepared by the methods disclosed in U.S. Patent No. 4,847,265 and International Publication Patent No. WO 2005/087779.
Comparative Example 1 : Preparation of clopidogrel hydrogen sulfate
Clopidogrel hydrogen sulfate as a crystalline form II was prepared according to the method similar to that disclosed in U.S. Patent No. 6,429,210 from clopidogrel free base having an optical purity of 98.5% ee.
m.p.: 176-177 °C (calculated value 176°C) water (Karl-Fisher titrator): below 0.1% optical purity (HPLC, condition C): 98.6% ee
Comparative Example 2: Preparation of clopidogrel benzenesulfonate
Clopidogrel benzenesulfonate as a crystalline form III was prepared according to the method similar to that disclosed in International Publication Patent No. 2005/0203122 from clopidogrel free base having an optical purity of 98.5% ee. m.p.: 134~136°C (calculated value 135-1380C) water (Karl-Fisher titrator): below 0.1% optical purity (HPLC): 99.3% ee
Example 1 : Preparation of clopidogrel (-)-(lR)-camphor~10-sulfonate (polymorphic form Al)
2Og of clopidogrel free base having an optical purity of 98.5% ee was dissolved in 20Om^ of acetone, and 14.5g of (-)-(lR)-camρhor-10-sulfonic acid was added thereto. Then, the mixture was stirred at room temperature for 4 hours. The precipitates formed were filtered, washed with cool acetone and dried at 500C , to obtain 1.48g of the title compound (yield: 86%) as an white crystal.
m.p.: 165-167°C water (Karl-Fisher titrator): below 0.1% specific rotatory power : [α]p20 + 25.0 (c=l, methanol) optical purity (KPLC5 condition C): above 99.6% ee IR (KBr, cm"1): 2956, 1756, 1737, 1471, 1454, 1438, 1324, 1304, 1266, 1243,
1226, 1190 (FIG. 3)
DSC (10°C/min): starting point about 165 TC, lowest point about 168 °C (heat absorption about 75.5 J/g, FIG. 2)
The result of powder X-ray diffraction analysis for the crystalline state of the polymorphic form Al of the clopidogrel (-)-(lR)-camphor-10-sulfonate showed that it was a crystal having the characteristic diffraction pattern as shown in FIG. 1. The main diffraction peaks having 1/I0 value greater than 20%, are listed in Table 1. <Table 1>
2Θ (± 0.2) d (± 0.2) 2Θ (± 0.2) d I/ϊo (H)
8.2 10.7 44.7 20.6 4.3 92.8
8.7 10.1 48.4 22.7 3.9 92.9
11.2 7.9 100.0 23.9 3.7 29.7
16.4 5.4 58.9 24.3 3.7 38.4
17.0 5.2 77.9 26.2 3.4 37.0
18.6 4.8 70.0 27.3 3.3 33.6
19.1 4.6 55.7 36.9 2.4 21.1
2Θ: angle of diffraction, d: distance within each crystal face, 1/I0 (%): relative intensity of peak
Example 2: Preparation of clopidogrel (+)-(lS)-camphor-10-sulfonate (polymorphic form B l)
2Og of clopidogrel free base having an optical purity of 98.5% ee was dissolved in 20Om-S of methyl ethyl ketone, and 14.5g of (+)-(lS)-camρhor-10- sulfonic acid was added thereto. The mixture was stirred at room temperature for 30 minutes, and then, at a temperature ranging from 0 to 5 °C for 4 hours.
The precipitates formed were filtered, washed with cool methyl ethyl ketone and dried at 50 °C , to obtain 29.6g of the title compound (yield: 86%) as an white crystal.
m.p.: 149-150°C water (Karl-Fisher titrator): below 0.2% specific rotatory power : [α]D 20 + 60.2 (c=l, methanol) optical purity (HPLC): above 99.6% ee
IR (KBr, cm"1): 2959, 2936, 1752, 1739, 1452, 1437, 1301, 1241, 1147, 1028, 753, 723, 613 (FIG 6)
DSC (10 °C/min): starting point about 145 °C , lowest point about 15 TC (heat absorption about 70 J/g, FIG. 5) The result of powder X-ray diffraction analysis for the crystalline state of the polymorphic form Bl of the clopidogrel (+)-(lS)-camρhor-10-sulfonate showed that it was a crystal having the characteristic diffraction pattern as shown in FIG 4. The main diffraction peaks having 1/I0 value greater than 20%, are listed in Table 2.
<Table 2>
2Θ (± 0.2) d (± 0.2) Vk (H) 2Θ (± 0.2) d VIo {%)
8.3 10.6 100.0 18.3 4.9 39.0
11,5 7.7 20.1 18.9 4.7 74.6
13.0 6.8 27.5 19.8 4.5 39.4
13.3 6.7 69.8 21.4 4.2 29.4
14.1 6.3 23.3 22.4 4.1 37.2
15.0 5.9 34.7 25.1 3.5 43.1
17.1 5.2 21.1 2Θ: angle of diffraction, d: distance within each crystal face, 1/I0 (%): relative intensity of peak
Example 3: Preparation of clopidogrel (+)-(lS)-camphor-10-sulfonate (polymorphic form Bl)
Ig of the polymorphic form Bl of the clopidogrel (+)-(lS)-camphor- 10-sulfonate (clopidogrel camsilate) obtained in Example 2 was dissolved in 12m-£ of acetone under a reflux. The solution was cooled to room temperature and a small quantity of the polymorphic form Bl was added thereto. The mixture was stirred at room temperature for 2 hours, and then, at a temperature ranging from 0 to 5 °C for 12 hours. The precipitates formed were filtered, washed with cool acetone and dried at 50 °C , to obtain 0.75g of the title compound (yield: 75%) as an white crystal. Example 4: Preparation of clopidogrel (+)-(lS)-camρhor~10-sulfonate (polymorphic form Bl)
Ig of clopidogrel free base was dissolved in 10 ml of ethyl acetate, and 0.72g of (+)-(lS)-camphor-10-sulfonic acid was added thereto. The mixture was stirred at room temperature for 1 hour, and then, at a temperature ranging from 0 to 5 °C for 4 hours. The precipitates formed were filtered, washed with cool ethyl acetate and dried at 50 °C, to obtain 1.55g of the title compound (yield: 90%) as an white crystal.
Example 5: Preparation of clopidogrel (+)-(lS)-camphor-10-sulfonate (polymorphic form Bl)
Ig of clopidogrel free base was dissolved in 10 ml of methyl isobutyl ketone, and 0.72g of (+)-(lS)-camphor-10-sulfonic acid was added thereto. The mixture was stirred at room temperature for 1 hour, and then, at a temperature ranging from 0 to 5 "C for 4 hours. The precipitates formed were filtered, washed with cool methyl isobutyl ketone and dried at 50 "C , to obtain 1.39g of the title compound as an white crystal.
Example 6: Preparation of clopidogrel (+)-(! S)-camphor-10-sulfonate (polymorphic form Bl)
Ig of clopidogrel free base was dissolved in 1O m-C of acetone, and 0.72g of (+)-(lS)-camphor-10-sulfonic acid and 10 ml of isopropyl ether were added thereto. The mixture was stirred at room temperature for 2 hours, and then, at a temperature ranging from 0 to 5 °C for 4 hours. The precipitates formed were filtered, washed with a mixture of acetone and isopropyl ether, and dried at 50 °C, to obtain 1.52g of the title compound (yield: 88%) as an white crystal. Example 7: Preparation of clopidogrel (+)-(lS)-camρhor-10-sulfonate (polymorphic form Bl)
Ig of clopidogrel free base was dissolved in 10-m.β of acetone, and 0.72g of (+)-( 1 S)-camρhor- 10-sulfonic acid and 1O m-C of methyl t-butyl ketone were added thereto. The mixture was stirred at room temperature for 2 hours, and then, at a temperature ranging from 0 to 5°C for 4 hours. The precipitates formed were filtered, washed with a mixture of acetone and methyl t-butyl ketone, and dried at 50 °C, to obtain 1.45g of the title compound (yield: 84%) as an white crystal.
Example 8: Preparation of clopidogrel (+)-(lS)-camphor-10-sulfonate (polymorphic form B2)
0.5g of clopidogrel free base was dissolved in 2 ml of methyl ethyl ketone, and 15 ml of methyl t-butyl ether were immediately added thereto. The resulting gel mixture was allowed to be solidified while scraping with a spatula. The solidified crystals were filtered, washed with methyl t-butyl ether and dried with a nitrogen flow, to obtain 0.6g of the title compound (yield: 70%) as an white powder.
m.p.: 135-136°C water (Karl-Fisher titrator): below 0.2% specific rotatory power : [α]o20 + 60.2 (c=l, methanol) optical purity (HPLC): above 99.5% ee
IR (KBr5 cm"1): 2959, 1748, 1479, 1446, 1322, 1301, 1233, 1201, 1145, 1024,
754, 725, 614 (FIG 9)
DSC (lOTC/min): starting point about 132 °C, lowest point about 138 °C (heat absorption about 54 J/g, FIG. 8)
The result of powder X-ray diffraction analysis for the crystalline state of the polymorphic form B2 of the clopidogrel (+)-(lS)~camphor~10-sulfonate showed that it was a crystal having the characteristic diffraction pattern as shown in FIG 7. The main diffraction peaks having 1/I0 value greater than 10%, are listed in Table 3.
<Table 3>
2Θ (± 0.2) d (± 0.2) ϊfk (%) 2Θ (± 0.2) d VIo {%)
. 7.9 9.9 100.0 17.8 5.0 37.6
11.9 7.5 12.5 19.2 4.6 13.7
14.1 6.3 10.5 19.5 4.5 45.5
15.1 5.9 13.9 20.9 4.3 12.1
15.7 5.6 13.9 24.9 3.6 19.5
17.5 5.1 23.6
20: angle of diffraction, d: distance within each crystal face, I/Io (%): relative intensity of peak
Example 9: Preparation of clopidogrel (+)-(lS)-camphor-10-sulfonate (polymorphic form B2)
Ig of clopidogrel free base was dissolved in 10 ml of ethyl acetate, and 0.72g of (+)-(lS)-camphor-10-sulfonic acid and lOmg of the polymorphic form
B2 obtained in Example 8 were added thereto. Then, the mixture was quickly cooled to a temperature ranging from 0 to 5 °C , and then, it was kept at that temperature for one night while intermittently stirring. The precipitates formed were filtered, washed with cool ethyl acetate and dried at 50 °C , to obtain 1 ,43g of the title compound (yield: 83%) as an white crystal.
Example 10: Preparation of clopidogrel (+)-(lS)-camρhor-10-sulfonate (polymorphic form B3)
Ig of clopidogrel (+)-(! S)-camphor-10-sulfonate was dissolved in 5 m# of methanol, and the solution was evaporated under a reduced pressure to remove the solvent therefrom. 15 mi of n-pentane was added to the foam residue and stirred for homogenization. The resulting solid was filtered, washed with n-pentane and dried with a nitrogen flow, to obtain 1.3g of the title compound (yield: 76%) as an white powder.
m.p.: starting at 65 °C and completed at 110°C water (Karl-Fisher titrator): below 0.5% optical purity (HPLC): 99.0% ee IR (KBr5 cm-1): 2956, 1745, 1479, 1438, 1229, 1147, 1035, 761, 615
DSC (10°C/min): no prominent heat absorption and discharge peaks (FIG. 11)
The result of powder X-ray diffraction analysis for the crystalline state of the polymorphic form B3 of the clopidogrel (+)-(lS)-camphor-10-sulfonate showed that it was amorphous having no characteristic diffraction pattern as shown in FIG. 10.
Test Example 1 : Optical purity measurement of acid addition salt of clopidogrel
Clopidogrel free bases having optical purities of about 90% ee, 95% ee and 98.5% ee, respectively, were prepared, and, clopidogrel hydrogen sulfates and clopidogrel (+)-(! S)-camphor-10-sulfonates were prepared using the clopidogrel free bases according to the procedures described in Comparative Example 1 and Example 2, respectively. The optical purities of the acid addition salts obtained were measured under HPLC condition C, and the extents of optical purity improvement are shown in Table 4. <Table 4>
Figure imgf000020_0001
As shown in Table 4, the optical purity of the clopidogrel camphorsulfonate according to the present invention was markedly enhanced during the process of preparing same, while that of clopidogrel hydrogen sulfate was not improved.
Clopidogrel is liable to be partially racemized to its levorotatory isomer, and thus, a plurality of purification steps is required to achieve a pharmaceutically acceptable optical purity. However, the inventive clopidogrel camphorsulfonate meets the pharmaceutical optical purity requirements without separate purification steps.
Test Example 2: Water-solubility measurement of acid addition salt of clopidogrel
The camphorsulfonate polymorphic form Al obtained in Example I5 the camphorsulfonate polymorphic form Bl obtained in Example 2, the hydrogen sulfate obtained in Comparative Example 1 and the benzenesulfonate obtained in Comparative Example 2 were each dissolved in unionized water until saturated. The amounts of clopidogrel in the resulting solutions were measured under HPLC condition A, and the results are shown in Table 5. <Table 5>
Figure imgf000021_0001
As shown in Table 5, the water-solubility of the clopidogrel camphorsulfonate according to the present invention was lower than that of hydrogen sulfate or benzenesulfonate, but such water-solubility level is more than sufficient for use in a pharmaceutical composition.
Test Example 3: Stability test of acid addition salt of clopidogrel under moist and heated condition
The camphorsulfonate polymorphic form Al obtained in Example I5 the camphorsulfonate polymorphic form Bl obtained in Example 2, the hydrogen sulfate obtained in Comparative Example 1 and the benzenesulfonate obtained in Comparative Example 2 were each subjected to a condition of 60±2°C and 75±5% relative humidity for a period of 28 days to test their stabilities. The changes of the assay of the acid addition salts of clopidogrel, and the amounts of hydro lyzed impurities and levorotatory isomers thereof and the water content thereof were measured at 7, 14, 21 and 28 days relative to that of the initial day (0) using HPLC. The results are shown in Tables 6 to 9 and FIGs. 12 to 15, respectively. <Table 6>
Figure imgf000022_0001
<Table 9>
Figure imgf000023_0001
As shown in Tables 6 to 9 and FIGs. 12 to 15, the inventive clopidogrel camphorsulfonate and its polymorphic forms were less hygroscopic, and more stable against moisture or heat, as compared to hydrogen sulfate and benzenesulfonate, which suggests that there is no significant decline in the amount of optically pure clopidogrel even after storage under a severe condition for a long period. These results confirm that a pharmaceutical composition comprising the inventive clopidogrel camphorsulfonate is more stable than conventional acid addition salts.
The inventive clopidogrel camphorsulfonate and its polymorphic forms may be formulated alone or in a combination with pharmaceutically acceptable additives, according to any of the conventional methods used to prepare soft or hard capsules and tablets.
The following Preparation Examples are intended to further illustrate the present invention without limiting its scope.
Preparation Example 1 : Soft or hard capsule A gelatin capsule was prepared using the following ingredients: Quantitvfmg/capsule)
Clopidogrel camphorsulfonate 129
(polymorphic form Bl)
Lactose 90
Corn starch 25
Silicon dioxide colloid 4
Magnesium stearate 2
Total 250
Preparation Example 2: Tablet
A tablet was prepared using the following ingredients:
Ouantitydng/tablet)
Clopidogrel camphorsulfonate 129
(polymorphic form Bl)
Anhydrous lactose 90
Microcrystalline cellulose 20
Hydroxypropylcellulose 6
Polysorbate 2
Hydrogenated castor oil 1
Magnesium stearate 1
Solid polyethylene glycol 1
Total 250
As discussed above, the inventive clopidogrel camphorsulfonate and its polymorphic forms are very stable against moisture and heat. Accordingly, the inventive pharmaceutical composition comprising same can maintain a high purity of an active ingredient for a prolonged time, and it can be very useful in the prevention and treatment for platelet aggregation-associated diseases. While the invention has been described with respect to the above specific embodiments, it should be recognized that various modifications and changes may be made to the invention by those skilled in the art which also fall within the scope of the invention as defined by the appended claims.

Claims

WHAT IS CLAIMED IS:
1. A pharmaceutical composition for treating or preventing a platelet aggregation-associated disease, which comprises clopidogrel camphorsulfonate of formula (I) or its polymorphic forms as an active ingredient:
Figure imgf000026_0001
2. The pharmaceutical composition of claim 1, wherein the platelet aggregation-associated disease is stroke, cerebral arteriosclerosis, myocardial infarction, angina pectoris, arrhythmia, peripheral arteries disease or Burger's disease.
3. The pharmaceutical composition of claim 1, wherein the clopidogrel camphorsulfonate of formula (I) or its polymorphic forms is clopidogrel (-)- (lR)-camphor-10-sulfonate of formula (Ia) or its polymorphic forms:
Figure imgf000026_0002
4. The pharmaceutical composition of claim 3, wherein the polymorphic form of the clopidogrel (-)-(lR)-camphor-10-sulfonate is polymorphic form Al whose powder X-ray diffraction scan shows major peaks having 1/I0 values greater than 20% at 2θ of 8.2, 8.7, 11.2, 16.4, 17.0, 18.6, 19.1, 20.6, 22.7, 23.9, 24.3, 26.2, 27.3 and 36.9.
5. The pharmaceutical composition of claim 3, wherein the polymorphic form of the clopidogrel (-)-(lR)-camphor-10-sulfonate is polymorphic form A2 which is amorphous.
6. The pharmaceutical composition of claim 1, wherein the clopidogrel camphorsulfonate of formula (I) or its polymorphic forms is clopidogrel (+)- (1 S)-camphor- 10-sulfonic acid of formula (Ib) or its polymorphic forms :
Figure imgf000027_0001
7. The pharmaceutical composition of claim 6, wherein the polymorphic form of the clopidogrel (+)-(lS)-camphor-10-sulfonate is polymorphic form Bl whose powder X-ray diffraction scan shows major peaks having I/To values greater than 20% at 2θ of 8.3, 11.5, 13.0, 13.3, 14.1, 15.0, 17.1, 18.3, 18.9, 19.8, 21.4, 22.4, 25.1 and 26.0.
8. The pharmaceutical composition of claim 6, wherein the polymorphic form of the clopidogrel (+)-(lS)-camphor-10-sulfonate is polymorphic form B2 whose powder X-ray diffraction scan shows major peaks having I/Io values greater than 10% at 20 of 7.9, 11.9, 14.1, 15.1, 15.7, 17.5, 17.8, 19.2, 19.5, 20.9 and 24.9.
9. The pharmaceutical composition of claim 6, wherein the polymorphic form of the clopidogrel (+)-(lS)-camphor-10-sulfonate is polymorphic form B3 which is amorphous.
10. The pharmaceutical composition of claim I5 which is orally administered.
11. The pharmaceutical composition of claim I5 wherein the clopidogrel camphorsulfonate or its polymorphic forms is present in an amount ranging from 0.1 to 95% by weight based on the total weight of the composition.
12. The pharmaceutical composition of claim H5 wherein the clopidogrel camphorsulfonate or its polymorphic forms is present in an amount ranging from 1 to 70% by weight based on the total weight of the composition.
13. A method for preparing clopidogrel camphorsulfonate of formula (I) or its polymorphic forms, which comprises reacting clopidogrel of formula (II) with camphorsulfonic acid in an organic solvent:
Figure imgf000028_0001
14. The method of claim 13, wherein the organic solvent is selected from the group consisting of diethyl ether, diisopropyl ether, methyl t-butyl ether, methyl acetate, ethyl acetate, n-propyl acetate, isopropyl acetate, n-butyl acetate, isobutyl acetate, acetone, methyl ethyl ketone, methyl isobutyl ketone, tetrahydrofuran, 1,4-dioxane, isopropanol and a mixture thereof.
15. The method of claim 13, wherein the camphorsulfonic acid is employed in an amount ranging from 0.9 to 1.2 moles based on 1.0 mole of clopidogrel.
16. Polymorphic form Al of clopidogrel camphorsulfonate whose powder X- ray diffraction scan shows major peaks having 1/I0 values greater than 20% at 2Θ of 8.2, 8.7, 11.2, 16.4, 17.0, 18.6, 19.1, 20.6, 22.7, 23.9, 24.3, 26.2, 27.3 and 36.9.
17. Polymorphic form A2 of clopidogrel camphorsulfonate which is amorphous.
18. Polymorphic form Bl of clopidogrel camphorsulfonate whose powder X- ray diffraction scan shows major peaks having 1/I0 values greater than 20% at 2Θ of 8.3, 11.5, 13.0, 13.3, 14.1, 15.0, 17.1, 18.3, 18.9, 19.8, 21.4, 22.4, 25.1 and 26.0.
19. Polymorphic form B2 of clopidogrel camphorsulfonate whose powder X- ray diffraction scan shows major peaks having 1/I0 values greater than 10% at 20 of 7.9, 11.9, 14.1, 15.1, 15.7, 17.5, 17.8, 19.2, 19.5, 20.9 and 24.9.
20. Polymorphic form B3 of clopidogrel camphorsulfonate which is amorphous.
PCT/KR2007/001278 2006-03-17 2007-03-15 Pharmaceutical composition containing clopidogrel camphorsulfonate or polymorphic forms thereof WO2007108604A1 (en)

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Cited By (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2008034912A2 (en) * 2006-09-22 2008-03-27 Krka, Tovarna Zdravil, D.D., Novo Mesto Process for the synthesis of clopidogrel and new forms of pharmaceutically acceptable salts thereof

Citations (2)

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Publication number Priority date Publication date Assignee Title
US4847265A (en) * 1987-02-17 1989-07-11 Sanofi Dextro-rotatory enantiomer of methyl alpha-5 (4,5,6,7-tetrahydro (3,2-c) thieno pyridyl) (2-chlorophenyl)-acetate and the pharmaceutical compositions containing it
US6737411B2 (en) * 2002-08-02 2004-05-18 Teva Pharmaceutical Industries Ltd. Racemization and enantiomer separation of clopidogrel

Patent Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US4847265A (en) * 1987-02-17 1989-07-11 Sanofi Dextro-rotatory enantiomer of methyl alpha-5 (4,5,6,7-tetrahydro (3,2-c) thieno pyridyl) (2-chlorophenyl)-acetate and the pharmaceutical compositions containing it
US6737411B2 (en) * 2002-08-02 2004-05-18 Teva Pharmaceutical Industries Ltd. Racemization and enantiomer separation of clopidogrel

Cited By (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2008034912A2 (en) * 2006-09-22 2008-03-27 Krka, Tovarna Zdravil, D.D., Novo Mesto Process for the synthesis of clopidogrel and new forms of pharmaceutically acceptable salts thereof
WO2008034912A3 (en) * 2006-09-22 2008-08-07 Krka Tovarna Zdravil D D Novo Process for the synthesis of clopidogrel and new forms of pharmaceutically acceptable salts thereof

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