Pharmacologically Acceptable Salts of Clopidogrel

Abstract

The invention relates to polymorphous forms of (+)-(S)-clopidogrel hydrogen bromide, described as polymorphous “form A”, polymorphous “form B”, polymorphous “form C”, polymorphous “form D”, polymorphous “form E”, and polymorphous “form F”, in addition to polymorphous forms of (+)-(S)-clopidogrel napsylate, that are described as polymorphous “form A” and polymorphous “form B” and differ in the X-ray powder diffraction diagrams (XRPD) thereof. The invention also relates to the salts clopidogrel besylate, clopidogrel tosylate and clopidogrel oxalate, and to methods for the production thereof.

Description

The present invention refers to salts of Clopidogrel, especially new polymorphic forms of Clopidogrel-hydrobromide, as well as salts of Clopidogrel with benzene sulfonic acid (besylate), with para-toluene sulfonic acid (tosylate), with Naphthalene-2-sulfonic acid (napsylate) and with oxalic acid (oxalate).

Clopidogrel is a known pharmaceutically active compound. Clopidogrel is the dextrorotary S-enantiomer of alfa-(2-chlorophenyl)-6,7-dihydro-thieno[3,2-c]pyridine-5(4H)acetic acid-methyl ester.

The present invention also refers to a method of making these compounds and to pharmaceutically active compositions, which contain at least one compound of the present invention in a concentration known per se. The present invention further refers to the use of the new compounds and forms for the preparation of pharmaceutically active compositions, which contain at least one compound of the present invention in a pharmaceutically effective concentration.

EP 0 099 802 discloses the racemic mixture as well as both enantiomeric forms of Clopidogrel. EP 1 087 976 discloses further salts of Clopidogrel.

The present invention refers to six new polymorphic forms of (+)-(S)-Clopidogrel-hydrogenbromide, which are named herein as polymorphic “Form A”, polymorphic “Form B”, polymorphic “Form C”, polymorphic “Form D”, polymorphic “Form E”, and as polymorphic “Form F”, as well as two new polymorphic forms of (+)-(S)-Clopidogrel-napsylate, which are named herein as polymorphic “Form A” and polymorphic “Form B”. These polymorphic forms differ from each other in their powder-roentgen-diagrams (XRPD). The polymorphic forms of Clopidogrel hydrobromide in addition differ from each other by their infrared spectra. In the present description the XRPD-peaks are used for the characterization of the compounds.

The characteristic XRPD-peaks of Clopidogrel-hydrobromide of the polymorphic forms A, B, C, D, E and F and Clopidogrel napsylate of the polymorphic forms A and B are given in degree 29 with an exactness of ±0.2 degree 2Θ, and are, as listed in the following Table 1 und Table 2, at the following divergence angles.

TABLE 1
Clopidogrel
hydrobromide Form	Angle [2Θ°]:	Relative intensity
A	9.83	medium
	10.35	medium
	19.98	strong
	23.03	strong
B	9.49	medium
	10.39	medium
	12.87	medium
	19.53	strong
C	8.20	strong
	8.92	strong
D	9.76	medium
	10.40	week-medium
	19.50	strong
	23.01	strong
E	7.72	medium
	9.27	medium
	9.88	medium
	11.91	medium
F	12.48	strong
	15.89	medium
	20.16	strong
	21.97	strong

TABLE 2
Clopidogrel
napsylate Form	Angle [2Θ°]:	Relative intensity
A	8.59	medium-strong
	13.55	medium-strong
	19.00	medium-strong
	21.34	strong
B	7.67	medium
	8.41	strong
	9.05	medium
	10.00	medium

Clopidogrel hydrobromide of Form A is obtained either by combining hydrogen bromide (HBr) and Clopidogrel base in a suitable solvent and subsequent crystallization, or by recrystallization or crystal transformation from the suspension of any form of Clopidogrel hydrobromide from a suitable solvent or mixture of solvents. Suitable solvents are acetone, acetic acid ethyl ester, diisopropylether, tert.-butyl-methylether, methyl-isobutylketone, dichloromethane, toluene, isobutyronitrile, isopropanol, preferably at temperatures between 18° C. and 22° C., using a mixture of solvents containing methyl-isobutylketone und isopropanol, preferably in a weight-ratio of 4:1.

In this sense the invention refers to a method of making Clopidogrel hydrobromide of Form A, which is characterized in that Clopidogrel hydrobromide of any crystalline form is crystallized from a solvent or a mixture of solvents, comprising acetone, acetic acid ethyl ester, diisopropylether, tert.-butyl-methylether, methyl-isobutylketone, dichloromethane, toluene, isobutyronitrile, and/or isopropanol, preferably methyl-isobutylketone and/or isopropanol, preferably in a weight ratio of 4:1, within a temperature range of 18° C. to 22° C.

Clopidogrel hydrobromide of Form B is obtained by combining hydrogenbromide (HBr) and Clopidogrel base in a suitable solvent and subsequent crystallization, preferably by crystallizing from this solution by quickly crossing the saturation curves using techniques such as quick addition of an antisolvens or by evaporation crystallization, or by very quick cooling of the crystallization solution (shock cooling). Suitable solvents are acetone and dichloromethane. Suitable antisolvens are aliphatic hydrocarbons such as heptane or hexane.

The invention refers to a method of making Clopidogrel hydrobromide of Form B, which is characterized in that Clopidogrel hydrobromide of any crystalline form is crystallized from a suitable solvent, preferably acetone and/or dichloromethane, by quickly crossing the saturation curve, preferably by quick addition of an antisolvens, preferably of an aliphatic hydrocarbon, preferably heptane and/or hexane, or by evaporation crystallization, or by very quick cooling of the crystallization solution (shock cooling).

Clopidogrel hydrobromide of Form C is obtained either by combining HBr and Clopidogrel base in a suitable solvent and subsequent crystallization or by recrystallization or by crystal transformation from a suspension of any Form of Clopidogrel hydrobromide from a suitable solvent or mixture of solvents. A suitable solvent is acetonitrile.

The invention refers to a method of making Clopidogrel hydrobromide of Form C, which is characterized in that Clopidogrel hydrobromide of any crystalline Form is crystallized from acetonitrile.

Clopidogrel hydrobromide of Form D is obtained by either combining HBr and Clopidogrel base in a suitable solvent and subsequent crystallization or by recrystallization or by crystal transformation from a suspension of any Form of Clopidogrel hydrobromide from a suitable solvent or mixture of solvents, comprising acetone, acetic acid ethyl ester, diisopropylether, tert.-butyl-methylether, methyl-isobutylketone,—dichloromethane, Toluene, isobutyronitrile and/or isopropanol, preferably methyl-isobutylketone and/or isopropanol, preferably in a weight ratio of 4:1, within a temperature range from 30° C. to 60° C.

The invention refers to a method of making Clopidogrel hydrobromide of Form D, which is characterized in that Clopidogrel hydrobromide of any crystalline Form is crystallized from a solvent or a mixture of solvents, comprising acetone, acetic acid ethyl ester, diisopropylether, tert.-butyl-methylether, methyl-isobutylketone, dichloromethane, toluene, isobutyronitrile and/or isopropanol, preferably methyl-isobutylketone and/or isopropanol, preferably in a weight ratio of 4:1, within a temperature range from 30° C. to 60° C.

Clopidogrel hydrobromide of Form E is obtained either by combining of HBr and Clopidogrel base in a suitable solvent and subsequent crystallization or by crystallization of any Form of Clopidogrel hydrobromide from a suitable solvent or a mixture of solvents. Suitable solvents are mixtures of dichloromethane and aliphatic hydrocarbons. Especially preferred are long crystallization times of up to 24 hours, a working temperature range of 0° C. to 25° C. and crystallization of Form E by slow evaporation of the lower boiling solvent from the solvent mixture.

The invention refers to a method of making Clopidogrel hydrobromide of Form E, which is characterized in that Clopidogrel hydrobromide of any crystalline Form is crystallized from dichloromethane and/or an aliphatic hydrocarbon with a boiling point of preferably 60° C. to 125° C., preferably hexane, heptane or octane, preferably within a temperature range from 0° C. to 25° C., or by crystallization by slow evaporation of the lower boiling solvent from the solvent mixture at temperatures within the temperature range of 0° C. to 25° C. Preferred are long crystallization times of up to 24 hours.

Clopidogrel hydrobromide of Form F is obtained by combining HBr und Clopidogrel base in a suitable solvent and subsequent crystallization or by recrystallization of any Form of Clopidogrel hydrobromide from a suitable solvent or mixture of solvents, comprising acetone, acetic acid ethyl ester, diisopropylether, tert.-butyl-methylether, methyl-isobutylketone, dichloromethane, Toluene, isobutyronitrile and/or isopropanol. Preferred is methyl-isobutylketone and/or isopropanol, preferably in a weight ration of 4:1, whereby crystallization is carried out within a temperature range of −5° C. to +15° C. Preferred are long crystallization and stirring times of the solution and suspensions, preferably longer than 24 hours.

The invention refers to a method of making of Clopidogrel hydrobromide of Form F, which is characterized in that Clopidogrel hydrobromide of any crystalline Form is crystallized from a solvent or a mixture of solvents, comprising acetone, acetic acid ethyl ester, diisopropylether, tert.-butyl-methylether, methyl-isobutylketone, dichloromethane, toluene, isobutyronitrile and/or isopropanol, preferably methyl-isobutylketone and/or isopropanol, preferably in a weight ration of 4:1, within a temperature range of −5° C. to +15° C.

Clopidogrel also forms salts with selected organic sulfonic acids. The present invention therefore also refers to the salts Clopidogrel besylate, Clopidogrel tosylate, and Clopidogrel napsylate as Form A and Form B, as well as to Clopidogrel oxalate.

Clopidogrel besylate is obtained by combining equimolar amounts of benzenesulfonic acid and Clopidogrel base in a suitable solvent to react together. Suitable solvents are for example alcohols, ethers and/or nitrites. Preferred as a solvent is methanol. Preferably the compound is isolated by solvent abstraction, i.e. for example by removing the solvent by distillation or by spray drying.

Clopidogrel tosylate is obtained by combining equimolar amounts of para-toluenesulfonic acid with Clopidogrel base in a suitable solvent to react together. Suitable solvents are for example alcohols, ethers and/or nitrites. Preferred as a solvent is methanol at a working temperature of 20-25° C. Preferably the compound is isolated by solvent abstraction.

Clopidogrel napsylate Form A is obtained by combining equimolar amounts of naphthalene-2-sulfonic acid with Clopidogrel base in a suitable solvent and initiating crystallization by inoculating the crystallization solution with Clopidogrel napsylate Form A. Suitable solvents are for example primary and secondary alcohols, ethers, nitrites, toluene and aqueous solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight (<10% by weight). The suitable temperature working range is between 20° C. and 60° C. Preferred solvents are isopropanol, water, diisopropylether, especially preferred is isopropanol. Alternatively Clopidogrel napsylate Form A is obtained from other Clopidogrel salts (e.g. from Clopidogrel hydrobromide) by salt transformation in the presence of naphthalene-2-sulfonic acid salts (e.g. sodium-2-naphthylsulfonate). Suitable solvents are: isopropanol, diisopropylether, and aqueous solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight of water. The preferred working temperature range is also here 20° C. to 60° C.

Clopidogrel napsylate Form A is obtained directly and without inoculation, by reacting equimolar amounts of naphthalene-2-sulfonic acid with Clopidogrel base in a suitable solvent, as described in the foregoing paragraph, wherein said naphthalene-2-sulfonic acid has a purity of at least 99.5% by weight and preferably, wherein the content of sulfonic-1-sulfonic acid is less than 0.5% by weight.

Clopidogrel napsylate Form B is obtained by dissolving equimolar amounts of naphthalene-2-sulfonic acid with Clopidogrel base in a suitable solvent and initiating crystallization by inoculation with Clopidogrel napsylate Form B. Suitable solvents are primary and secondary alcohols, nitrites, toluene and/or aqueous solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight of water. Especially preferred is isopropanol as a solvent, a strongly over saturated crystallizing solution (>20%), a temperature working range from 15° C. to 20° C., as well as prolonged mixing times of up to 24 hours (crystallization and mixing of the suspension).

Alternatively Clopidogrel napsylate Form B is also obtained by salt transformation from other Clopidogrel salts (e.g. Clopidogrel hydrobromide) in the presence of naphthalene-2-sulfonic acid salts (e.g. sodium-2-naphthylsulfonate) as well as by recrystallization from Clopidogrel napsylate Form A by inoculating the solution with the Form B. Suitable solvents are isopropanol, diisopropylether, and aqueous solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight (<10% by weight) water, at a preferred temperature working range of 15° C. to 20° C. as well as prolonged mixing times of up to 24 hours (crystallizing and mixing of the suspension).

Clopidogrel napsylate Form B is obtained directly without inoculation by reacting equimolar amounts of naphthalene-2-sulfonic acid with Clopidogrel base in a suitable solvent, as described herein before, wherein the naphthalene-2-sulfonic acid used has a purity of less than 99.0% by weight and especially, if its content of naphthalene-1-sulfonic acid is higher than 1.0% by weight.

The present invention refers to the compound Clopidogrel oxalate. Clopidogrel oxalate is obtained by reacting equimolar amounts of oxalic acid with Clopidogrel base in a suitable solvent. Suitable solvents are for example alcohols, ethers, nitrites, and/or aqueous solvent mixtures with a water content of preferably less than 10% by weight of water. Preferred solvents are isopropanol, diisopropylether and solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight of water (<10% by weight). Preferably the compound is isolated by solvent abstraction. In the previous cases mentioned, the condition that the water content is less than 10% by weight is a preferred but not a critical limitation.

FIGS. 1-11 show the XRPD diagram of Clopidogrel HBr Form A (FIG. 1), Form B (FIG. 2), Form C (FIG. 3), Form D (FIG. 4), Form E (FIG. 5), Form F (FIG. 6), Clopidogrel besylate (FIG. 7), Clopidogrel tosylate (FIG. 8), Clopidogrel napsylate Form A (FIG. 9), Clopidogrel napsylate Form B (FIG. 10) und Clopidogrel oxalate (FIG. 11). The following examples illustrate the invention.

EXAMPLE 1

Clopidogrel Hydrobromide of Form A

160 g Clopidogrel base are dissolved in 260 g acetone. Hydrogen bromide gas (HBr) is being introduced into this solution under ice cooling (inside temperature: 0° C.-5° C.) until the pH-value of the solution (measured with humid indicator paper) is 2 (two). The formed suspension is left to warm up to 20° C. and is stirred for two hours. The solid is isolated using vacuum filtration and is washed with cold acetone. The humid product is dried under vacuum until it shows a constant weight. There are obtained 130 g Clopidogrel hydrobromide of Form A with the following properties:

HPLC content of Clopidogrel HBr: 100%

DSC: endothermic-maximum: 143° C.

IR (KBr pressed mass) [cm⁻¹ at % transmission]:

3484	67%;	3075	76%;	3005	58%;	2952	50%;	2704	59%;
2628	46%;	2476	21%;	1753	3%;	1593	73%;	1474	37%;
1437	17%;	1404	37%;	1349	42%;	1319	18%;	1297	20%;
1226	8%;	1180	22%;	1135	55%;	1056	37%;	983	59%;
965	45%;	919	65%;	885	75%;	845	46%;	789	61%;
762	24%;	740	30%;	706	51%;	626	86%;	597	72%;
534	78%;	454	70%.

XRPD [Cu Kα₁]:

Angle [2Θ°]: Relative intensity [%]
9.83         33
10.35        22
13.24        14
14.01        51
14.37        30
16.40        8
17.44        10
18.39        18
19.22        18
19.68        18
19.98        100
20.73        16
22.08        25
22.53        19
23.03        90
25.93        11
26.26        30
26.44        34
27.13        11
27.49        11
28.01        28
28.91        37
29.29        8
29.85        16
30.71        10
31.42        12
31.75        34
33.17        19
36.22        9
37.33        7
40.16        9
41.58        10
42.23        10
48.92        7

EXAMPLE 2

Clopidogrel Hydrobromide of Form B

10 g Clopidogrel hydrobromide are dissolved in 60 g acetone whereby the mixture is mildly warmed up until complete solution of the compound. The solution is evacuated under stirring in a large round bottom flask. A white residue of 10 g of Clopidogrel hydrobromide of the amorphous Form B is obtained with the following properties:

HPLC content of Clopidogrel HBr: 100%

DSC: endothermic-maximum: week minimum at about 130° C.

IR (KBr pressed mass) [cm⁻¹ at % transmission]:

3436	39%;	2952	50%;	2479	27%;	1754	3%;	1708	50%;
1636	69%;	1480	38%;	1437	13%;	1320	26%;	1296	26%;
1224	13%;	1179	25%;	1134	64%;	1056	46	1038	44%;
1011	47%;	963	63%;	917	78%;	883	76%;	843	60%;
788	68%;	762	26%;	727	41%;	627	79%;	597	65%;
531	76%;	455	67%.

XRPD [Cu Kα₁]:

Angle [2Θ°]: Relative intensity [%]
9.50         34.95
10.39        34.57
12.87        24.42
13.74        23.08
14.14        38.5
16.13        31.84
16.86        20.24
18.52        18.04
19.53        100
20.88        44.26
21.63        20.92
22.34        18.09
22.93        47.93
23.23        52.29
23.60        17.76
24.83        32.92
25.12        47.4
25.41        40.78
27.25        24.32
27.54        26.55
28.50        25.57
29.01        30.56
30.07        16.68
30.67        19.36
31.23        19.37
31.53        14.47
32.26        29.23
33.57        15.51
34.16        10.02
36.09        10.93
36.83        12.91
40.70        11.28
44.15        11.06
48.63        8.98
9.50         34.95

EXAMPLE 3

Clopidogrel Hydrobromide of Form C

13 g Clopidogrel hydrobromide are stirred in 30 ml acetonitrile for several hours at room temperature. The solid material is then isolated by vacuum filtration. The humid material is dried under vacuum until a constant weight. 11 g Clopidogrel hydrobromide of Form C are obtained having the following properties:

HPLC content of Clopidogrel HBr: 100%

DSC: endothermic-maximum: 145° C.

IR (KBr pressed mass) [cm⁻¹ at % transmission]:

3437	65%;	3064	48%;	3003	56%;	2952	51%;	2910	51%;
2533	24%;	1758	3%;	1593	77%;	1480	44%;	1439	21%;
1392	47%;	1348	44%;	1320	32%;	1295	12%;	1217	17%;
1178	18%;	1071	51%;	1031	44%;	1015	43%;	973	59%;
952	63%;	911	72%;	891	69%;	838	65%;	784	76%;
756	22%;	712	33%;	624	68%;	591	71%;	536	84%;
456	74%.

XRPD [Cu Kα₁]:

Angle [2Θ°]: Relative intensity [%]
8.20         63
8.92         100
13.91        21
14.76        21
15.07        22
16.67        52
18.52        45
19.42        17
20.49        22
21.31        27
21.62        23
22.49        14
22.88        25
23.31        28
24.46        74
25.83        55
26.87        25
27.60        25
27.96        21
28.81        15
29.66        18
30.60        22
32.67        22
37.51        11

EXAMPLE 4

Clopidogrel Hydrobromide of Form D

1 g Clopidogrel hydrobromide is stirred over night in 2 ml isopropanol at 40° C. The solid material is then isolated using vacuum filtration. The humid material is then dried under vacuum until constant weight. There are obtained 0.8 g Clopidogrel hydrobromide of Form D with the following properties:

HPLC content of Clopidogrel HBr: 100%

DSC: endothermic-maximum: 144° C.

IR (KBr pressed mass) [cm⁻¹ at % transmission]:

3483	58%;	3110	78%;	3075	82%;	3021	79%;	2906	61%;
2486	30%;	2362	34%;	1753	3%;	1484	58%;	1436	29%;
1391	47%;	1337	51%;	1316	46%;	1295	22%;	1260	47%;
1228	19%;	1188	35%;	1136	72%;	1061	57%;	1035	51%;
1009	45%;	967	66%;	944	63%;	903	72%;	845	69%;
787	84%;	748	39%;	733	38%;	708	52%;	622	82%;
597	76%;	542	91%;	484	87%;	454	80%.

XRPD [Cu Kα₁]:

Angle [2Θ°]: Relative intensity [%]
9.76         43
10.40        10
11.38        11
12.85        13
13.73        52
14.30        27
15.02        22
17.23        24
19.50        100
19.91        33
20.65        68
22.03        29
23.01        95
23.97        35
25.07        52
26.86        31
27.45        30
28.76        44
29.63        30
31.10        32

EXAMPLE 5

Clopidogrel Hydrobromide of Form E

13.5 g Clopidogrel hydrobromide are dissolved in 140 g dichloromethane. 82 g heptane (isomeric mixture) are added to the solution at room temperature and stirred over night under nitrogen gas. The solid material is isolated from the suspension obtained using vacuum filtration and is dried until constant weight. 13 g Clopidogrel hydrobromide of Form E are obtained having the following properties:

HPLC content of Clopidogrel HBr: 100%

DSC: endothermic-maximum: 125° C.

IR (KBr pressed mass) [cm⁻¹ at % transmission]:

3485	57%;	3007	64%;	2956	44%;	2908	41%;	2489	19%;
1748	3%;	1593	75%;	1481	40%;	1438	18%;	1397	46%;
1345	42%;	1321	31%;	1297	13%;	1263	43%;	1229	12%;
1180	26%;	1059	52%;	1034	43%;	1015	33%;	968	65%;
951	64%;	909	72%;	892	71%;	841	60%;	786	72%;
758	24%;	720	17%;	623	72%;	593	73%;	539	87%;
480	81%;	456	73%;	421	86%.

XRPD [Cu Kα₁]:

Angle [2Θ°]: Relative intensity [%]
7.72         41
9.27         47
9.88         65
11.91        51
14.28        41
15.45        42
16.91        34
20.65        32
21.10        59
21.38        71
22.17        50
23.15        68
24.11        86
25.36        52
25.87        100
26.96        43
28.74        64
29.74        39

EXAMPLE 6

Clopidogrel Hydrobromide of Form F

A mixture of 3500 g isopropanol and 620 g Clopidogrel hydrobromide of Form A are heated until a clear, slightly yellow solution is obtained (inside temperature (IT): 60° C.-65° C.). After quick cooling to an inside temperature of 10° C. there crystallizes spontaneously, optionally after inoculation, a white powdery mass, which is isolated by vacuum filtration and is dried until constant weight. 361 g Clopidogrel hydrobromide of Form F are obtained having the following properties: HPLC content of Clopidogrel HBr: 100%; DSC: endothermic-maximum: 107.6° C.

IR (KBr pressed mass) [cm⁻¹ at % transmission]:

3325	16%	3113	46%	3067	61%	3013	53%	3001	51%
2961	50%	2889	57%	2858	57%	2725	55%	2479	37%
2349	57%	2299	60%	2142	66%	1956	81%	1744	3%
1613	58%	1588	63%	1573	77%	1493	49%	1470	26%
1453	26%	1434	19%	1423	15%	1390	52%	1364	60%
1351	41%	1334	30%	1322	28%	1285	29%	1276	33%
1257	29%	1239	23%	1222	29%	1211	19%	1188	30%
1171	23%	1093	66%	1056	30%	1043	39%	1028	41%
1011	28%	984	62%	965	57%	955	60%	930	73%
918	78%	906	57%	877	75%	865	69%	842	48%
826	77%	786	53%	762	8%	729	19%	715	44%
672	82%	637	70%	598	47%	590	43%	530	42%
505	58%	485	59%	457	47%	434	76%	425	69%

XRPD [Cu Kα₁]:

Angle [2Θ°]: Relative intensity [%]
8.95         19
9.74         27
12.48        82
13.83        34
15.89        66
16.67        28
17.99        25
18.84        20
19.53        54
20.02        80
20.16        100
20.52        56
20.86        21
21.52        33
21.97        94
22.32        22
23.35        42
24.20        45
24.65        18
25.46        32
26.16        36
26.36        45
27.91        73
28.44        54
31.28        25
32.14        28
33.33        31
34.91        25
36.43        12
37.85        16
41.01        13

EXAMPLE 7

Clopidogrel Besylate

3.0 g benzenesulfonic acid and 5.5 g Clopidogrel base are dissolved in 30 ml methanol. The solvent is evaporated in vacuum. 8.5 g Clopidogrel besylate are obtained with the following properties:

HPLC content of Clopidogrel besylate: 100%

DSC: endothermic-maximum: none

IR (KBr pressed mass) [cm⁻¹ at % transmission]:

3437	28%;	3066	56%;	2957	42%;	2579	44%;	1752	3%;
1636	65%;	1593	76%;	1479	31%;	1444	14%;	1322	36%;
1226	3%;	1159	3%;	1122	4%;	1069	32%;	1034	11%;
1016	6%;	996	14%;	913	69%;	887	70%;	840	67%;
759	16%;	727	10%;	694	20%;	611	4%;	565	26%;
480	76%;	457	74%.

XRPD [Cu Kα₁]: no clear peaks detectable

EXAMPLE 8

Clopidogrel Tosylate

3.2 g para-toluenesulfonic acid and 5.5 g Clopidogrel base are dissolved in 30 ml methanol. The solvent is evaporated by vacuum. There remain 8.7 g Clopidogrel tosylate with the following properties:

HPLC content of Clopidogrel besylate: 100%

DSC: endothermic-maximum: none

IR (KBr pressed mass) [cm⁻¹ at % transmission]:

XRPD [Cu Kα₁]: no clear peaks detectable

EXAMPLE 9

Clopidogrel Napsylate, Form A

52.5 g sodium-2-naphthylsulfonate are dissolved in 430 ml dematerialized water under heating at about 75° C. A solution of 50 g Clopidogrel hydrogen sulfate in 200 ml water is added to the solution. The resulting mixture is cooled to room temperature and the upper oily phase is separated. The separated oil is dissolved in 230 g isopropanol. The obtained solution is dried with magnesium sulfate and diluted with 250 g diisopropylether. The solution is inoculated at a temperature of about 60° C. with Clopidogrel napsylate and stirred over night whilst cooling to room temperature. The solid material is isolated by vacuum filtration, washed with diisopropylether and dried under vacuum. 37 g Clopidogrel napsylate of Form A are obtained with the following properties:

HPLC content of Clopidogrel napsylate: 100%

DSC: endothermic maximum: 149° C.

IR (KBr pressed mass) [cm⁻¹ at % transmission]:

3438	57%;	2969	47%;	2672	63%;	2593	59%;	2362	72%;
1751	10%;	1595	79%;	1475	54%;	1438	53%;	1329	54%;
1301	59%;	1222	11%;	1171	3%;	1135	29%;	1090	21%;
1032	10%;	993	60%;	956	78%;	906	82%;	886	83%;
866	74%;	830	64%;	783	83%;	753	27%;	724	76%;
698	48%;	676	21%;	650	71%;	623	73%;	597	76%;
567	47%;	480	69%;	461	76%;	421	78%.

XRPD [Cu Kα₁]:

Angle [2Θ°]: Relative intensity [%]
6.79         32
8.27         33
8.59         59
12.44        21
12.62        22
13.07        31
13.55        62
16.87        59
17.24        63
18.25        14
19.00        71
19.69        52
20.02        19
20.24        47
21.34        100
21.82        17
22.40        42
22.72        19
23.02        50
23.27        25
23.65        47
24.75        49
25.09        33
25.34        56
25.85        18
27.11        25
27.61        19
28.12        22
32.14        15
32.55        20
32.97        14
35.10        11

EXAMPLE 10

Clopidogrel Napsylate, Form A

2.5 g sodium-2-naphthylsulfonate are dissolved in 60 ml of water. Suspended material is separated by filtration. 30 ml methanol and 2.9 g Clopidogrel hydrobromide are then added. The solution obtained is vigorously stirred and put under slight vacuum and kept at room temperature until about 50% by weight of the solvent has slowly evaporated. The white solid thus formed is isolated by vacuum filtration, washed with water and dried under vacuum until constant weight. 3 g Clopidogrel napsylate of Form A are obtained.

EXAMPLE 11

Clopidogrel Napsylate, Form B

A previously prepared hot solution (about 65° C.) of 82 g Clopidogrel napsylate Form A in 462 g isopropanol is cooled to 20-25° C. and inoculated with Clopidogrel napsylate Form B. The mixture is well stirred during 24 hours at 15-20° C. The solid is then isolated from the suspension by vacuum filtration. The filter cake is washed with isopropanol at 15-20° C. and dried in air at an inside temperature of 20-25° C. until constant weight is obtained. 70 g Clopidogrel napsylate, Form B, are obtained.

DSC: endothermic-maximum: 114.4° C.

XRPD [Cu Kα₁]:

Angle [2Θ°] Relative intensity [%]
7.67        21
8.41        100
9.05        27
10.00       34
11.58       30
15.03       25
16.39       35
16.86       18
17.41       20
17.75       26
18.35       36
18.75       48
19.21       85
19.91       47
20.81       23
21.70       37
22.78       21
23.33       27
23.95       36
25.01       30
25.35       27
25.95       27
26.13       45
26.69       27
28.29       23
30.36       17
33.65       15
34.62       16

EXAMPLE 12

Clopidogrel Oxalate

10 g Clopidogrel base and 3.1 g oxalic acid are dissolved in 100 ml dichloromethane. The solvent is evaporated under vacuum. There remains 13 g Clopidogrel oxalate with the following properties:

HPLC content of Clopidogrel oxalate: 100%

DSC: endothermic-maximum: none

Raman [cm−1, intensity]:

1737.5	week	1621.8	medium	1594.1	week	1576.0	week	1
1514.5	medium	1498.7	medium	1451.5	medium	1396.7	week	1
1329.7	week	1316.3	week	1281.7	week	1252.5	week	1
1192.9	week	1167.5	week	1135.3	week	1089.5	week	1
1004.6	week	917.9	week	867.7	week	847.6	medium
785.9	week	764.0	week	718.4	medium	687.9	week
670.3	week	635.1	medium	609.5	week	584.9	week
542.7	week	534.5	week	506.0	week	486.8	week
432.1	week	410.3	week

XRPD [Cu Kα₁]: no distinct peaks are obtained.

EXAMPLE 13

Clopidogrel Napsylate, Form A

170 g Clopidogrel base and 115 g naphthalene-2-sulfonic acid monohydrate are dissolved in 600 ml isopropanol at a 60° C. and slowly cooled. At 50° C. the clear solution is inoculated with Clopidogrel napsylate of Form A and further cooled at a rate of 10° C./h to room temperature. The crystals are isolated by vacuum filtration and dried under vacuum. There are obtained 223 g Clopidogrel napsylate of Form A.

Claims

1. Polymorphic forms of (+)-(S)-Clopidogrel-hydrogenbromide, which are named herein as polymorphic “Form A”, polymorphic “Form B”, polymorphic “Form C”, polymorphic “Form D”, polymorphic “Form E”, and as polymorphic “Form F”, and which differ from each other in their powder-roentgen-diagrams (XRPD), according to the characteristic peaks as listed in Table 1, given in degree 2Θ with an exactness of ±0.2 Grad 2Θ:

2. Polymorphic forms of (+)-(S)-Clopidogrel-napsylate, which are named herein as polymorphic “Form A” and polymorphic “Form B” and which differ from each other in their powder-roentgen-diagrams (XRPD), according to the characteristic peaks as listed in Table 2, given in degree 2Θ with an exactness of ±2 Grad 2Θ:

3. Method of making Clopidogrel hydrobromide of Form A according to claim 1, characterized in that Clopidogrel hydrobromide of any crystalline form is crystallized from a solvent or a mixture of solvents, comprising acetone, acetic acid ethyl ester, diisopropylether, tert.-butyl-methylether, methyl-isobutylketone, dichloromethane, toluene, isobutyronitrile, and/or isopropanol, preferably methyl-isobutylketone and/or isopropanol, preferably in a weight ratio of 4:1, within a temperature range of 18° C. to 22° C.

4. Method of making Clopidogrel hydrobromide of Form B according to claim 1, characterized in that Clopidogrel hydrobromide of any crystalline form is crystallized from a suitable solvent, preferably acetone and/or dichloromethane, by quickly crossing the saturation curve, preferably by quick addition of an antisolvens, preferably of an aliphatic hydrocarbon, preferably heptane and/or hexane, or by evaporation crystallization, or by very quick cooling of the crystallization solution (shock cooling).

5. Method of making Clopidogrel hydrobromide of Form C according to claim 1, characterized in that Clopidogrel hydrobromide of any crystalline Form is crystallized from acetonitrile.

6. Method of making Clopidogrel hydrobromide of Form D according to claim 1, characterized in that Clopidogrel hydrobromide of any crystalline Form is crystallized from a solvent or a mixture of solvents, comprising acetone, acetic acid ethyl ester, diisopropylether, tert.-butyl-methylether, methyl-isobutylketone, dichloromethane, toluene, isobutyronitrile and/or isopropanol, preferably methyl-isobutylketone and/or isopropanol, preferably in a weight ratio of 4:1, within a temperature range from 30° C. to 60° C.

7. Method of making Clopidogrel hydrobromide of Form E according to claim 1, characterized in that Clopidogrel hydrobromide of any crystalline Form is crystallized from dichloromethane and/or an aliphatic hydrocarbon with a boiling point of preferably 60° C. to 125° C., preferably hexane, heptane or octane, preferably within a temperature range from 0° C. to 25° C., or by crystallization by slow evaporation of the lower boiling solvent from the solvent mixture at temperatures within the temperature range of 0° C. to 25° C., preferably at long crystallization times of up to 24 hours.

8. Method of making of Clopidogrel hydrobromide of Form F according to claim 1, characterized in that Clopidogrel hydrobromide of any crystalline Form is crystallized from a solvent or a mixture of solvents, comprising acetone, acetic acid ethyl ester, diisopropylether, tert.-butyl-methylether, methyl-isobutylketone, dichloromethane, toluene, isobutyronitrile and/or isopropanol, preferably methyl-isobutylketone and/or isopropanol, preferably in a weight ration of 4:1, within a temperature range of −5° C. to +15° C.

9. The salts Clopidogrel besylate, Clopidogrel tosylate and Clopidogrel oxalate.

10. Method of making Clopidogrel besylate according to claim 9, characterized in that equimolar amounts of benzenesulfonic acid and Clopidogrel base are combined in a suitable solvent to react together, preferably in an alcohol, ether and/or nitrile, preferably in methanol, whereby the compound is preferably isolated by solvent abstraction, preferably by removing the solvent by distillation or by spray drying.

11. Method for making Clopidogrel tosylate according to claim 9, characterized in that equimolar amounts of para-toluenesulfonic acid are combined with Clopidogrel base in a suitable solvent to react together, preferably in an alcohol, ether and/or nitrile, preferably in methanol, preferably at a working temperature of 20-25° C., whereby the compound is preferably isolated by solvent abstraction.

12. Method of making Clopidogrel oxalate according to claim 9, characterized in that equimolar amounts of oxalic acid are reacted with Clopidogrel base in a suitable solvent, preferably in an alcohol, ether, a nitrile, and/or an aqueous solvent mixtures thereof, preferably in isopropanol and/or diisopropylether and aqueous solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight of water (<10% by weight), whereby the compound is isolated by solvent abstraction.

13. Method of making Clopidogrel napsylate Form A according to claim 2, characterized in that equimolar amounts of naphthalene-2-sulfonic acid are combined with Clopidogrel base in a suitable solvent and initiating crystallization by inoculating the crystallization solution with Clopidogrel napsylate Form A, preferably in primary and/or secondary alcohols, ethers, nitrites, toluene and aqueous solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight (<10% by weight), preferably at a temperature working range between 20° C. and 60° C., preferably in isopropanol-water mixtures, diisopropylether, preferred is isopropanol-water mixtures.

14. Method of making Clopidogrel napsylate Form A according to claim 2, characterized in that said Clopidogrel napsylate Form A is made from another Clopidogrel salt by salt transformation in the presence of naphthalene-2-sulfonic acid salts, preferably sodium-2-naphthylsulfonate, preferably from Clopidogrel hydrobromide, preferably in isopropanol, diisopropylether, and/or aqueous solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight of water preferably at a working temperature range of 20° C. to 60° C.

15. Method of making Clopidogrel napsylate Form A according to claim 2, characterized in that said Clopidogrel napsylate Form A is obtained directly and without inoculation, by reacting equimolar amounts of naphthalene-2-sulfonic acid with Clopidogrel base in a suitable solvent, preferably in isopropanol, diisopropylether, and/or aqueous solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight wherein said naphthalene-2-sulfonic acid has a purity of at least 99.5% by weight and preferably, wherein the content of naphthalene-1-sulfonic acid is less than 0.5% by weight.

16. Method of making Clopidogrel napsylate Form B according to claim 2, characterized in that equimolar amounts of naphthalene-2-sulfonic acid are dissolved with Clopidogrel base in a suitable solvent and crystallization is initiated by inoculation with Clopidogrel napsylate Form B, preferably in a primary and/or secondary alcohol, a nitrile, toluene and/or an aqueous solvent mixture, preferably thereof, with a water content of preferably less than 10% by weight of water, preferably in isopropanol as a solvent, preferably in a strongly over saturated crystallizing solution (>20%), at a temperature working range from 15° C. to 20° C.

17. Method of making Clopidogrel napsylate Form B according to claim 2, characterized in that said Clopidogrel napsylate Form B is obtained by salt transformation from another Clopidogrel salt, preferably Clopidogrel hydrobromide, in the presence of a naphthalene-2-sulfonic acid salt, preferably sodium-2-naphthylsulfonate, or by recrystallization from Clopidogrel napsylate Form A, by inoculating the solution with the Clopidogrel napsylate Form B, preferably in isopropanol and/or diisopropylether, and aqueous solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight (<10% by weight) of water, preferably at a temperature working range of 15° C. to 20° C.

18. Method of making Clopidogrel napsylate Form B according to claim 2, characterized in that said Clopidogrel napsylate Form B is obtained directly without inoculation by reacting equimolar amounts of naphthalene-2-sulfonic acid with Clopidogrel base in a suitable solvent, preferably isopropanol and/or diisopropylether, and/or aqueous solvent mixtures, preferably thereof, with a water content of preferably less than 10% by weight of water, wherein the naphthalene-2-sulfonic acid used has a purity of less than 99.0% by weight and preferably if its content of naphthalene-1-sulfonic acid is higher than 1.0% by weight.

19. Pharmaceutically active compositions which contain at least one compound according to claim 1 in a pharmaceutically effective concentration.

20. Use of the compounds according to claim 1 for the preparation of pharmaceutically active compositions which contain at least one of said compounds in a pharmaceutically effective concentration.