Title of Invention

PROCESS FOR PREPARING TELMISARTAN

Abstract The invention relates to polymorphs of 4'-[2-n-propyl-4-methyl-6(1- methylbenzimidazol -2-yl) benzimidazol -1-ylmethyl] biphenyl-2-carboxylic acid (INN: telmisartan), and in particular the polymorphous form B of formula (I), characterized by an endothermic peak at 183 ± 2°C during thermal analysis by differential scanning calorimetry. The invention also relates to mixtures of said polymorphs, methods for producing telmisartan containing form B and to the use thereof in the preparation of a medicament.
Full Text FORM 2
THE PATENTS ACT, 1970
[39 OF 1970]
COMPLETE SPECIFICATION
[See Section 10; Rule 13]
"PROCESS FOR PREPARING TELMISARTAN"
BOEHRINGER INGELHEIM PHARMA GMBH & CO. KG, (formerly known as BOEHRINGER INGELHEIM PHARMA KG), a German company of D-55216 Ingelheim am Rhein, Germany,
The following specification particularly describes the nature of the invention and the manner in which it is to be performed:-

3 MAY 2005

The invention relates to polymorphs of 4"-[2-n-propyl-4-methyl- 6 -(1-methylbenzimidazol-2-yl)benzimidazol-1-ylmethyl]biphenyl-2-carboxylic acid (INN: telmisartan), particularly the polymorphic form B, mixtures of the polymorphs, processes for preparing telmisartan containing form B and the use thereof for preparing a pharmaceutical composition.
Background of the invention The compound telmisartan is known from European Patent EP 505 314 Bl and has the following chemical structure:

Telmisartan and the design physiologically acceptable salts thereof have valuable pharmacological properties. Telmisartan is an angiotensin antagonist, particularly an angiotensin-II-antagonist which by virtue of its pharmacological properties may be used for example to treat hypertension and cardiac insufficiency, to treat ischaemic peripheral circulatory disorders, myocardial ischaemia (angina), to prevent the progression of cardiac insufficiency after myocardial infarct, to treat diabetic neuropathy, glaucoma, gastrointestinal diseases and bladder diseases. Other possible therapeutic applications
2

I
can be found in EP (502314JB1, the contents of which are hereby referred to.
In the course of the synthesis of telmisartan, the final step of the synthesis comprises saponifying the tert.butyl ester (II) according to Diagram 1.
Me Me

Diagram 1:
The corresponding experimental procedure which may be carried out on a laboratory scale can be found in EP 502314 Bl. Surprisingly, however, it proved to be simple to transfer the method of synthesis already known to a large-scale industrial manufacturing process. The telmisartan synthesised on an industrial scale according to Diagram 1 is obtained after working up in the form of a product which has to be subjected to a further crystallisation step to complete the purification. In this obligatory crystallisation step the morphology of the end product which crystallises out leads to unforeseen problems.
The product which is precipitated as a solid in the form of long needles is difficult to filter, wash and isolate, is further characterised by a very long drying time on account of the presence of solvent and forms large, very hard fragments during the drying process. Grinding these fragments produces a dry powder which exhibits a strong tendency to electrostatic charging and is virtually impossible to pour.
3

The disadvantageous properties of a product as described above have always proved to be a serious obstacle to the large-scale manufacture of a compound, as reproducible manufacture of large amounts of the compound in highly pure form is only possible with considerable difficulty or with high additional technical costs.
The aim of the present invention is therefore to prepare telmisartan in a form which permits the large-scale synthesis, working up, purification and isolation of telmisartan in which the above disadvantages are overcome.
Detailed description of the invention Surprisingly, it has been found that telmisartan may occur as a solid in different crystalline modifications. Depending on the nature of the crystallisation process it may be converted into two different polymorphic forms A and B.
Polymorph A is a form of telmisartan which is obtainable according to the prior art, and which gives rise to the abovementioned problems in large-scale manufacture or purification, isolation and drying of the product.
The polymorphic form B of telmisartan which was surprisingly found, however, shows virtually no tendency to electrostatic charging, is easy to suction filter, centrifuge, wash and dry and is free-flowing even without being ground up.
The following procedure is used according to the invention to prepare the polymorphic form B of telmisartan.
Crude telmisartan product (crystallised for example from dimethylformamide, dimethylacetamide or the like) is taken


1(1
up, in a suitably sized stirring apparatus, optionally with 1-5 wt.-%, preferably with 3 wt.-% of activated charcoal in a mixture of solvents consisting of water, formic acid and a suitable organic solvent and then dissolved at elevated temperature, preferably at a temperature of from 50-90°C, most preferably at 60-80°C. According to the invention it is essential to use the solvent mixture of formic acid and water with an organic solvent which must satisfy the following criteria according to the invention. It must be capable_of forming a solution with the mixture of formic acid and water It
must be largely chemically inert relative to the mixture of formic acid _and water and it must be capable of being separated from the mixture of formic acid and water by
1$ distillation. Organic carboxylic acid esters ketone or
ethers may be used Acetone, methylethylketone, methyl acetate, ethyl acetate, ethyl formate, ethyleneglycol dimethylether or tetrahydrofuran may be mentioned by way of example. Acetone, methylethylketone, methyl acetate,
2d) ethyl acetate and THF are preferred according to the
invention, while ethyl acetate is particularly preferred. According to the invention, the mixture of solvents should be made up of 0.3-0.7 1 of water, 10-15 mol of formic acid and 0.3-0.9 1 of the organic solvent per mol of.
2$ telmisartan. A ratio of 0.4-0.6 1 of water, 11-13 mol of formic acid and 0-4-0.7 1 of the organic solvent based on 1 mol of telmisartan is preferred. A ratio of about 0.5 1 of water, about 11.5-12 mol of formic acid and about 0.5 1 of the organic solvent based on 1 mol of telmisartan is particularly preferred.



According to the invention,_ after the abovementioned heating, the solution obtained is filtered and washed with a mixture of the abovementioned organic solvent and formic acid. The washing solution may contain _0_.3-1. 0 mol, preferably 0 . 4-0 . 6 mol, most preferably about
5

0.5 mol of formic acid per mol of telmisartan. The quantity of washing solution will naturally depend on the quantity of dissolved telmisartan. According to the invention, 0.1-0.4, preferably 0.15-0.3, most preferably 0.2 1 of the organic solvent are used to each mol of telmisartan.
After the filter residue has been washed with the washing solution described above, the organic solvent is distilled
off as much as possible whilst water is added
simultaneously. The temperature is kept in the range from 60-100°C, preferably from 70-100°C. The total quantity of water added corresponds substantially to the total amount of solvent distilled off. Almost total distillation of the organic solvent is desirable according to the invention. Accordingly, the distillation is continued until water is also distilled off, partly azeotropically. The organic solvent distilled off may be used again in subsequent reactions, if necessary after removal of the aqueous
phase.
In order to precipitate the telmisartan-polymorphic B it is then cooled to a temperature in the range from 15-60°C, preferably to 20-30°C, and precipitated with a base. The quantity of base to be used depends on the amount of formic acid used. Preferably, 0-2 mol less base is added than there is formic acid present. Most preferably, 0.3-1.5 mol less base is added than there is formic acid present. It is most particularly preferred to add 0.5-1 mol less base than there is formic acid present. Suitable bases might be either aqueous solutions of potassium hydroxide, sodium hydroxide, lithium hydroxide or ammonia. It is also possible to use suitable organic bases such as triethylamine, diisopropylethylamine or DBU (diazabicycloundecene). Particularly preferred bases are the abovementioned aqueous solutions of the potassium


hydroxide, sodiuifl hydroxide, lithium hydroxide or ammonia, the aqueous solutions of ammonia being particularly important.
The product precipitated is centrifuged, washed with water and normally dri^d in vacuo at 120-125°C.
A sample taken directly after centrifuging and dried in a thin layer in a circulating air drier in the laboratory typically shows 3- content of 95,-99% of crystalline form E. After centrifugafcion, the product begins to change partially into form A depending on the temperature, pH, retention time, and water content, towards the end of the drying. Therefore, in working mixtures, ratios of form A to form B of at best about 10: 90 are obtained after drying, but ratios of 60:40=may also be obtained.
However, even a content of form B as low as this guarantees that the product will have the positive qualities required for large-scale production (e.g. a low tendency to electrostatic charging, a low tendency to clumping, free-flowing characteristics etc.). What is
essential to the invention in the crystallisation process mentioned above is that initially only form B is produced,
with its characteristic macroscopic crystalline form. This macroscopic crystalline form is largely retained under the drying conditions/ in spite of partial microscopic rearrangement into form A.
Other highly advantageous aspects of the procedure according to the invention are the high space/time yield of the present process and the high yield of pure telmisartan product, which can be isolated in virtually quantitative amounts.
The telmisartan of form A which can be obtained by the manufacturing process known from the prior art differs from the telmisartan obtainable according to the invention, which is characterised in that it contains some



15

polymorphic form B, in the advantageous qualities of the product already mentioned hereinbefore. Other distinguishing features will be described hereinafter.
Telmisartan of form A crystallises as long, fine or thin needles which cling together in a felt-like manner. The crystal modification of telmisartan of form B produces very compact cubic to spherical crystals which trickle like sand or silica gel.
The two polymorph forms A and B of telmisartan differ considerably in their melting point. Form B melts at 183 + /2oC (determined by DSC) , form A at 269+/-2°C (determined.by... DSC) . After melting, the lower-melting form B of telmisartan crystallises out again as form A. This results, for example, in the endothermic maximum at 183+/-2°C determined by DSC being followed by a characteristic exothermic maximum which reflects the crystallisation of the melt of form B into the high-melting form A. The DSC diagrams (DSC=Differential Scanning Calorimetry) obtained with a Mettler DSC-20, TA8000 system are shown in Figure 1.

The polymorphs A and B also differ in their IR spectrum.
2j5 On the basis of this difference, the IR spectroscopy may optionally be used for quantitative determination of the ratio of the two crystal modifications in the end product after drying. Pure polymorph A has a characteristic band at 81j5cm _1 in the IR spectrum. In polymorph B this oscillation is shifted to 830cm _1. Since these two characteristic bands of polymorphs A and B are sufficiently far apart, they are particularly suitable for the abovementioned quantitative determination of the ratio of the two crystal modifications.
The IR-spectroscopic characterisation of the two
polymorphic forms A and B was carried out using the
-&■


Nicolet FTIR Spectrometer Magna - IR 550 in KBr (2.5/xmol per 300 mg KBr; Nicolet software package OMNIC, version 1.20) .
The Examples which follow serve to illustrate purification and crystallisation processes carried out by way of example in order to prepare the polymorphic form B of telmisartan. They should be regarded purely as possible procedures described by way of example, without restricting the invention to their contents.
Example 1
205.6 kg of recrystallised telmisartan (recrystallised from dimethyl formamide or dimethylacetamide), 6.2 kg of activated charcoal, 205.6 1 of water, 211.6 kg of formic acid (99-100%) and 205.6 1 of ethyl acetate are placed in a 1200 1 stirring apparatus. The mixture is stirred for about 1 h at 70 - 80°C and then filtered into another 1200 1 stirring apparatus and washed with a mixture of 82.2 1 of ethyl acetate and 9.2 kg of formic acid (99-100%). About 308 1 of solvent are distilled off at 80 -100°C whilst simultaneously 3 08 1 of water are added. The mixture is then cooled to 20 - 30°C and precipitated by the metered addition of 313 kg of 25 % ammonia solution.
The product precipitated is centrifuged, washed with water
and dried at 120-125°C.
Yield : 200 kg telmisartan (97.3 % of theory)
Example 2
185 kg of recrystallised telmisartan (recrystallised from dimethylformamide or dimethylacetamide), 5.6 kg of activated charcoal, 185 1 of water, 190.4 kg of formic acid (99-100%) and 185 1 of tetrahydrofuran are placed in a 1200 1 stirring apparatus. The mixture is stirred for

9
about 1 h at 60 - 70°C and then filtered into another 1200 1 stirring apparatus and washed with a mixture of 74 1 of tetrahydrofuran and 8.3 kg of formic acid (99-100%). About 278 1 of solvent are distilled off at 70 - 100°C whilst simultaneously 278 1 of water are added. The mixture is then cooled to 20 - 30°C and precipitated by the metered addition of 281.5 kg of 25 % ammonia solution. The product precipitated is centrifuged.^ washed, with water and dried at 120-125°C. Yield : 180 kg telmisartan (97.3 % of theory)
Example 3
185 kg of recrystallised telmisartan (recrystallised from dimethylformamide or dimethylacetamide), 5.6 kg of
15 activated charcoal, 185 1 of water, 190.4 kg of formic
acid (99-100%) and 185 1 of methylethylketone are placed in a 1200 1 stirring apparatus. The mixture is stirred for about 1 h at 60 - 70°C and then filtered into another 1200 1 stirring apparatus and washed with a mixture of 74 1 of methylethylketone and 8.3 kg of formic acid (99-100%). About 278 1 of solvent are distilled off at 80 -100°C whilst simultaneously 278 1 of water are added. The mixture is then cooled to 20 - 30°C and precipitated by the metered addition of 281.5 kg of 25 % ammonia solution.
The product precipitated is centrifuged, washed with water and dried at 120-125°C. Yield : 178 kg of telmisartan (96.2 % of theory)
Comparison Example
150 kg of telmisartan (recrystallised from dimethylformamide or dimethylacetamide), 7.5 kg of activated charcoal, 750 1 of ethanol and 3 0 kg of 25% aqueous ammonia solution are placed in a 1200 1 stirring
filtered into another 1200 1 stirring apparatus and washed with 150 1 of ethanol. The mixture is heated to 70 -

80°C, 35 kg of glacial acetic acid are added and the mixture is stirred for a further 1.5 - 2 h at 75 - 80°C. The mixture is then cooled to 0 - 10°C and stirred for a further 2 h. The product precipitated is centrifuged, washed with 300 1 of ethanol and with 300 1 of water and dried at 70 - 90°C. Yield : 135 kg of telmisartan (90 % of theory) pure form A
In the preparation process according to the invention, as a result of the partial conversion of the polymorphic form B into the polymorphic form A during the drying process, telmisartan occurs as a pure substance in a mixture of two polymorphic forms. However, this does not affect the properties of the pharmaceutical composition, as in the course of the manufacture of telmisartan tablets, for example, the mixture of the polymorphic forms A and B is dissolved in 0.1 N NaOH solution and converted by spray drying into a homogeneous and totally amorphous granulate which is then subjected to the other tablet making steps. For more detailed information on the use of the products according to the invention for preparing a pharmaceutical composition, cf. EP 502314 Bl, the contents of which are hereby referred to.

WE CLAIM :
1. Process for preparing telmisartan (formula I), characterized in that

a) telmisartan is taken up in a mixture of solvents consisting of water, formic acid and an organic solvent selected from among organic carboxylic acid esters, ketones or ethers miscible therewith, heated, and the resulting solution is then filtered and washed with a mixture of organic solvent: and formic acid,
b) the organic solvent is distilled off, optionally while water is simultaneously added in metered amounts,
c) the telmisartan form B is precipitated out of the remaining solution by the addition of a base and,
d) the product precipitated is centrifuged, washed and dried.
2. Process as claimed in claim 1, wherein acetone, methylethylketone, methyl acetate, ethyl acetate, ethyl formate, ethyleneglycol dimethylether or tetrahydrofuran is used as the organic solvent.
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Documents:

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in-pct-2001-652-mum-abstract(3-5-2005).doc

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in-pct-2001-652-mum-cancelled pages(3-5-2005).pdf

in-pct-2001-652-mum-claims(granted)-(3-5-2005).doc

in-pct-2001-652-mum-claims(granted)-(3-5-2005).pdf

in-pct-2001-652-mum-correspondence(8-7-2005).pdf

in-pct-2001-652-mum-correspondence(ipo)-(4-7-2005).pdf

in-pct-2001-652-mum-drawing(3-5-2005).pdf

in-pct-2001-652-mum-form 13(5-5-2003).pdf

in-pct-2001-652-mum-form 19(5-5-2004).pdf

in-pct-2001-652-mum-form 1a(3-5-2005).pdf

in-pct-2001-652-mum-form 2(granted)-(3-5-2005).doc

in-pct-2001-652-mum-form 2(granted)-(3-5-2005).pdf

in-pct-2001-652-mum-form 3(3-5-2005).pdf

in-pct-2001-652-mum-form 3(6-6-2001).pdf

in-pct-2001-652-mum-form 5(6-6-2001).pdf

in-pct-2001-652-mum-form-pct-ipea-409(6-6-2001).pdf

in-pct-2001-652-mum-petition under rule 137(3-5-2005).pdf

in-pct-2001-652-mum-petition under rule 138(3-5-2005).pdf

in-pct-2001-652-mum-power of authority(3-5-2005).pdf


Patent Number 215601
Indian Patent Application Number IN/PCT/2001/00652/MUM
PG Journal Number 13/2008
Publication Date 28-Mar-2008
Grant Date 28-Feb-2008
Date of Filing 06-Jun-2001
Name of Patentee BOEHRINGER INGELHEIM PHARMA GMBH & CO. KG.
Applicant Address D-55216 INGELHEIM AM RHEIN, GERMANY
Inventors:
# Inventor's Name Inventor's Address
1 HEINRICH SCHNEIDER TANNENWEG 13, D-55218 INGELHEIM AM RHEIN, GERMANY
PCT International Classification Number C07D235/18
PCT International Application Number PCT/EP2000/000065
PCT International Filing date 2000-01-07
PCT Conventions:
# PCT Application Number Date of Convention Priority Country
1 199 01 921.2 1999-01-19 Germany