Organic compounds -- part of the class 532-570 series – Organic compounds – Heterocyclic carbon compounds containing a hetero ring...
Reexamination Certificate
2001-05-31
2002-05-07
Owens, Amelia (Department: 1625)
Organic compounds -- part of the class 532-570 series
Organic compounds
Heterocyclic carbon compounds containing a hetero ring...
C549S292000
Reexamination Certificate
active
06384238
ABSTRACT:
FIELD OF THE INVENTION
This invention relates to a novel process for the acylation of sterically hindered alcohols which is one of the crucial steps in the process for the preparation of simvastatin and derivatives thereof as well as other related HMG-CoA reductase inhibitors. More particularly, this invention relates to a novel acylation process which is applicable in the preparation of simvastatin and derivatives thereof from alcohols of formula I (R representing a protective group).
BACKGROUND OF THE INVENTION
Lovastatin, pravastatin, simvastatin, mevastatin, atorvastatin, derivatives and analogs thereof are known as HMG-CoA reductase inhibitors and are used as antihypercholesterolemic agents. The majority of them are produced by fermentation using microorganisms of different species identified as species belonging to Aspergillus, Monascus, Nocardia, Amycolatopsis, Mucor or Penicillium genus, some are obtained by treating the fermentation products using the methods of chemical synthesis (simvastatin) or they are the products of total chemical synthesis.
In the literature several processes for the preparation of simvastatin are known which are mainly based on one of the two following basic principles.
A process of direct methylation of the 2-(S)-methylbutyryloxy side chain of lovastatin is disclosed in U.S. Pat. No. 4,582,915. That process is based on direct methylation of the 2-(S)-methylbutyryloxy side chain of lovastatin using a methyl alkyl amide and a methyl halide in a single step. The described process has certain disadvantages: the low level of conversion in the C-methylation step, low temperatures (−70 to −15° C.) required for the reaction to be carried out and a number of undesired side reactions of methylation occurring at other sites of the molecule as well as using of butyl lithium which produces an explosive reaction with water and is highly pyrogen at higher concentrations. With minor modifications the yields in the methylation step may be improved, however, the total yields remain relatively low. U.S. Pat. No. 4,820,850 discloses a process for methylation of the 2-(S)-methylbutyrylox side chain of lovastatin using a single charge of amide base and alkyl halide. The process disclosed therein involves six steps; despite the fact that the level of conversion is high in the methylation step, the process is not economical.
The second basic principle is de-esterification of the 2-methylbutyrate side chain of lovastatin and re-esterification wherein the desired 2,2-dimethylbutyrate (simvastatin) is formed. U.S. Pat. No. 4,444,784 discloses a process which comprises de-esterification of the 2-methylbutyrate side chain of lovastatin, protection of the 4-hydroxy group on the pyranone ring with t-butyldimethyl-chlorosilane, re-esterification with 2,2-dimethylbutyryl chloride and deprotection of the 4-hydroxy group. The reaction of re-esterification as described in the example is however very slow and requires 18 to 36 hours and a high temperature of 100° C., and the yields are very low. In addition, the reaction leads to a number of side products which are formed during the reaction since a protecting group is easily eliminated under these rigid conditions. Apart from side products, unconverted starting materials additionally complicate the isolation of pure simvastatin and lower the yield of the disclosed process.
EP 0 287 340 discloses an improvement of the acylation step in the above process which involves the addition of alkali metal bromides under the presence of dialkylaminopyridine as a catalyst in a solvent, preferably pyridine. The presumed mechanism of reaction is characterized by in situ generated reactive acylated intermediates such as the acyl bromides (a), a pyridinium complex (h) or a dialkylaminopyridinium complex (c), wherein X is a chloride ion or bromide ion. The reaction times are shorter (6 to 8 hours), and the temperatures required are much lower (from 25 to 75° C.).
SUMMARY OF THE INVENTION
It is an object of the present invention to provide a novel improved method for the acylation of sterically hindered alcohols which is applicable in the process for the preparation of simvastatin and derivatives thereof as well as other related HMG-CoA reductase inhibitors and exerts an excellent yield, is cheaper, less toxic and shows less side reactions.
This is accomplished by the present invention.
According to the present invention, there is provided a process for the preparation of compounds of formula
wherein R
1
and R
2
are independently hydrogen or alkyl with one to ten C atoms, R
3
and R
4
are independently hydrogen or alkyl with one to three C atoms, R
5
is hydrogen, halogen or alkyl with one to three C atoms, R
6
is a protecting group; which comprises combining of acyl chlorides of the formula
in the presence of a halide of the formula KX
n
in which K is Li, Mg, Ca, Zn, Fe, Ni or Al and X is Cl or Br, and n is 1, 2 or 3 (depending on the cation charge of K) with an alcohol of formula
in an organic solvent in the absence of dialkylaminopyridine as a catalyst to yield a compound of formula:
DESCRIPTION OF THE INVENTION
In our developmental and research work, contrary to the statements in EP 0 287 340, we have surprisingly found the following:
Acylation reactions are accomplished equally well with LiCl and LiBr; in case the former is used slightly higher temperature (80 to 95° C.) is required for the equivalent effectiveness.
Acylation reactions with NaBr and KBr are carried out much slower and with more side effects than with LiBr and LiCl.
Acylation reactions are also successfully carried out with other suitable metal halides. MgBr
2
and MgCl
2
are effective wherein under the same conditions the reactions with MgBr
2
proceed slightly faster than with MgCl
2
. MgCl
2
catalyses slightly slower than LiCl. MgBr
2
and LiBr are approximately comparable by the reaction rate. Similar reactivity has been observed when ZnBr
2
and ZnCl
2
are used. The results were very good with NiCl
2
and FeCl
2
. The use of AlCl
3
and especially of BF
3
showed the tendency of a formation of impurities.
The rate of acylation reaction and its effectiveness remain almost unchanged if a catalyst from the group of N,N-dialkylaminopyridines or the group of cycloalkylated aminopyridines is not added as disclosed in EP 0 287 340. If any of the above chlorides (Mg, Zn, Li) is used without addition of the catalyst, the intermediate (c), as disclosed in EP 0 237 340, is not generated and the reaction is carried oat equally successfully as in the examples described in this invention. Regarding the statements from the cited patent, the conclusion may be drawn that the acylation reaction would proceed slower than that described in U.S. Pat. No. 4,444,784 wherein the catalyst from the group of N,N-dialkylaminopyridines or cycloalkylated aminopyridines was not added.
As it is evident from EP 0 287 384, in situ generated reactive acyl bromides (a) being more reactive than acyl chlorides, and reactive acylated intermediates (b) and (c) are responsible for acceleration of the acylation reaction. However, the results of our experiments suggest that the, progress of the reaction depends on the cation in the halide added as a catalyst rather than on the bromide ion from the alkali metal bromide and in situ generated more reactive acyl bromides. We have also found that the progress of the reaction primarily depends on the size of cation, positive charge per cation area unit and on its ability for complexing with the carbonyl group in the acyl chloride. The cation site is important primarily because it may be sterically hindered during the generation of reactive intermediate II (only sufficiently small cations are capable of generating reactive acylated intermediates), and the reactivity of generated acylated intermediate II depends on charge and the ability of complexing with the carbonyl group.
X may denote Cl or Br
K may denote Li, Mg, Ca, Zn, Fe, Ni or Al
n may denote 1, 2 or 3 depending on cation charge
The molecule KX
n
is approached to the car
Bromberg & Sunstein LLP
Lek Pharmaceutical and Chemical Company d.d.
Owens Amelia
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