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Preparation method of high chiral purity lactam intermediate and brivaracetam

A technology for intermediates and lactams, applied in the preparation of high chiral purity lactam intermediates, in the field of preparation of brivaracetam, can solve the problems of cumbersome steps, high activity of intermediates, easy occurrence of racemization, etc., and achieves simple operation. Safe, simple separation process, improved selectivity

Inactive Publication Date: 2018-06-01
YANGZHOU AORUITE PHARMA CO LTD +1
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Problems solved by technology

[0005] At present, the preparation process of buvaracetam is mainly divided into three categories. One is the process represented by the original research UCB, which requires chiral chromatographic columns to separate isomers, which requires high equipment and greatly increases production costs. For example, patent CN1882535A discloses a A preparation method of buvaracetam, the final obtained is a mixture of buvaracetam and its diastereoisomers, which needs to pass through (CHIRALPAK AD 20um) chiral stationary phase, n-hexane / ethanol (45 / 55, V / V) is the eluent, and the above-mentioned mixture can be separated by chromatography to obtain the higher purity of Buvaracetam, which cannot be produced on a large scale
One is chiral source method synthesis. Taking CN106432030A as an example, this kind of method has the disadvantages of long reaction route, high activity of intermediates, difficulty in purification, easy occurrence of racemization in the reaction process, etc., which is not conducive to quality control and cost control. For the resolution method, the lactam intermediate is resolved by enzymes, chemical reagents, etc., but this type of method generally has many shortcomings such as long routes and cumbersome steps, especially the chemical resolution method. The introduction of the resolution agent has a great impact on the quality of the product. Control is particularly disadvantageous, therefore, there is a need for a simple and cost-effective process for the preparation of high-purity brivaracetam to obtain brivaracetam of high optical purity

Method used

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  • Preparation method of high chiral purity lactam intermediate and brivaracetam
  • Preparation method of high chiral purity lactam intermediate and brivaracetam
  • Preparation method of high chiral purity lactam intermediate and brivaracetam

Examples

Experimental program
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Effect test

Embodiment 1

[0027] Preparation of Compound D

[0028] Add citric acid monohydrate (50g 0.237mol) to a 1L four-necked reaction flask, stir to dissolve in 500ml of water, add 5g of 5% palladium carbon, stir, add 50g (0.237mol) of the compound of chemical formula C, control the temperature at 30°C, replace with hydrogen, The hydrogen pressure was 2 bar, and the reaction was stirred. After 20 hours of reaction, the TLC was controlled until the raw materials disappeared completely, the reaction was stopped, filtered, 2M hydrochloric acid was adjusted to pH=2, the temperature was lowered to 5°C, filtered, and washed with 50ml of water to obtain 46g of white solid. 100ml of methyl tert-butyl ether was recrystallized to obtain 41g (0.192mol) of white solid, yield 81%, HPLC 99.52%, de% 99.2%.

Embodiment 2

[0030] Preparation of Compound D

[0031] Add 12g (0.115mol) of malonic acid, 250ml of water and 250ml of isopropanol into a 1L four-necked reaction flask, stir to dissolve, add 5g of 10% palladium carbon, stir, add 50g (0.237mol) of the compound of chemical formula C, and control the temperature at 30°C. Replace with hydrogen, the hydrogen pressure is 4 bar, stir the reaction, after 20 hours of reaction, TLC control until the raw material disappears completely, stop the reaction, filter, adjust the pH=2 with 2M hydrochloric acid, cool down to 5°C, filter, wash with 50ml of water, the crude product is washed with methanol 100 ml of tert-butyl ether was recrystallized to obtain 44 g (0.206 mol) of white solid, yield 87%, HPLC 99.23%, de% 99.1%.

Embodiment 3

[0033] Preparation of Compound D

[0034] Add 20g (0.095mol) of citric acid monohydrate to a 500ml reaction bottle, stir to dissolve in 100ml of water, add 0.5g of 10% palladium carbon, add 1,3,5-triazine-2,4,6-trithione trisodium Add 0.0001g of salt, stir after adding, then add 10g (0.047mol) of the compound of chemical formula C, control the temperature at 5°C, replace with hydrogen, the pressure of hydrogen is 5bar, stir and react, after 20 hours of reaction, control in TLC until the raw materials disappear completely, stop the reaction , filtered, adjusted to pH=2 with 2M hydrochloric acid, cooled to 5°C, filtered, washed with 20ml of water, and the crude product was recrystallized with 20ml of methyl tert-butyl ether to obtain 8.1g (0.038mol) of white solid, yield 82%, HPLC95 .6%, de% 99.1%.

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Abstract

The invention discloses a preparation method of a high chiral purity lactam intermediate and brivaracetam. The preparation method of the lactam intermediate structural formula compound D includes thesteps of: in a solvent, by means of a heavy metal catalyst and a chiral inducer, conducting hydrogenation reduction on a compound C into the lactam intermediate D. The lactam intermediate structural formula compound D provided by the invention can be made into brivaracetam by only one step, the synthesis route is short, the reaction conditions are mild, the post-treatment is simple, the reaction yield is high, the chiral selectivity is good, and the production cost is low. In the reaction process, the conversion rate of the compound C reaches 81%, and the de value of the compound D reaches 99%or more, therefore the method is suitable for industrial production.

Description

technical field [0001] The invention relates to the field of organic synthesis. Specifically, the invention provides a method for preparing a lactam intermediate with high chiral purity and a method for preparing buvaracetam. Background technique [0002] Brivaracetam, the chemical name is (2S)-2-[(4R)-2-oxo-4-propyl-1-pyrrolidinyl]butanamide, and its structural formula is as follows: [0003] [0004] Brivaracetam is a third-generation antiepileptic drug developed by Belgian UCB Company, which was approved by EMEA and FDA in January and February 2016, respectively, for the treatment of partial seizures in adults and adolescents over 16 years old with epilepsy, With or without adjuvant therapy for secondary generalized seizures. [0005] At present, the preparation process of buvaracetam is mainly divided into three categories. One is the process represented by the original research UCB, which requires chiral chromatographic columns to separate isomers, which requires hi...

Claims

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Application Information

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Patent Type & Authority Applications(China)
IPC IPC(8): C07D207/27
CPCC07D207/27C07B2200/07
Inventor 于振鹏肖飞王国平戚淑娴高贺
Owner YANGZHOU AORUITE PHARMA CO LTD
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