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Preparation method of Brivaracetam intermediate

A technology of chiral intermediates and equations, applied in the medical field, can solve problems such as unstable chemical properties, difficult to purchase, and expensive, and achieve the effect of optical purity and easier purification

Inactive Publication Date: 2019-10-22
重庆经致制药技术开发有限公司
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Problems solved by technology

This method mainly has the following shortcoming: the starting material of the first step needs to use (1R, 2S, 5R)-(-)menthol (S)-p-toluene sulfinate, and this raw material can not be purchased from the market, And the synthesis is difficult, the process is difficult, and the expensive rhodium catalyst is used
This method has the following disadvantages: the starting material (1R, 2R)-(-)-N, N'-dimethyl-1,2-cyclohexanediamine in the first step is expensive, and allyl dichloride It is difficult to buy phosphine in the market, and the third step requires the use of ozone, which requires very high production equipment
This method has the following disadvantages: the price of the starting material 2(5H)-furanone of the first step reaction is expensive; the starting material allyl p-toluene sulfinate is difficult to buy on the market, and if it is prepared by itself, its synthetic difficulty large, the process is difficult and the chemical properties are unstable, and it needs to be produced and used immediately, which brings uncertainty to the production. Therefore, considering the cost of raw materials and the operability of the process, although this method can finally obtain (R)- 4-Propyl-dihydrofuran-2-one, but it is difficult to apply to industrial production
[0010] The final products of these three methods still need to be separated and purified by chiral preparative columns, the steps are cumbersome, the production cost is high, and the industrial feasibility is poor.

Method used

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  • Preparation method of Brivaracetam intermediate
  • Preparation method of Brivaracetam intermediate
  • Preparation method of Brivaracetam intermediate

Examples

Experimental program
Comparison scheme
Effect test

Embodiment 1

[0047] Such as figure 1 Shown:

[0048] Preparation of the compound of formula (1): Add N,N-dimethylformamide into the reaction bottle, start stirring, add 0.662 mmol of potassium hydroxide, and lower the temperature in the bottle to 0°C. Add 0.662 mmol of diethyl malonate, add 0.662 mmol of bromopropane, and keep warm at 0°C for 4 to 6 hours. After the reaction, slowly add 400 g of tap water and 360 g of ethyl acetate to the reaction solution and stir for 30 minutes. Stand still and separate to obtain an organic layer. Concentrate the organic layer under reduced pressure to dryness to obtain the compound of formula (1).

[0049] Preparation of the compound of formula (2): Add N,N-dimethylformamide into the reaction flask, start stirring and add 0.494 mmol of potassium hydroxide, after the addition is complete, cool down to 0°C, add 0.494 mmol of the compound of formula (1), add 0.494 Mmol tert-butyl bromoacetate, keep warm at 0°C for 2-3 hours. After the reaction, slowly add...

Embodiment 2

[0056] Such as figure 1 Shown:

[0057] Preparation of the compound of formula (1): Add dimethyl sulfoxide into the reaction bottle, start stirring, add 1.324 mmol potassium carbonate, and lower the temperature inside the bottle to 45°C. Add 0.662 mmol of diethyl malonate, add 1.324 mmol of bromopropane, and keep warm at 45° C. for 4 to 6 hours. After the reaction, slowly add 400 g of tap water and 360 g of ethyl acetate to the reaction solution and stir for 30 minutes. Stand still and separate to obtain an organic layer. Concentrate the organic layer under reduced pressure to dryness to obtain the compound of formula (1).

[0058] Preparation of the compound of formula (2): Add dimethyl sulfoxide etc. into the reaction flask, start stirring and add 0.988 mmol of sodium carbonate, after the addition is complete, cool down to 45°C, add 0.494 mmol of the compound of formula (1), add 0.988 mmol of For tert-butyl bromoacetate, keep warm at 45 for 2 to 3 hours. After the reactio...

Embodiment 3

[0065] Such as figure 1 Shown:

[0066] Preparation of the compound of formula (1): add tetrahydrofuran to the reaction bottle, start stirring, add 0.728mmol of sodium hydroxide, lower the temperature in the bottle to 20°C, add 0.662mmol of diethyl malonate, add 0.728mmol of bromopropane , keep warm at 20°C and react for 4-6 hours. After the reaction, slowly add 400 g of tap water and 360 g of ethyl acetate to the reaction solution and stir for 30 minutes. Stand still and separate to obtain an organic layer. Concentrate the organic layer under reduced pressure to dryness to obtain the compound of formula (1).

[0067] Preparation of the compound of formula (2): Add tetrahydrofuran into the reaction flask, start stirring and add 0.543 mmol of sodium hydroxide, after the addition is complete, cool down to 20°C, add 0.494 mmol of compound of formula (1), and add 0.543 mmol of tert-butyl bromoacetate Ester, keep warm at 20°C for 2-3 hours. After the reaction, slowly add 600 g o...

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Abstract

The invention discloses a preparation method of a Brivaracetam intermediate, wherein the reaction equation is shown as follows: diethyl malonate, bromopropane and an aprotic polar solvent are used forpreparing a compound of formula (1) under the action of an alkali; the compound of formula (1), tert-butyl bromoacetate and an aprotic polar solvent are used to prepare a compound of formula (2) under the action of an alkali; the compound of formula (2) and a polar solvent are used to prepare a compound of formula (3) under the action of an alkali; the compound of formula (3) is used to prepare acompound of formula (4) at high temperature; the compound of formula (4) and a polar solvent are used to prepare a compound of formula (5) under the action of an alkali; the compound of formula (5) and the resolving agent prepare the compound of formula (6) under the resolving solvent; the compound of formula (6) and a reducing agent are subjected to reduction reaction and hydrolysis reaction toprepare a compound of the formula (7). According to the invention, conventional raw materials are selected and can be prepared through conventional reactions, the optical purity materials are easier to purify, and the method is suitable for large-scale industrial production.

Description

technical field [0001] The invention relates to the medical field, in particular to a preparation method of a chiral intermediate of Buvaracetam. Background technique [0002] Brivaracetam is a third-generation epilepsy drug developed by Belgian UCB company. It is a new type of synaptic vesicle protein 2 compound (SV2 compound) high-affinity ligand, and it is also effective for voltage-dependent sodium ion channels. Certain inhibitory effect. In 2005, brivaracetam was approved by the FDA and the European Union for the treatment of rare myoclonic seizures. In February 2016, the US FDA approved brivaracetam as an add-on treatment for other drugs for epilepsy patients over 16 years old partial seizures. During the chemical synthesis of Buvaracetam, the preparation of the chiral intermediate (R)-4-propyl-dihydrofuran-2-one is a key part of the synthesis of Buvaracetam. [0003] There are several methods for preparing chiral (R)-4-propyl-dihydrofuran-2-one in the prior art. Ho...

Claims

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Application Information

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Patent Type & Authority Applications(China)
IPC IPC(8): C07D307/33
CPCC07D307/33
Inventor 李倩金加平余孟君
Owner 重庆经致制药技术开发有限公司
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