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A kind of preparation method of (1r, 2s) and (1s, 2r)-bedaquiline

A bedaquiline and solution technology, which is applied in the field of preparation of and-bedaquiline, can solve the problems of many reaction steps, increased high-pressure hydrogenation steps, danger and the like, and achieves less residual impurities, improved production efficiency, and improved reaction steps. less effect

Active Publication Date: 2019-10-18
JIANGSU TIANHE PHARMA CO LTD
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Problems solved by technology

[0013] Among the above synthetic methods, there are many problems in the first method, such as many reaction steps and extremely low yield, the manufacturing cost is very high, and there is no practical application value; the four optical isomer mixtures in the original research patent of the second method are separated, The yield of (1R, 2S)-bedaquiline is still very low; there are many reaction steps in method three, and the ratio of the four optical isomers has not been reported; in method four, a high-pressure hydrogenation step is added, which has certain dangers, and Ratio of target optical isomers not improved

Method used

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  • A kind of preparation method of (1r, 2s) and (1s, 2r)-bedaquiline
  • A kind of preparation method of (1r, 2s) and (1s, 2r)-bedaquiline
  • A kind of preparation method of (1r, 2s) and (1s, 2r)-bedaquiline

Examples

Experimental program
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Effect test

Embodiment 1

[0034]Add 30mL of anhydrous dichloromethane, 4.44g of (1R, 2R)-bedaquiline and (1S, 2S)-bedaquiline into a 500mL three-neck flask, blow nitrogen, stir and cool to -70℃~-78℃ Slowly add 1.36g of boron trifluoride·diethyl ether complex within 10min, keep the temperature constant, add 15mL of 2mol / L sodium hydroxide solution after 15min of reaction, raise the temperature to room temperature, and stir the solution at room temperature for 30min, Remove the water phase, wash the dichloromethane layer with 60mL of saturated sodium chloride solution, and then dry and concentrate the dichloromethane layer to obtain an oily product. The ratio of (B+B') is 62 / 38;

[0035] Then add 25mL of tetrahydrofuran to this oil, heat to reflux, and then cool to room temperature, a white solid and mother liquor are precipitated, the white solid is filtered off, and the filtered solid is (1R, 2R)-bedaquiline and (1S, 2S )-bedaquiline, after concentrating the mother liquor to obtain an oily substance, ...

Embodiment 2

[0046] Add 41mL of anhydrous dichloromethane, 5.99g of (1R,2R)-bedaquiline and (1S,2S)-bedaquiline mixture into a 500mL three-necked flask, blow nitrogen, stir and cool to -70°C~-78°C ℃, slowly add 3.71g of boron trifluoride·diethyl ether complex within 10min, keep the temperature constant, add 28mL of 2mol / L sodium hydroxide solution after 15min of reaction, raise the temperature to room temperature, and stir the solution at room temperature for 30min , remove the water phase, wash the dichloromethane layer with 80mL saturated sodium chloride solution, and then dry and concentrate the dichloromethane layer to obtain an oily product. The ratio of / (B+B') is 63 / 37;

[0047] Then add 25mL of tetrahydrofuran to this oil, heat to reflux, and then cool to room temperature, a white solid and mother liquor are precipitated, the white solid is filtered off, and the filtered solid is (1R, 2R)-bedaquiline and (1S, 2S )-bedaquiline, after concentrating the mother liquor to obtain an oil...

Embodiment 3

[0049] Add 36mL of anhydrous dichloromethane, 5.33g of (1R, 2R)-bedaquiline and (1S, 2S)-bedaquiline mixture into a 500mL three-neck flask, blow nitrogen, stir and cool to -70°C ~ -78°C ℃, slowly add 1.63g of boron trifluoride·diethyl ether complex within 10min, keep the temperature constant, add 18mL of 2mol / L sodium carbonate solution after 15min of reaction, raise the temperature to room temperature, and stir the solution at room temperature for 30min, Remove the water phase, wash the dichloromethane layer with 60mL of saturated sodium chloride solution, and then dry and concentrate the dichloromethane layer to obtain an oily product. The ratio of (B+B') is 62 / 38;

[0050] Then add 25mL of tetrahydrofuran to this oil, heat to reflux, and then cool to room temperature, a white solid and mother liquor are precipitated, the white solid is filtered off, and the filtered solid is (1R, 2R)-bedaquiline and (1S, 2S )-bedaquiline, after concentrating the mother liquor to obtain an ...

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Abstract

The invention discloses a method for preparing (1R, 2S)-bedaquiline and (1S, 2R)-bedaquiline and belongs to the technical field of chemical synthesis. The method comprises the steps of subjecting (1R,2R)-bedaquiline and (1S, 2S)-bedaquiline to a Lewis acid action to form carbenium ions, then, subjecting the carbenium ions to action by OH<-> in an alkaline solution to form novel chiral tertiary alcohol, and then, carrying out resolution, thereby preparing (1R, 2S)-bedaquiline. According to the method, the number of reaction steps is small, the production efficiency is greatly increased, the (1R, 2S)-bedaquiline of relatively high yield is easy to obtain, and thus, the industrial production is facilitated; and meanwhile, the impurity residual is low, the purity of target products is high, and dangerous steps such as high-pressure hydrogenation are not required to be added, so that the entire production process is high in safety.

Description

technical field [0001] The invention belongs to the technical field of chemical synthesis, and in particular relates to a preparation method of (1R, 2S) and (1S, 2R)-bedaquiline. Background technique [0002] MDR-TB is a bacterial disease that is resistant to isoniazid and rifampicin, as well as any fluoroquinolones and any second-line injectable anti-TB drugs (amikacin, kanamycin, or capreomycin ) have drug-resistant tuberculosis. In December 2012, the U.S. FDA accelerated the approval of Johnson & Johnson's (1R, 2S)-bedaquiline fumaric acid drug for the treatment of drug-resistant tuberculosis, fumaric acid (1R, 2S)-bedaquiline Daquinoline kills Mycobacterium tuberculosis by inhibiting the ATP synthase of Mycobacterium tuberculosis, its 50% cure time is 13 weeks, and the time of 80% cure rate is 6 months, combined with drug (2-4 Compared with other drugs), the cure rate of this drug is greatly improved, and the treatment cycle is greatly shortened. The structural formul...

Claims

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Application Information

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Patent Type & Authority Patents(China)
IPC IPC(8): C07D215/227C07B57/00C07B53/00
Inventor 赵学清赵云德朱林飞郑治尧廖伟科刘磊
Owner JIANGSU TIANHE PHARMA CO LTD
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