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通过与左乙拉西坦对映体共结晶拆分卤代扁桃酸。

Resolution of Halogenated Mandelic Acids through Enantiospecific Co-Crystallization with Levetiracetam.

机构信息

School of Chemical Engineering, East China University of Science and Technology, Shanghai 200237, China.

出版信息

Molecules. 2021 Sep 12;26(18):5536. doi: 10.3390/molecules26185536.

Abstract

The resolution of halogenated mandelic acids using levetiracetam (LEV) as a resolving agent via forming enantiospecific co-crystal was presented. Five halogenated mandelic acids, 2-chloromandelic acid (2-ClMA), 3-chloromandelic acid (3-ClMA), 4-chloromandelic acid (4-ClMA), 4-bromomandelic acid (4-BrMA), and 4-fluoromandelic acid (4-FMA), were selected as racemic compounds. The effects of the equilibrium time, molar ratio of the resolving agent to racemate, amount of solvent, and crystallization temperature on resolution performance were investigated. Under the optimal conditions, the resolution efficiency reached up to 94% and the enantiomeric excess (%e.e.) of ()-3-chloromandelic acid was 63%e.e. All five halogenated mandelic acids of interest in this study can be successfully separated by LEV via forming enantiospecific co-crystal, but the resolution performance is significantly different. The results showed that LEV selectively co-crystallized with enantiomers of 2-ClMA, 3-ClMA, 4-ClMA, and 4-BrMA, while it co-crystallized with enantiomers of 4-FMA. This indicates that the position and type of substituents of racemic compounds not only affect the co-crystal configuration, but also greatly affect the efficiency of co-crystal resolution.

摘要

本文介绍了一种使用左乙拉西坦(LEV)作为拆分剂通过形成对映选择性共晶拆分卤代扁桃酸的方法。选择 5 种卤代扁桃酸(2-氯扁桃酸(2-ClMA)、3-氯扁桃酸(3-ClMA)、4-氯扁桃酸(4-ClMA)、4-溴扁桃酸(4-BrMA)和 4-氟扁桃酸(4-FMA))作为外消旋化合物。考察了平衡时间、拆分剂与外消旋体的摩尔比、溶剂用量和结晶温度对拆分性能的影响。在最佳条件下,拆分效率高达 94%,()-3-氯扁桃酸的对映体过量(%ee)为 63%ee。本研究中感兴趣的所有 5 种卤代扁桃酸均可通过 LEV 形成对映选择性共晶成功分离,但拆分性能差异显著。结果表明,LEV 选择性地与 2-ClMA、3-ClMA、4-ClMA 和 4-BrMA 的对映体共结晶,而与 4-FMA 的对映体共结晶。这表明外消旋化合物的位置和取代基类型不仅影响共晶构型,而且极大地影响共晶拆分的效率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6e86/8465588/09ed4b670763/molecules-26-05536-g001.jpg

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