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β受体阻滞剂动力学拆分中的机械酶学:以普萘洛尔为例的研究

Mechanoenzymology in the Kinetic Resolution of β-Blockers: Propranolol as a Case Study.

作者信息

Gamboa-Velázquez Gonzalo, Juaristi Eusebio

机构信息

Departamento de Química, Centro de Investigación y de Estudios Avanzados, 07360 Ciudad de México, Mexico.

El Colegio Nacional, Luis González Obregón 23, Centro Histórico, 06020 Ciudad de México, Mexico.

出版信息

ACS Org Inorg Au. 2022 Apr 6;2(4):343-350. doi: 10.1021/acsorginorgau.1c00049. eCollection 2022 Aug 3.

Abstract

Recent advances in biotechnology, protein engineering, and enzymatic immobilization have made it possible to carry out biocatalytic transformations through alternative non-conventional activation strategies. In particular, mechanoenzymology (i.e., the use of the mechanical force produced by milling or grinding to activate a biotransformation) has become a new area in so-called "green chemistry", reshaping key fundaments of biocatalysis and leading to the exploration of enzymatic transformations under more sustainable conditions. Significantly, numerous chiral active pharmaceutical ingredients have been synthesized via mechanoenzymatic methods, boosting the use of biocatalysis in the synthesis of chiral drugs. In this regard and aiming to widen the scope of the young field of mechanoenzymology, a dual kinetic resolution of propranolol precursors was explored. The biocatalytic methodology mediated by Lipase B (CALB) and activated by mechanical force allowed the isolation of both enantiomeric precursors of propranolol with high enantiomeric excess (up to 99% ee), complete conversion ( = 50%), and excellent enantiodifferentiation ( > 300). Moreover, the enantiomerically pure products were used to synthesize both enantiomers of the β-blocker propranolol with high enantiopurity.

摘要

生物技术、蛋白质工程和酶固定化技术的最新进展使得通过替代性非传统活化策略进行生物催化转化成为可能。特别是,机械酶学(即利用研磨或粉碎产生的机械力来激活生物转化)已成为所谓“绿色化学”中的一个新领域,重塑了生物催化的关键基础,并促使人们在更可持续的条件下探索酶促转化。值得注意的是,许多手性活性药物成分已通过机械酶法合成,这推动了生物催化在手性药物合成中的应用。在这方面,为了拓宽机械酶学这一新兴领域的范围,人们探索了普萘洛尔前体的双动力学拆分。由脂肪酶B(CALB)介导并由机械力激活的生物催化方法能够以高对映体过量(高达99% ee)、完全转化(= 50%)和出色的对映体区分(> 300)分离出普萘洛尔的两种对映体前体。此外,对映体纯的产物被用于合成具有高对映体纯度的β受体阻滞剂普萘洛尔的两种对映体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d476/9955203/1795b142df86/gg1c00049_0002.jpg

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