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探索细菌羧酸还原酶用于双功能羧酸的还原。

Exploring Bacterial Carboxylate Reductases for the Reduction of Bifunctional Carboxylic Acids.

机构信息

Department of Chemical Engineering and Applied Chemistry, University of Toronto, 200 College Street, ON, M5S 3E5, Canada.

Midwest Center for Structural Genomics and Structural Biology Center, Biosciences Division, Argonne National Laboratory, Argonne, IL, 60439, USA.

出版信息

Biotechnol J. 2017 Nov;12(11). doi: 10.1002/biot.201600751. Epub 2017 Sep 5.

Abstract

Carboxylic acid reductases (CARs) selectively reduce carboxylic acids to aldehydes using ATP and NADPH as cofactors under mild conditions. Although CARs attracts significant interest, only a few enzymes have been characterized to date, whereas the vast majority of CARs have yet to be examined. Herein the authors report that 12 bacterial CARs reduces a broad range of bifunctional carboxylic acids containing oxo-, hydroxy-, amino-, or second carboxyl groups with several enzymes showing activity toward 4-hydroxybutanoic (4-HB) and adipic acids. These CARs exhibits significant reductase activity against substrates whose second functional group is separated from the carboxylate by at least three carbons with both carboxylate groups being reduced in dicarboxylic acids. Purified CARs supplemented with cofactor regenerating systems (for ATP and NADPH), an inorganic pyrophosphatase, and an aldo-keto reductase catalyzes a high conversion (50-76%) of 4-HB to 1,4-butanediol (1,4-BDO) and adipic acid to 1,6-hexanediol (1,6-HDO). Likewise, Escherichia coli strains expressing eight different CARs efficiently reduces 4-HB to 1,4-BDO with 50-95% conversion, whereas adipic acid is reduced to a mixture of 6-hydroxyhexanoic acid (6-HHA) and 1,6-HDO. Thus, our results illustrate the broad biochemical diversity of bacterial CARs and their compatibility with other enzymes for applications in biocatalysis.

摘要

羧酸还原酶(CARs)在温和条件下使用 ATP 和 NADPH 作为辅助因子选择性地将羧酸还原为醛。尽管 CARs 引起了极大的兴趣,但迄今为止仅对少数几种酶进行了表征,而绝大多数 CARs尚未被研究。在此,作者报告 12 种细菌 CARs 可还原含有羰基、羟基、氨基或第二个羧基的广泛的双功能羧酸,其中几种酶对 4-羟基丁酸(4-HB)和己二酸具有活性。这些 CARs 对其第二个官能团与羧酸盐之间至少相隔三个碳原子的底物表现出显著的还原酶活性,并且在二羧酸中还原两个羧酸盐基团。用辅因子再生系统(用于 ATP 和 NADPH)、无机焦磷酸酶和醛酮还原酶补充纯化的 CARs,可催化 4-HB 高转化率(50-76%)转化为 1,4-丁二醇(1,4-BDO),以及将己二酸高转化率(50-76%)转化为 1,6-己二醇(1,6-HDO)。同样,表达八种不同 CAR 的大肠杆菌菌株可将 4-HB 高效还原为 1,4-BDO,转化率为 50-95%,而己二酸被还原为 6-羟基己酸(6-HHA)和 1,6-HDO 的混合物。因此,我们的结果说明了细菌 CARs 的广泛的生化多样性及其与其他酶在生物催化中的兼容性。

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