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酶工具箱:新型对映体互补亚胺还原酶

Enzyme toolbox: novel enantiocomplementary imine reductases.

作者信息

Scheller Philipp N, Fademrecht Silvia, Hofelzer Sebastian, Pleiss Jürgen, Leipold Friedemann, Turner Nicholas J, Nestl Bettina M, Hauer Bernhard

机构信息

Institute of Technical Biochemistry, University of Stuttgart, Allmandring 31, 70569 Stuttgart (Germany).

出版信息

Chembiochem. 2014 Oct 13;15(15):2201-4. doi: 10.1002/cbic.201402213. Epub 2014 Aug 27.

Abstract

Reducing reactions are among the most useful transformations for the generation of chiral compounds in the fine-chemical industry. Because of their exquisite selectivities, enzymatic approaches have emerged as the method of choice for the reduction of C=O and activated C=C bonds. However, stereoselective enzymatic reduction of C=N bonds is still in its infancy-it was only recently described after the discovery of enzymes capable of imine reduction. In our work, we increased the spectrum of imine-reducing enzymes by database analysis. By combining the currently available knowledge about the function of imine reductases with the experimentally uncharacterized diversity stored in protein sequence databases, three novel imine reductases with complementary enantiopreference were identified along with amino acids important for catalysis. Furthermore, their reducing capability was demonstrated by the reduction of the pharmaceutically relevant prochiral imine 2-methylpyrroline. These novel enzymes exhibited comparable to higher catalytic efficiencies than previously described enzymes, and their biosynthetic potential is highlighted by the full conversion of 2-methylpyrroline in whole cells with excellent selectivities.

摘要

还原反应是精细化工行业中生成手性化合物最有用的转化反应之一。由于其出色的选择性,酶促方法已成为还原C=O和活化C=C键的首选方法。然而,C=N键的立体选择性酶促还原仍处于起步阶段——直到最近发现能够还原亚胺的酶后才被描述。在我们的工作中,通过数据库分析增加了亚胺还原酶的种类。通过将目前关于亚胺还原酶功能的现有知识与蛋白质序列数据库中未经过实验表征的多样性相结合,鉴定出了三种具有互补对映体选择性的新型亚胺还原酶以及对催化重要的氨基酸。此外,通过还原与药物相关的前手性亚胺2-甲基吡咯啉证明了它们的还原能力。这些新型酶表现出与先前描述的酶相当或更高的催化效率,并且通过在全细胞中以优异的选择性将2-甲基吡咯啉完全转化突出了它们的生物合成潜力。

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