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构建用于合成非天然蛋氨酸前体 2,4-二羟基丁酸的合成代谢途径。

Construction of a synthetic metabolic pathway for biosynthesis of the non-natural methionine precursor 2,4-dihydroxybutyric acid.

机构信息

LISBP, Université de Toulouse, CNRS, INRA, INSA, Toulouse, France, 135 Avenue de Rangueil, F-31077 Toulouse, France.

TWB, 3 rue des Satellites, Canal Biotech Building 2, Toulouse F-31400, France.

出版信息

Nat Commun. 2017 Jun 20;8:15828. doi: 10.1038/ncomms15828.

Abstract

2,4-Dihydroxybutyric acid (DHB) is a molecule with considerable potential as a versatile chemical synthon. Notably, it may serve as a precursor for chemical synthesis of the methionine analogue 2-hydroxy-4-(methylthio)butyrate, thus, targeting a considerable market in animal nutrition. However, no natural metabolic pathway exists for the biosynthesis of DHB. Here we have therefore conceived a three-step metabolic pathway for the synthesis of DHB starting from the natural metabolite malate. The pathway employs previously unreported malate kinase, malate semialdehyde dehydrogenase and malate semialdehyde reductase activities. The kinase and semialdehyde dehydrogenase activities were obtained by rational design based on structural and mechanistic knowledge of candidate enzymes acting on sterically cognate substrates. Malate semialdehyde reductase activity was identified from an initial screening of several natural enzymes, and was further improved by rational design. The pathway was expressed in a minimally engineered Escherichia coli strain and produces 1.8 g l DHB with a molar yield of 0.15.

摘要

2,4-二羟基丁酸(DHB)是一种具有很大潜力的多功能化学合成前体。值得注意的是,它可以作为蛋氨酸类似物 2-羟基-4-(甲硫基)丁酸的化学合成前体,从而瞄准动物营养领域的一个巨大市场。然而,DHB 的生物合成不存在天然代谢途径。因此,我们从天然代谢产物苹果酸出发,设计了一个三步骤的 DHB 合成代谢途径。该途径利用了以前未报道过的苹果酸激酶、苹果酸半醛脱氢酶和苹果酸半醛还原酶活性。激酶和半醛脱氢酶活性是基于对具有空间位阻相似底物的候选酶的结构和机制知识进行合理设计获得的。苹果酸半醛还原酶活性是从几种天然酶的初步筛选中鉴定出来的,并通过合理设计进一步得到了改善。该途径在经过最小工程化改造的大肠杆菌菌株中表达,可生产 1.8 g/L 的 DHB,摩尔产率为 0.15。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a8e7/5481828/eadeee34d48c/ncomms15828-f1.jpg

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