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构建辅酶A旁路以扩大产物范围并提高埃利希途径的选择性。

Engineering a Coenzyme A Detour To Expand the Product Scope and Enhance the Selectivity of the Ehrlich Pathway.

作者信息

Black William B, King Edward, Wang Yixi, Jenic Ana, Rowley Andrew T, Seki Kosuke, Luo Ray, Li Han

出版信息

ACS Synth Biol. 2018 Dec 21;7(12):2758-2764. doi: 10.1021/acssynbio.8b00358. Epub 2018 Nov 20.

Abstract

The Ehrlich pathway is a major route for the renewable production of higher alcohols. However, the product scope of the Ehrlich pathway is restricted, and the product selectivity is suboptimal. Here, we demonstrate that a Coenzyme A (CoA) detour, which involves conversion of the 2-keto acids into acyl-CoAs, expands the biological toolkit of reaction chemistries available in the Ehrlich pathway to include the gamut of CoA-dependent enzymes. As a proof-of-concept, we demonstrated the first biosynthesis of a tertiary branched-alcohol, pivalcohol, at a level of ∼10 mg/L from glucose in Escherichia coli, using a pivalyl-CoA mutase from Xanthobacter autotrophicus. Furthermore, engineering an enzyme in the CoA detour, the Lactobacillus brevis CoA-acylating aldehyde dehydrogenase, allowed stringent product selectivity. Targeted production of 3-methyl-1-butanol (3-MB) in E. coli mediated by the CoA detour showed a 3-MB:side-product (isobutanol) ratio of >20, an increase over the ratios previously achieved using the conventional Ehrlich pathway.

摘要

埃利希途径是可再生生产高级醇的主要途径。然而,埃利希途径的产物范围有限,且产物选择性欠佳。在此,我们证明了一条辅酶A(CoA)迂回途径,该途径涉及将2-酮酸转化为酰基辅酶A,从而扩展了埃利希途径中可用的反应化学的生物工具包,使其包括一系列依赖辅酶A的酶。作为概念验证,我们利用自养黄色杆菌的新戊酰辅酶A变位酶,在大肠杆菌中从葡萄糖首次生物合成了叔支链醇新戊醇,产量约为10 mg/L。此外,对CoA迂回途径中的一种酶——短乳杆菌CoA酰化醛脱氢酶进行工程改造,可实现严格的产物选择性。由CoA迂回途径介导的大肠杆菌中3-甲基-1-丁醇(3-MB)的靶向生产显示,3-MB与副产物(异丁醇)的比例>20,高于先前使用传统埃利希途径所达到的比例。

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