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动态控制反馈调节机制可提高工程大肠杆菌中的 NADPH 通量和木糖醇生物合成。

Dynamic control over feedback regulatory mechanisms improves NADPH flux and xylitol biosynthesis in engineered E. coli.

机构信息

Department of Chemistry, Duke University, USA.

Department of Biomedical Engineering, Duke University, USA.

出版信息

Metab Eng. 2021 Mar;64:26-40. doi: 10.1016/j.ymben.2021.01.005. Epub 2021 Jan 16.

Abstract

We report improved NADPH flux and xylitol biosynthesis in engineered E. coli. Xylitol is produced from xylose via an NADPH dependent reductase. We utilize 2-stage dynamic metabolic control to compare two approaches to optimize xylitol biosynthesis, a stoichiometric approach, wherein competitive fluxes are decreased, and a regulatory approach wherein the levels of key regulatory metabolites are reduced. The stoichiometric and regulatory approaches lead to a 20-fold and 90-fold improvement in xylitol production, respectively. Strains with reduced levels of enoyl-ACP reductase and glucose-6-phosphate dehydrogenase, led to altered metabolite pools resulting in the activation of the membrane bound transhydrogenase and an NADPH generation pathway, consisting of pyruvate ferredoxin oxidoreductase coupled with NADPH dependent ferredoxin reductase, leading to increased NADPH fluxes, despite a reduction in NADPH pools. These strains produced titers of 200 g/L of xylitol from xylose at 86% of theoretical yield in instrumented bioreactors. We expect dynamic control over the regulation of the membrane bound transhydrogenase as well as NADPH production through pyruvate ferredoxin oxidoreductase to broadly enable improved NADPH dependent bioconversions or production via NADPH dependent metabolic pathways.

摘要

我们报告了在工程大肠杆菌中提高了 NADPH 通量和木糖醇生物合成。木糖醇是通过 NADPH 依赖的还原酶从木糖生产的。我们利用两阶段动态代谢控制来比较两种方法来优化木糖醇生物合成,一种是计量方法,其中竞争通量减少,另一种是调节方法,其中关键调节代谢物的水平降低。计量方法和调节方法分别使木糖醇产量提高了 20 倍和 90 倍。降低烯酰-ACP 还原酶和葡萄糖-6-磷酸脱氢酶水平的菌株导致代谢物池发生变化,从而激活膜结合转氢酶和 NADPH 生成途径,该途径由丙酮酸铁氧还蛋白氧化还原酶与 NADPH 依赖的铁氧还蛋白还原酶偶联,导致 NADPH 通量增加,尽管 NADPH 池减少。这些菌株在仪器化生物反应器中以 86%的理论产率从木糖生产出 200g/L 的木糖醇。我们期望通过丙酮酸铁氧还蛋白氧化还原酶对膜结合转氢酶以及 NADPH 产生的调节进行动态控制,从而广泛实现改善的 NADPH 依赖性生物转化或通过 NADPH 依赖性代谢途径进行生产。

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