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通过代谢工程优化 NADH/NADPH 平衡,从木糖生产 1,2,4-丁三醇在酿酒酵母中。

Optimization of 1,2,4-butanetriol production from xylose in Saccharomyces cerevisiae by metabolic engineering of NADH/NADPH balance.

机构信息

Graduate School of Science, Technology and Innovation, Kobe University, Kobe, Japan.

Biomolécules et Biotechnologies Végétales, EA 2106, Département of Agronomie, productions animale et végétale et agro-alimentaire, Université de Tours, Tours, France.

出版信息

Biotechnol Bioeng. 2021 Jan;118(1):175-185. doi: 10.1002/bit.27560. Epub 2020 Sep 29.

Abstract

1,2,4-Butanetriol (BT) is used as a precursor for the synthesis of various pharmaceuticals and the energetic plasticizer 1,2,4-butanetriol trinitrate. In Saccharomyces cerevisiae, BT is biosynthesized from xylose via heterologous four enzymatic reactions catalyzed by xylose dehydrogenase, xylonate dehydratase, 2-ketoacid decarboxylase, and alcohol dehydrogenase. We here aimed to improve the BT yield in S. cerevisiae by genetic engineering. First, the amount of the key intermediate 2-keto-3-deoxy-xylonate as described previously was successfully reduced in 41% by multiple integrations of Lactococcus lactis 2-ketoacid decarboxylase gene kdcA into the yeast genome. Since the heterologous BT synthetic pathway is independent of yeast native metabolism, this manipulation has led to NADH/NADPH imbalance and deficiency during BT production. Overexpression of the NADH kinase POS5Δ17 lacking the mitochondrial targeting sequence to relieve NADH/NADPH imbalance resulted in the BT titer of 2.2 g/L (31% molar yield). Feeding low concentrations of glucose and xylose to support the supply of NADH resulted in BT titer of 6.6 g/L with (57% molar yield). Collectively, improving the NADH/NADPH ratio and supply from glucose are essential for the construction of a xylose pathway, such as the BT synthetic pathway, independent of native yeast metabolism.

摘要

1,2,4-丁三醇(BT)被用作合成各种药物和高能增塑剂 1,2,4-丁三醇三硝酸酯的前体。在酿酒酵母中,BT 通过异源的四个酶促反应从木糖生物合成,由木酮糖脱氢酶、木酮酸盐脱水酶、2-酮酸脱羧酶和醇脱氢酶催化。我们旨在通过基因工程提高酿酒酵母中的 BT 产量。首先,通过将乳球菌 2-酮酸脱羧酶基因 kdcA 多次整合到酵母基因组中,成功地将先前描述的关键中间产物 2-酮-3-脱氧木酮酸的量减少了 41%。由于异源 BT 合成途径独立于酵母天然代谢,这种操作导致在 BT 生产过程中 NADH/NADPH 失衡和缺乏。过表达缺乏线粒体靶向序列的 NADH 激酶 POS5Δ17 以缓解 NADH/NADPH 失衡,导致 BT 产量达到 2.2g/L(摩尔收率 31%)。低浓度葡萄糖和木糖的补料喂养以支持 NADH 的供应,导致 BT 产量达到 6.6g/L(摩尔收率 57%)。总的来说,提高 NADH/NADPH 比值和葡萄糖的供应对于构建独立于天然酵母代谢的木糖途径,如 BT 合成途径,是必不可少的。

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