亮氨酸
生物化学
焊剂(冶金)
代谢工程
大肠杆菌
生物合成
生物
柠檬酸循环
代谢通量分析
氨基酸
代谢途径
拉伤
新陈代谢
化学
酶
基因
有机化学
解剖
作者
Yanan Hao,Xuewei Pan,Guo‐Min Li,Jiajia You,Hengwei Zhang,Sihan Yan,Meijuan Xu,Zhiming Rao
标识
DOI:10.1186/s13068-023-02397-x
摘要
L-Leucine is a high-value amino acid with promising applications in the medicine and feed industries. However, the complex metabolic network and intracellular redox imbalance in fermentative microbes limit their efficient biosynthesis of L-leucine.In this study, we applied rational metabolic engineering and a dynamic regulation strategy to construct a plasmid-free, non-auxotrophic Escherichia coli strain that overproduces L-leucine. First, the L-leucine biosynthesis pathway was strengthened through multi-step rational metabolic engineering. Then, a cooperative cofactor utilization strategy was designed to ensure redox balance for L-leucine production. Finally, to further improve the L-leucine yield, a toggle switch for dynamically controlling sucAB expression was applied to accurately regulate the tricarboxylic acid cycle and the carbon flux toward L-leucine biosynthesis. Strain LEU27 produced up to 55 g/L of L-leucine, with a yield of 0.23 g/g glucose.The combination of strategies can be applied to the development of microbial platforms that produce L-leucine and its derivatives.
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