代谢工程
酿酒酵母
酵母
生物化学
焊剂(冶金)
糖酵解
化学
代谢途径
新陈代谢
生物合成
合成生物学
基因
生物
有机化学
计算生物学
作者
Quanli Liu,Tao Yu,Xiaowei Li,Yu Chen,Kate Campbell,Jens Nielsen,Yun Chen
标识
DOI:10.1038/s41467-019-12961-5
摘要
The production of bioactive plant compounds using microbial hosts is considered a safe, cost-competitive and scalable approach to their production. However, microbial production of some compounds like aromatic amino acid (AAA)-derived chemicals, remains an outstanding metabolic engineering challenge. Here we present the construction of a Saccharomyces cerevisiae platform strain able to produce high levels of p-coumaric acid, an AAA-derived precursor for many commercially valuable chemicals. This is achieved through engineering the AAA biosynthesis pathway, introducing a phosphoketalose-based pathway to divert glycolytic flux towards erythrose 4-phosphate formation, and optimizing carbon distribution between glycolysis and the AAA biosynthesis pathway by replacing the promoters of several important genes at key nodes between these two pathways. This results in a maximum p-coumaric acid titer of 12.5 g L-1 and a maximum yield on glucose of 154.9 mg g-1.
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