Multi‐modular engineering of Saccharomyces cerevisiae for high‐titre production of tyrosol and salidroside

酪醇 红景天苷 代谢工程 生物化学 酿酒酵母 化学 酵母 酚类 色谱法
作者
Huayi Liu,Yujuan Tian,Yi Zhou,Yeyi Kan,Tingting Wu,Wenhai Xiao,Yunzi Luo
出处
期刊:Microbial biotechnology [Wiley]
卷期号:14 (6): 2605-2616 被引量:63
标识
DOI:10.1111/1751-7915.13667
摘要

Summary Tyrosol and its glycosylated product salidroside are important ingredients in pharmaceuticals, nutraceuticals and cosmetics. Despite the ability of Saccharomyces cerevisiae to naturally synthesize tyrosol, high yield from de novo synthesis remains a challenge. Here, we used metabolic engineering strategies to construct S. cerevisiae strains for high‐level production of tyrosol and salidroside from glucose. First, tyrosol production was unlocked from feedback inhibition. Then, transketolase and ribose‐5‐phosphate ketol‐isomerase were overexpressed to balance the supply of precursors. Next, chorismate synthase and chorismate mutase were overexpressed to maximize the aromatic amino acid flux towards tyrosol synthesis. Finally, the competing pathway was knocked out to further direct the carbon flux into tyrosol synthesis. Through a combination of these interventions, tyrosol titres reached 702.30 ± 0.41 mg l −1 in shake flasks, which were approximately 26‐fold greater than that of the WT strain. RrU8GT33 from Rhodiola rosea was also applied to cells and maximized salidroside production from tyrosol in S. cerevisiae . Salidroside titres of 1575.45 ± 19.35 mg l −1 were accomplished in shake flasks. Furthermore, titres of 9.90 ± 0.06 g l −1 of tyrosol and 26.55 ± 0.43 g l −1 of salidroside were achieved in 5 l bioreactors, both are the highest titres reported to date. The synergistic engineering strategies presented in this study could be further applied to increase the production of high value‐added aromatic compounds derived from the aromatic amino acid biosynthesis pathway in S. cerevisiae .

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