利用表型异质性提高酵母生产谷胱甘肽的能力。

IF 4.3 2区 生物学 Q1 BIOTECHNOLOGY & APPLIED MICROBIOLOGY
Mingzhi Xu, Cindy Vallières, Chris Finnis, Klaus Winzer, Simon V Avery
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引用次数: 0

摘要

背景:基因表达噪音(基因一致的细胞群体中单个细胞之间的基因表达差异)会导致工业微生物产生不同的代谢物,培养物中既有低产细胞,也有高产细胞。低产个体的存在可能是限制高产潜力的一个因素。本研究测试了一种假设,即酵母细胞群中的低产变体可以持续逆向选择,以增加谷胱甘肽(GSH)这一示范产品的净产量:根据已知的对γ-谷氨酰半胱氨酸合成酶(GSH1)基因表达的反馈抑制作用,在酿酒酵母(Saccharomyces cerevisiae)中设计了一个反选择系统,GSH1 ORF 和反选择标记 GAP1 分别在 TEF1 和 GSH 调节的 GSH1 启动子控制下表达。在添加了 D-组氨酸的工程菌株培养物中,细胞平均 GSH 水平提高了 18%,从而反选择出 GAP1 高表达的细胞(即低 GSH 产细胞)。这种表型是不可遗传的,并不是对 D-组氨酸的一般反应,这与使用替代标记物制备的某些其他测试结构不同:结论:研究结果证实,本文开发的系统通过靶向低产细胞提高了 GSH 的产量。这支持了利用终产物/启动子的相互作用来富集表型异质性群体中的高产细胞,从而提高酵母生产代谢产物的潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Exploiting phenotypic heterogeneity to improve production of glutathione by yeast.

Background: Gene expression noise (variation in gene expression among individual cells of a genetically uniform cell population) can result in heterogenous metabolite production by industrial microorganisms, with cultures containing both low- and high-producing cells. The presence of low-producing individuals may be a factor limiting the potential for high yields. This study tested the hypothesis that low-producing variants in yeast cell populations can be continuously counter-selected, to increase net production of glutathione (GSH) as an exemplar product.

Results: A counter-selection system was engineered in Saccharomyces cerevisiae based on the known feedback inhibition of gamma-glutamylcysteine synthetase (GSH1) gene expression, which is rate limiting for GSH synthesis: the GSH1 ORF and the counter-selectable marker GAP1 were expressed under control of the TEF1 and GSH-regulated GSH1 promoters, respectively. An 18% increase in the mean cellular GSH level was achieved in cultures of the engineered strain supplemented with D-histidine to counter-select cells with high GAP1 expression (i.e. low GSH-producing cells). The phenotype was non-heritable and did not arise from a generic response to D-histidine, unlike that with certain other test-constructs prepared with alternative markers.

Conclusions: The results corroborate that the system developed here improves GSH production by targeting low-producing cells. This supports the potential for exploiting end-product/promoter interactions to enrich high-producing cells in phenotypically heterogeneous populations, in order to improve metabolite production by yeast.

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来源期刊
Microbial Cell Factories
Microbial Cell Factories 工程技术-生物工程与应用微生物
CiteScore
9.30
自引率
4.70%
发文量
235
审稿时长
2.3 months
期刊介绍: Microbial Cell Factories is an open access peer-reviewed journal that covers any topic related to the development, use and investigation of microbial cells as producers of recombinant proteins and natural products, or as catalyzers of biological transformations of industrial interest. Microbial Cell Factories is the world leading, primary research journal fully focusing on Applied Microbiology. The journal is divided into the following editorial sections: -Metabolic engineering -Synthetic biology -Whole-cell biocatalysis -Microbial regulations -Recombinant protein production/bioprocessing -Production of natural compounds -Systems biology of cell factories -Microbial production processes -Cell-free systems
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