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工程改造酿酒酵母胞质乙酰辅酶A的供应:途径化学计量、自由能守恒和氧化还原辅因子平衡

Engineering cytosolic acetyl-coenzyme A supply in Saccharomyces cerevisiae: Pathway stoichiometry, free-energy conservation and redox-cofactor balancing.

作者信息

van Rossum Harmen M, Kozak Barbara U, Pronk Jack T, van Maris Antonius J A

机构信息

Department of Biotechnology, Delft University of Technology, Julianalaan 67, 2628 BC Delft, The Netherlands.

Department of Biotechnology, Delft University of Technology, Julianalaan 67, 2628 BC Delft, The Netherlands.

出版信息

Metab Eng. 2016 Jul;36:99-115. doi: 10.1016/j.ymben.2016.03.006. Epub 2016 Mar 23.

DOI:10.1016/j.ymben.2016.03.006
PMID:27016336
Abstract

Saccharomyces cerevisiae is an important industrial cell factory and an attractive experimental model for evaluating novel metabolic engineering strategies. Many current and potential products of this yeast require acetyl coenzyme A (acetyl-CoA) as a precursor and pathways towards these products are generally expressed in its cytosol. The native S. cerevisiae pathway for production of cytosolic acetyl-CoA consumes 2 ATP equivalents in the acetyl-CoA synthetase reaction. Catabolism of additional sugar substrate, which may be required to generate this ATP, negatively affects product yields. Here, we review alternative pathways that can be engineered into yeast to optimize supply of cytosolic acetyl-CoA as a precursor for product formation. Particular attention is paid to reaction stoichiometry, free-energy conservation and redox-cofactor balancing of alternative pathways for acetyl-CoA synthesis from glucose. A theoretical analysis of maximally attainable yields on glucose of four compounds (n-butanol, citric acid, palmitic acid and farnesene) showed a strong product dependency of the optimal pathway configuration for acetyl-CoA synthesis. Moreover, this analysis showed that combination of different acetyl-CoA production pathways may be required to achieve optimal product yields. This review underlines that an integral analysis of energy coupling and redox-cofactor balancing in precursor-supply and product-formation pathways is crucial for the design of efficient cell factories.

摘要

酿酒酵母是一种重要的工业细胞工厂,也是评估新型代谢工程策略的理想实验模型。这种酵母目前的许多产品以及潜在产品都需要乙酰辅酶A(acetyl-CoA)作为前体,且通往这些产品的途径通常在其细胞质中表达。酿酒酵母产生细胞质乙酰辅酶A的天然途径在乙酰辅酶A合成酶反应中消耗2个ATP当量。产生这种ATP可能需要的额外糖底物的分解代谢会对产品产量产生负面影响。在此,我们综述了可以引入酵母以优化细胞质乙酰辅酶A供应作为产品形成前体的替代途径。特别关注了从葡萄糖合成乙酰辅酶A的替代途径的反应化学计量、自由能守恒和氧化还原辅因子平衡。对四种化合物(正丁醇、柠檬酸、棕榈酸和法尼烯)在葡萄糖上可达到的最大产量的理论分析表明,乙酰辅酶A合成的最佳途径配置对产品有很强的依赖性。此外,该分析表明,可能需要组合不同的乙酰辅酶A生产途径才能实现最佳产品产量。本综述强调,对前体供应和产品形成途径中的能量耦合和氧化还原辅因子平衡进行综合分析对于设计高效细胞工厂至关重要。

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