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Model of central and trimethylammonium metabolism for optimizing L-carnitine production by E. coli.

机译:用于优化大肠杆菌生产左旋肉碱的中枢和三甲基铵代谢模型。

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The application of metabolic engineering principles to the rational design of microbial production processes crucially depends on the ability to make quantitative descriptions of the systemic ability of the central carbon metabolism to redirect fluxes to the product-forming pathways. The aim of this work was to further our understanding of the steps controlling the biotransformation of trimethylammonium compounds into L-carnitine by Escherichia coli. Despite the importance of L-carnitine production processes, development of a model of the central carbon metabolism linked to the secondary carnitine metabolism of E. coli has been severely hampered by the lack of stoichiometric information on the metabolic reactions taking place in the carnitine metabolism. Here we present the design and experimental validation of a model which, for the first time, links the carnitine metabolism with the reactions of glycolysis, the tricarboxylic acid cycle and the pentose-phosphate pathway. The results demonstrate a needfor a high production rate of ATP to be devoted to the biotransformation process. The results demonstrate that ATP is used up in a futile cycle, since both trimethylammonium compound carriers CaiT and ProU operate simultaneously. To improve the biotransformation process, resting processes as well as CaiT or ProU knock out mutants would yield a more efficient system for producing L-carnitine from crotonobetaine or D-carnitine.
机译:代谢工程原理在微生物生产过程的合理设计中的应用至关重要地取决于能否对中央碳代谢将通量重定向到产品形成途径的系统能力进行定量描述。这项工作的目的是使我们进一步了解控制大肠杆菌将三甲基铵化合物生物转化为L-肉碱的步骤。尽管左旋肉碱生产过程很重要,但由于缺乏关于肉碱代谢中发生的代谢反应的化学计量信息,严重阻碍了与大肠杆菌的次级肉碱代谢有关的中央碳代谢模型的开发。在这里,我们提出模型的设计和实验验证,该模型首次将肉碱代谢与糖酵解,三羧酸循环和戊糖-磷酸途径的反应联系起来。结果表明需要高生产率的ATP专门用于生物转化过程。结果表明,ATP无效,因为三甲基铵化合物载体CaiT和ProU同时运行。为了改善生物转化过程,静置过程以及CaiT或ProU敲除突变体将产生一个更有效的系统,用于从巴豆甜菜碱或D-肉碱生产L-肉碱。

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