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利用气相色谱 - 质谱联用技术对大肠杆菌中心碳代谢突变体进行代谢通量分析。

Metabolic flux profiling of Escherichia coli mutants in central carbon metabolism using GC-MS.

作者信息

Fischer Eliane, Sauer Uwe

机构信息

Institute of Biotechnology, ETH Zürich, CH-8093 Zürich, Switzerland.

出版信息

Eur J Biochem. 2003 Mar;270(5):880-91. doi: 10.1046/j.1432-1033.2003.03448.x.

Abstract

We describe here a novel methodology for rapid diagnosis of metabolic changes, which is based on probabilistic equations that relate GC-MS-derived mass distributions in proteinogenic amino acids to in vivo enzyme activities. This metabolic flux ratio analysis by GC-MS provides a comprehensive perspective on central metabolism by quantifying 14 ratios of fluxes through converging pathways and reactions from [1-13C] and [U-13C]glucose experiments. Reliability and accuracy of this method were experimentally verified by successfully capturing expected flux responses of Escherichia coli to environmental modifications and seven knockout mutations in all major pathways of central metabolism. Furthermore, several mutants exhibited additional, unexpected flux responses that provide new insights into the behavior of the metabolic network in its entirety. Most prominently, the low in vivo activity of the Entner-Doudoroff pathway in wild-type E. coli increased up to a contribution of 30% to glucose catabolism in mutants of glycolysis and TCA cycle. Moreover, glucose 6-phosphate dehydrogenase mutants catabolized glucose not exclusively via glycolysis, suggesting a yet unidentified bypass of this reaction. Although strongly affected by environmental conditions, a stable balance between anaplerotic and TCA cycle flux was maintained by all mutants in the upper part of metabolism. Overall, our results provide quantitative insight into flux changes that bring about the resilience of metabolic networks to disruption.

摘要

我们在此描述一种用于快速诊断代谢变化的新方法,该方法基于概率方程,这些方程将蛋白质ogenic氨基酸中气相色谱 - 质谱法衍生的质量分布与体内酶活性相关联。这种通过气相色谱 - 质谱法进行的代谢通量比率分析,通过量化来自[1 - 13C]和[U - 13C]葡萄糖实验的汇聚途径和反应的14种通量比率,提供了对中心代谢的全面视角。通过成功捕获大肠杆菌对环境修饰和中心代谢所有主要途径中的七个基因敲除突变的预期通量响应,实验验证了该方法的可靠性和准确性。此外,几个突变体表现出额外的、意想不到的通量响应,这为整个代谢网络的行为提供了新的见解。最显著的是,野生型大肠杆菌中Entner - Doudoroff途径的低体内活性在糖酵解和三羧酸循环突变体中增加到对葡萄糖分解代谢的贡献高达30%。此外,6 - 磷酸葡萄糖脱氢酶突变体并非仅通过糖酵解分解葡萄糖,这表明存在尚未确定的该反应旁路。尽管受到环境条件的强烈影响,但所有突变体在代谢上部维持了回补和三羧酸循环通量之间的稳定平衡。总体而言,我们的结果提供了对通量变化的定量见解,这些变化导致代谢网络对破坏具有恢复力。

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