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Integration of Metabolic Modeling with Gene Co-expression Reveals Transcriptionally Programmed Reactions Explaining Robustness in Mycobacterium tuberculosis

机译:代谢建模与基因共表达的整合揭示了结核分枝杆菌的稳健性的转录程序反应。

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摘要

Robustness of metabolic networks is accomplished by gene regulation, modularity, re-routing of metabolites and plasticity. Here, we probed robustness against perturbations of biochemical reactions of M. tuberculosis in the form of predicting compensatory trends. In order to investigate the transcriptional programming of genes associated with correlated fluxes, we integrated with gene co-expression network. Knock down of the reactions NADH2r and ATPS responsible for producing the hub metabolites, and Central carbon metabolism had the highest proportion of their associated genes under transcriptional co-expression with genes of their flux correlated reactions. Reciprocal gene expression correlations were observed among compensatory routes, fresh activation of alternative routes and in the multi-copy genes of Cysteine synthase and of Phosphate transporter. Knock down of 46 reactions caused the activation of Isocitrate lyase or Malate synthase or both reactions, which are central to the persistent state of M. tuberculosis. A total of 30 new freshly activated routes including Cytochrome c oxidase, Lactate dehydrogenase, and Glycine cleavage system were predicted, which could be responsible for switching into dormant or persistent state. Thus, our integrated approach of exploring transcriptional programming of flux correlated reactions has the potential to unravel features of system architecture conferring robustness.
机译:代谢网络的鲁棒性是通过基因调节,模块化,代谢物重新路由和可塑性来实现的。在这里,我们以预测代偿性趋势的形式探讨了抗结核分枝杆菌生化反应扰动的鲁棒性。为了研究与相关通量相关的基因的转录程序设计,我们将其与基因共表达网络整合在一起。敲除负责产生轮毂代谢产物的反应NADH2r和ATPS,并且在与它们的通量相关反应的基因转录共表达下,中央碳代谢具有最高的相关基因比例。在补偿途径,替代途径的新鲜活化以及半胱氨酸合酶和磷酸盐转运蛋白的多拷贝基因中观察到相互的基因表达相关性。击倒46种反应导致异柠檬酸裂合酶或苹果酸合酶或两种反应的激活,这对于结核分枝杆菌的持续状态至关重要。预计总共有30条新激活的新途径,包括细胞色素c氧化酶,乳酸脱氢酶和甘氨酸裂解系统,这可能是导致进入休眠或持久状态的原因。因此,我们探索通量相关反应的转录程序的综合方法有可能揭示赋予鲁棒性的系统架构特征。

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