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Metabolic fluxes during strong carbon catabolite repression by malate in Bacillus subtilis

机译:苹果酸在枯草芽孢杆菌中强烈抑制碳分解代谢物过程中的代谢通量

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摘要

Commonly glucose is considered to be the only preferred substrate in Bacillus subtilis whose presence represses utilization of other alternative substrates. Because recent data indicate that malate might be an exception, we quantify here the carbon source utilization hierarchy. Based on physiology and transcriptional data during co-utilization experiments with eight carbon substrates, we demonstrate that malate is a second preferred carbon source for B. subtilis, which is rapidly co-utilized with glucose and strongly represses the uptake of alternative substrates. From the different hierarchy and degree of catabolite repression exerted by glucose and malate, we conclude that both substrates might act through different molecular mechanisms. To obtain a quantitative and functional network view of how malate is (co)metabolized, we developed a novel approach to metabolic flux analysis that avoids error-prone, intuitive, and ad hoc decisions on (13)C rearrangements. In particular, we developed a rigorous approach for deriving reaction reversibilities by combining in vivo intracellular metabolite concentrations with a thermodynamic feasibility analysis. The thus-obtained analytical model of metabolism was then used for network-wide isotopologue balancing to estimate the intracellular fluxes. These (13)C-flux data revealed an extraordinarily high malate influx that is primarily catabolized via the gluconeogenic reactions and toward overflow metabolism. Furthermore, a considerable NADPH-producing malic enzyme flux is required to supply the biosynthetically required NADPH in the presence of malate. Co-utilization of glucose and malate resulted in a synergistic decrease of the respiratory tricarboxylic acid cycle flux.
机译:通常,葡萄糖被认为是枯草芽孢杆菌中唯一优选的底物,其存在抑制了其他替代底物的利用。因为最近的数据表明苹果酸可能是一个例外,所以我们在这里量化碳源利用层次。基于与八种碳底物共同利用实验中的生理和转录数据,我们证明苹果酸是枯草芽孢杆菌的第二种优选碳源,它与葡萄糖迅速地共同利用,并强烈抑制其他底物的吸收。从葡萄糖和苹果酸对分解代谢物抑制的不同层次和程度,我们得出结论,两种底物可能通过不同的分子机制起作用。为了获得苹果酸如何(共)代谢的定量和功能网络视图,我们开发了一种新的代谢通量分析方法,该方法避免了对(13)C重排容易出错,直观且临时的决定。特别是,我们通过结合体内细胞内代谢物浓度和热力学可行性分析,开发了一种严格的方法来获得反应可逆性。然后将由此获得的代谢分析模型用于网络范围的同位素同位素平衡,以估计细胞内通量。这些(13)C-flux数据显示苹果酸大量涌入,主要通过糖原异生反应分解代谢,并向溢流代谢。此外,在苹果酸的存在下需要大量产生NADPH的苹果酸酶通量以提供生物合成所需的NADPH。葡萄糖和苹果酸的共同利用导致呼吸三羧酸循环通量的协同降低。

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