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Construction of a Genome-Scale Kinetic Model of Mycobacterium Tuberculosis Using Generic Rate Equations

机译:用通用速率方程构建结核分枝杆菌基因组规模的动力学模型

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The study of biological systems at the genome scale helps us understand fundamental biological processes that govern the activity of living organisms and regulate their interactions with the environment. Genome-scale metabolic models are usually analysed using constraint-based methods, since detailed rate equations and kinetic parameters are often missing. However, constraint-based analysis is limited in capturing the dynamics of cellular processes. In this paper, we present an approach to build a genome-scale kinetic model of Mycobacterium tuberculosis metabolism using generic rate equations. M. tuberculosis causes tuberculosis which remains one of the largest killer infectious diseases. Using a genetic algorithm, we estimated kinetic parameters for a genome-scale metabolic model of M. tuberculosis based on flux distributions derived from Flux Balance Analysis. Our results show that an excellent agreement with flux values is obtained under several growth conditions, although kinetic parameters may vary in different conditions. Parameter variability analysis indicates that a high degree of redundancy remains present in model parameters, which suggests that the integration of other types of high-throughput datasets will enable the development of better constrained models accounting for a variety of in vivo phenotypes.
机译:对基因组规模的生物系统的研究有助于我们了解控制生物体活动并调节其与环境相互作用的基本生物学过程。通常使用基于约束的方法来分析基因组规模的代谢模型,因为通常缺少详细的速率方程和动力学参数。但是,基于约束的分析在捕获细胞过程的动力学方面受到限制。在本文中,我们提出了一种使用通用速率方程建立结核分枝杆菌代谢基因组规模动力学模型的方法。结核分枝杆菌引起结核病,其仍然是最大的杀手传染病之一。使用遗传算法,我们根据通量平衡分析得出的通量分布,估算了结核分枝杆菌基因组规模代谢模型的动力学参数。我们的结果表明,尽管动力学参数可能在不同条件下有所不同,但在几种生长条件下均能获得与通量值极好的一致性。参数变异性分析表明,模型参数中仍然存在高度冗余,这表明其他类型的高通量数据集的集成将能够开发出更好的受约束模型,从而考虑到多种体内表型。

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