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Flux Coupling Analysis of Genome-Scale Metabolic Network Reconstructions

机译:基因组规模代谢网络重构的通量耦合分析

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摘要

In this paper, we introduce the Flux Coupling Finder (FCF) framework for elucidating the topological and flux connectivity features of genome-scale metabolic networks. The framework is demonstrated on genome-scale metabolic reconstructions of Helicobacter pylori, Escherichia coli, and Saccharomyces cerevisiae. The analysis allows one to determine whether any two metabolic fluxes, v1 and v2, are (1) directionally coupled, if a non-zero flux for v1 implies a non-zero flux for v2 but not necessarily the reverse; (2) partially coupled, if a non-zero flux for v1 implies a non-zero, though variable, flux for v2 and vice versa; or (3) fully coupled, if a non-zero flux for v1 implies not only a non-zero but also a fixed flux for v2 and vice versa. Flux coupling analysis also enables the global identification of blocked reactions, which are all reactions incapable of carrying flux under a certain condition; equivalent knockouts, defined as the set of all possible reactions whose deletion forces the flux through a particular reaction to zero; and sets of affected reactions denoting all reactions whose fluxes are forced to zero if a particular reaction is deleted. The FCF approach thus provides a novel and versatile tool for aiding metabolic reconstructions and guiding genetic manipulations.
机译:在本文中,我们介绍了通量耦合查找器(FCF)框架,用于阐明基因组规模代谢网络的拓扑和通量连通性特征。该框架在幽门螺杆菌,大肠杆菌和酿酒酵母的基因组规模的代谢重建中得到证明。通过这种分析,可以确定v1和v2这两个代谢通量是否是有方向性耦合的,如果v1的非零通量意味着v2的非零通量,但不一定相反; (2)部分耦合,如果v1的通量为非零,则意味着v2的通量为非零(尽管是可变的),反之亦然;或(3)完全耦合,如果v1的非零通量不仅意味着v2的非零,还意味着v2的固定通量,反之亦然。磁通偶合分析还可以全局识别受阻的反应,这些反应在一定条件下都无法携带助焊剂。等效敲除,定义为所有可能的反应的集合,其删除将通过特定反应的通量强制为零;以及一组受影响的反应,表示删除特定反应后其通量被强制为零的所有反应。因此,FCF方法为协助代谢重建和指导遗传操作提供了一种新颖且通用的工具。

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