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通量耦合分析的代谢子系统。

On flux coupling analysis of metabolic subsystems.

机构信息

FB Mathematik und Informatik, Freie Universität Berlin, Arnimallee 6, D-14195 Berlin, Germany.

出版信息

J Theor Biol. 2012 Jun 7;302:62-9. doi: 10.1016/j.jtbi.2012.02.023. Epub 2012 Mar 3.

Abstract

Genome-scale metabolic networks are useful tools for achieving a system-level understanding of metabolism. However, due to their large size, analysis of such networks may be difficult and algorithms can be very slow. Therefore, some authors have suggested to analyze subsystems instead of the original genome-scale models. Flux coupling analysis (FCA) is a well-known method for detecting functionally related reactions in metabolic networks. In this paper, we study how flux coupling relations may change if we analyze a subsystem instead of the original network. We show mathematically that a pair of fully, partially or directionally coupled reactions may be detected as uncoupled in certain subsystems. Interestingly, this behavior is the opposite of the flux coupling changes that may occur due to missing reactions, or equivalently, deletion of reactions. Computational experiments suggest that the analysis of plastid (but not mitochondrial) subsystems may significantly influence the results of FCA. Therefore, the results of FCA for subsystems, especially plastid subsystems, should be interpreted with care.

摘要

基因组规模的代谢网络是实现代谢系统水平理解的有用工具。然而,由于其规模庞大,对这些网络的分析可能很困难,算法可能非常缓慢。因此,一些作者建议分析子系统而不是原始的基因组规模模型。通量耦合分析(FCA)是一种用于检测代谢网络中功能相关反应的知名方法。在本文中,我们研究了如果我们分析子系统而不是原始网络,通量耦合关系可能会如何变化。我们从数学上证明,一对完全、部分或方向耦合的反应可能会在某些子系统中被检测为不耦合。有趣的是,这种行为与由于缺失反应(或等效地,反应的删除)而可能发生的通量耦合变化相反。计算实验表明,质体(而非线粒体)子系统的分析可能会显著影响 FCA 的结果。因此,对子系统(特别是质体子系统)的 FCA 结果的解释应该谨慎。

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