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Modular decomposition of metabolic reaction networks based on flux analysis and pathway projection

机译:基于通量分析和路径投影的代谢反应网络模块分解

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Motivation: The rational decomposition of biochemical networks into sub-structures has emerged as a useful approach to study the design of these complex systems. A biochemical network is characterized by an inhomogeneous connectivity distribution, which gives rise to several organizational features, including modularity. To what extent the connectivity-based modules reflect the functional organization of the network remains to be further explored. In this work, we examine the influence of physiological perturbations on the modular organization of cellular metabolism.Results: Modules were characterized for two model systems, liver and adipocyte primary metabolism, by applying an algorithm for top-down partition of directed graphs with non-uniform edge weights. The weights were set by the engagement of the corresponding reactions as expressed by the flux distribution. For the base case of the fasted rat liver, three modules were found, carrying out the following biochemical transformations: ketone body production, glucose synthesis and transamination. This basic organization was further modified when different flux distributions were applied that describe the liver's metabolic response to whole body inflammation. For the fully mature adipocyte, only a single module was observed, integrating all of the major pathways needed for lipid storage. Weaker levels of integration between the pathways were found for the early stages of adipocyte differentiation. Our results underscore the inhomogeneous distribution of both connectivity and connection strengths, and suggest that global activity data such as the flux distribution can be used to study the organizational flexibility of cellular metabolism.
机译:动机:生化网络合理分解为子结构已经成为研究这些复杂系统设计的有用方法。生化网络的特征是连接分布不均匀,这导致了多种组织功能,包括模块化。基于连接性的模块在多大程度上反映了网络的功能组织,仍有待进一步探讨。在这项工作中,我们研究了生理扰动对细胞代谢的模块化组织的影响。结果:通过应用一种算法对自上而下划分有向图的模型进行划分,从而针对肝脏和脂肪细胞初级代谢两个模型系统对模块进行了表征均匀的边缘权重。通过通量分布表示的相应反应的参与来设定权重。对于禁食大鼠肝脏的基础病例,发现了三个模块,它们执行以下生化转化:酮体产生,葡萄糖合成和氨基转移。当应用不同的通量分布描述肝脏对全身炎症的代谢反应时,该基本组织得到了进一步的修改。对于完全成熟的脂肪细胞,仅观察到一个模块,整合了脂质存储所需的所有主要途径。在脂肪细胞分化的早期阶段,发现通路之间的整合程度较弱。我们的结果强调了连接强度和连接强度的不均匀分布,并表明诸如通量分布之类的全球活动数据可用于研究细胞代谢的组织灵活性。

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