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Scale-space measures for graph topology link protein network architecture to function

机译:图拓扑的尺度空间度量使蛋白质网络体系结构起作用

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Motivation: The network architecture of physical protein interactions is an important determinant for the molecular functions that are carried out within each cell. To study this relation, the network architecture can be characterized by graph topological characteristics such as shortest paths and network hubs. These characteristics have an important shortcoming: they do not take into account that interactions occur across different scales. This is important because some cellular functions may involve a single direct protein interaction (small scale), whereas others require more and/or indirect interactions, such as protein complexes (medium scale) and interactions between large modules of proteins (large scale). Results: In this work, we derive generalized scale-aware versions of known graph topological measures based on diffusion kernels. We apply these to characterize the topology of networks across all scales simultaneously, generating a so-called graph topological scale-space. The comprehensive physical interaction network in yeast is used to show that scale-space based measures consistently give superior performance when distinguishing protein functional categories and three major types of functional interactions-genetic interaction, co-expression and perturbation interactions. Moreover, we demonstrate that graph topological scale spaces capture biologically meaningful features that provide new insights into the link between function and protein network architecture.
机译:动机:蛋白质相互作用的网络结构是决定每个细胞内分子功能的重要决定因素。为了研究这种关系,可以通过图形拓扑特征(例如最短路径和网络集线器)来表征网络体系结构。这些特征有一个重要的缺点:它们没有考虑到交互作用发生在不同的规模上。这很重要,因为某些细胞功能可能涉及单一的直接蛋白质相互作用(小规模),而其他细胞功能则需要更多和/或间接的相互作用,例如蛋白质复合物(中等规模)和大型蛋白质模块之间的相互作用(大规模)。结果:在这项工作中,我们基于扩散核派生了已知图拓扑度量的广义尺度感知版本。我们将它们应用于同时表征所有规模的网络拓扑,从而生成所谓的图拓扑规模空间。酵母中的综合物理相互作用网络用于显示,当区分蛋白质功能类别和三种主要类型的功能相互作用(遗传相互作用,共表达和微扰相互作用)时,基于尺度空间的度量始终可提供出色的性能。此外,我们证明了图拓扑尺度空间捕获了生物学上有意义的特征,这些特征为功能和蛋白质网络体系结构之间的联系提供了新的见解。

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