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Topological Properties of Co-Occurrence Networks in Published Gene Expression Signatures

机译:共发网络在已发表的基因表达签名中的拓扑性质

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摘要

Meta-analysis of high-throughput gene expression data is often used for the interpretation of proprietary gene expression data sets. We have recently shown that co-occurrence patterns of gene expression in published cancer-related gene expression signatures are reminiscent of several cancer signaling pathways. Indeed, significant co-occurrence of up to ten genes in published gene expression signatures can be exploited to build a co-occurrence network from the sets of co-occurring genes (“co-occurrence modules”). Such co-occurrence network is represented by an undirected graph, where single genes are assigned to vertices and edges indicate that two genes are significantly co-occurring. Thus, graph-cut methods can be used to identify groups of highly interconnected vertices (“network communities”) that correspond to sets of genes that are significantly co-regulated in human cancer. Here, we investigate the topological properties of co-occurrence networks derived from published gene expression signatures and show that co-occurrence networks are characterized by scale-free topology and hierarchical modularity. Furthermore, we report that genes with a “promiscuous” or a “faithful” co-occurrence pattern can be distinguished. This behavior is reminiscent of date and party hubs that have been identified in protein-protein interaction networks.
机译:高通量基因表达数据的荟萃分析通常用于解释专有基因表达数据集。我们最近显示,已发表的癌症相关基因表达特征中基因表达的共现模式使人联想到几种癌症信号通路。实际上,可以利用已公开的基因表达特征中多达十个基因的显着共现来从共现基因集(“共现模块”)构建共现网络。这样的共现网络由无向图表示,其中单个基因被分配给顶点,并且边缘指示两个基因显着共现。因此,图切方法可用于识别高度互连的顶点(“网络社区”)的组,这些顶点对应于在人类癌症中显着共调节的基因集。在这里,我们调查了共现网络的拓扑特性,这些共现网络是从已发布的基因表达签名中衍生出来的,并且表明共现网络的特征在于无标度拓扑和分层模块化。此外,我们报告可以区分具有“混杂”或“忠实”共现模式的基因。此行为让人联想到在蛋白质-蛋白质相互作用网络中已确定的日期和聚会中心。

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