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Hierarchical Modularity in ERα Transcriptional Network Is Associated with Distinct Functions and Implicates Clinical Outcomes

机译:ERα转录网络中的分层模块与不同的功能相关并涉及临床结果

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摘要

Recent genome-wide profiling reveals highly complex regulation networks among ERα and its targets. We integrated estrogen (E2)-stimulated time-series ERα ChIP-seq and gene expression data to identify the ERα-centered transcription factor (TF) hubs and their target genes, and inferred the time-variant hierarchical network structures using a Bayesian multivariate modeling approach. With its recurrent motif patterns, we determined three embedded regulatory modules from the ERα core transcriptional network. The GO analyses revealed the distinct biological function associated with each of three embedded modules. The survival analysis showed the genes in each module were able to render a significant survival correlation in breast cancer patient cohorts. In summary, our Bayesian statistical modeling and modularity analysis not only reveals the dynamic properties of the ERα-centered regulatory network and associated distinct biological functions, but also provides a reliable and effective genomic analytical approach for the analysis of dynamic regulatory network for any given TF.
机译:最近的全基因组分析揭示了ERα及其靶标之间高度复杂的调控网络。我们整合了雌激素(E2)刺激的时间序列ERαChIP-seq和基因表达数据,以鉴定以ERα为中心的转录因子(TF)集线器及其靶基因,并使用贝叶斯多元模型推断时变的分层网络结构方法。借助其反复出现的图案模式,我们从ERα核心转录网络中确定了三个嵌入式调控模块。 GO分析揭示了与三个嵌入式模块各自相关的独特生物学功能。生存分析表明,每个模块中的基因均能够在乳腺癌患者队列中提供显着的生存相关性。总而言之,我们的贝叶斯统计建模和模块化分析不仅揭示了以ERα为中心的调控网络的动态特性以及相关的独特生物学功能,而且还为任何给定TF的动态调控网络分析提供了可靠而有效的基因组分析方法。

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