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Identification of novel prostate cancer drivers using RegNetDriver: a framework for integration of genetic and epigenetic alterations with tissue-specific regulatory network

机译:使用RegNetDriver识别新型前列腺癌驱动程序:整合遗传和表观遗传学改变与组织特异性调节网络的框架

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摘要

We report a novel computational method, RegNetDriver, to identify tumorigenic drivers using the combined effects of coding and non-coding single nucleotide variants, structural variants, and DNA methylation changes in the DNase I hypersensitivity based regulatory network. Integration of multi-omics data from 521 prostate tumor samples indicated a stronger regulatory impact of structural variants, as they affect more transcription factor hubs in the tissue-specific network. Moreover, crosstalk between transcription factor hub expression modulated by structural variants and methylation levels likely leads to the differential expression of target genes. We report known prostate tumor regulatory drivers and nominate novel transcription factors (ERF, CREB3L1, and POU2F2), which are supported by functional validation.Electronic supplementary materialThe online version of this article (doi:10.1186/s13059-017-1266-3) contains supplementary material, which is available to authorized users.
机译:我们报告了一种新型的计算方法RegNetDriver,使用编码和非编码单核苷酸变体,结构变体和基于DNase I超敏性的调节网络中的DNA甲基化变化的组合效应来识别致瘤驱动程序。来自521个前列腺肿瘤样本的多组学数据的整合表明,结构变体的调节作用更强,因为它们影响组织特异性网络中更多的转录因子中心。此外,由结构变体调节的转录因子中心表达与甲基化水平之间的串扰可能导致靶基因的差异表达。我们报告了已知的前列腺肿瘤调节驱动程序并提名了新的转录因子(ERF,CREB3L1和POU2F2),这些都得到功能验证的支持。电子补充材料本文的在线版本(doi:10.1186 / s13059-017-1266-3)包含补充材料,授权用户可以使用。

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