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首页> 外文期刊>Nucleic acids research >Integrative construction of regulatory region networks in 127 human reference epigenomes by matrix factorization
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Integrative construction of regulatory region networks in 127 human reference epigenomes by matrix factorization

机译:基于矩阵分解的127个人类参考表观基因组调控区域网络的整合构建

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Despite large experimental and computational efforts aiming to dissect the mechanisms underlying disease risk, mapping cis-regulatory elements to target genes remains a challenge. Here, we introduce a matrix factorization framework to integrate physical and functional interaction data of genomic segments. The framework was used to predict a regulatory network of chromatin interaction edges linking more than 20 000 promoters and 1.8 million enhancers across 127 human reference epigenomes, including edges that are present in any of the input datasets. Our network integrates functional evidence of correlated activity patterns from epigenomic data and physical evidence of chromatin interactions. An important contribution of this work is the representation of heterogeneous data with different qualities as networks. We show that the unbiased integration of independent data sources suggestive of regulatory interactions produces meaningful associations supported by existing functional and physical evidence, correlating with expected independent biological features.
机译:尽管大量的实验和计算努力旨在剖析疾病风险的潜在机制,但将顺式调控元件定位于靶基因仍然是一个挑战。在这里,我们介绍一个矩阵分解框架,以整合基因组片段的物理和功能相互作用数据。该框架用于预测染色质相互作用边缘的调控网络,该相互作用网络跨127个人类参考表观基因组连接了20000多个启动子和180万个增强子,包括任何输入数据集中存在的边缘。我们的网络整合了来自表观基因组数据的相关活动模式的功能证据和染色质相互作用的物理证据。这项工作的重要贡献是将具有不同质量的异构数据表示为网络。我们表明独立的数据源的无偏见的暗示监管相互作用产生了由现有功能和物理证据支持的有意义的关联,与预期的独立生物学特征相关。

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