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Understanding transcriptional regulation by integrative analysis of transcription factor binding data

机译:通过对转录因子结合数据的综合分析来了解转录调控

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Statistical models have been used to quantify the relationship between gene expression and transcription factor (TF) binding signals. Here we apply the models to the large-scale data generated by the ENCODE project to study transcriptional regulation by TFs. Our results reveal a notable difference in the prediction accuracy of expression levels of transcription start sites (TSSs) captured by different technologies and RNA extraction protocols. In general, the expression levels of TSSs with high CpG content are more predictable than those with low CpG content. For genes with alternative TSSs, the expression levels of downstream TSSs are more predictable than those of the upstream ones. Different TF categories and specific TFs vary substantially in their contributions to predicting expression. Between two cell lines, the differential expression of TSS can be precisely reflected by the difference of TF-binding signals in a quantitative manner, arguing against the conventional on-and-off model of TF binding. Finally, we explore the relationships between TF-binding signals and other chromatin features such as histone modifications and DNase hypersensitivity for determining expression. The models imply that these features regulate transcription in a highly coordinated manner.
机译:统计模型已用于量化基因表达与转录因子(TF)结合信号之间的关系。在这里,我们将模型应用于ENCODE项目生成的大规模数据,以研究TF的转录调控。我们的结果揭示了由不同技术和RNA提取协议捕获的转录起始位点(TSS)的表达水平的预测准确性的显着差异。通常,具有高CpG含量的TSS的表达水平比具有低CpG含量的TSS的表达水平更可预测。对于具有替代TSS的基因,下游TSS的表达水平比上游TSS的表达水平更可预测。不同的TF类别和特定的TF在预测表达上的贡献差异很大。在两个细胞系之间,可以通过定量的TF结合信号差异准确地反映TSS的差异表达,这与TF结合的常规开-关模型有关。最后,我们探索了TF结合信号与其他染色质特征(例如组蛋白修饰和DNase超敏性)之间的关系,以确定表达。该模型暗示这些特征以高度协调的方式调节转录。

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