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Towards a map of cis-regulatory sequences in the human genome

机译:朝向人类基因组的顺式调控序列的地图

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Accumulating evidence indicates that transcription factor (TF) binding sites, or cis-regulatory elements (CREs), and their clusters termed cis-regulatory modules (CRMs) play a more important role than do gene-coding sequences in specifying complex traits in humans, including the susceptibility to common complex diseases. To fully characterize their roles in deriving the complex traits/diseases, it is necessary to annotate all CREs and CRMs encoded in the human genome. However, the current annotations of CREs and CRMs in the human genome are still very limited and mostly coarse-grained, as they often lack the detailed information of CREs in CRMs. Here, we integrated 620 TF ChIP-seq datasets produced by the ENCODE project for 168 TFs in 79 different cell/tissue types and predicted an unprecedentedly completely map of CREs in CRMs in the human genome at single nucleotide resolution. The map includes 305 912 CRMs containing a total of 1 178 913 CREs belonging to 736 unique TF binding motifs. The predicted CREs and CRMs tend to be subject to either purifying selection or positive selection, thus are likely to be functional. Based on the results, we also examined the status of available ChIP-seq datasets for predicting the entire regulatory genome of humans.
机译:累积证据表明转录因子(TF)结合位点或顺式调节元件(CRES)及其簇称为顺式调节模块(CRMS)起比在人体中指定复杂性状的基因编码序列发挥更重要的作用,包括对常见复杂疾病的敏感性。为了充分表征其在衍生复杂的特征/疾病方面的作用,有必要注释在人类基因组中编码的所有CRES和CRM。然而,人类基因组中的CRE和CRM的当前注释仍然非常有限,大多数粗粒,因为它们通常缺乏CRES中的CRES的详细信息。在这里,我们在79种不同的细胞/组织类型中集成了由编码项目产生的620 TF芯片-SEQ数据集,以在79种不同的细胞/组织类型中预测人类基因组中的CRES在单一核苷酸分辨率下完全完全映射。该地图包括305 912个CRM,总共1178 913个CRES属于736个独特的TF绑定图案。预测的CRE和CRMS往往受纯化选择或阳性选择,因此可能是功能性的。根据结果​​,我们还研究了可用芯片-SEQ数据集的状态,以预测人类的整个监管基因组。

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