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A high-resolution map of three-dimensional chromatin interactome in human cells

机译:人体细胞中三维染色质相互作用组的高分辨率图

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摘要

A large number of cis-regulatory sequences have been annotated in the human genome,, but defining their target genes remains a challenge. One strategy is to identify the long-range looping interactions at these elements with the use of chromosome conformation capture (3C) based techniques. However, previous studies lack either the resolution or coverage to permit a whole-genome, unbiased view of chromatin interactions. Here, we report a comprehensive chromatin interaction map generated in human fibroblasts using a genome-wide 3C analysis method (Hi-C). We determined over one million long-range chromatin interactions at 5–10kb resolution, and uncovered general principles of chromatin organization at different types of genomic features. We also characterized the dynamics of promoter-enhancer contacts upon TNF-α signaling in these cells. Unexpectedly, we found that TNF-α responsive enhancers are already in contact with their target promoters prior to signaling. Such pre-existing chromatin looping, which also exists in other cell types with different extra-cellular signaling, is a strong predictor of gene induction. Our observations suggest that the three-dimensional chromatin landscape, once established in a particular cell type, is rather stable and could influence the selection or activation of target genes by a ubiquitous transcription activator in a cell-specific manner.
机译:人类基因组中已经注释了许多顺式调控序列,但定义其靶基因仍然是一个挑战。一种策略是使用基于染色体构象捕获(3C)的技术 来识别这些元件上的远程循环相互作用。但是,以前的研究缺乏分辨率或覆盖范围,无法对染色质相互作用进行全基因组,无偏见的观察。在这里,我们报告了使用全基因组3C分析方法(Hi-C) 在人成纤维细胞中生成的全面染色质相互作用图。我们以5-10kb的分辨率确定了超过一百万的长距离染色质相互作用,并揭示了不同类型的基因组特征中染色质组织的一般原理。我们还表征了这些细胞中TNF-α信号传导时启动子-增强子接触的动力学。出乎意料的是,我们发现TNF-α反应增强剂在信号传导之前已经与它们的靶标启动子接触。这种预先存在的染色质环,也存在于具有不同细胞外信号转导的其他细胞类型中,是基因诱导的强烈预测因子。我们的观察结果表明,一旦在特定的细胞类型中建立了三维染色质格局,它就相当稳定,并可能以细胞特异性方式通过遍在转录激活因子影响靶基因的选择或激活。

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