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CTCF-Mediated Human 3D Genome Architecture Reveals Chromatin Topology for Transcription

机译:CTCF介导的人类3D基因组架构揭示了染色质拓扑的转录。

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摘要

Spatial genome organization and its effect on transcription remains a fundamental question. We applied an advanced chromatin interaction analysis by paired-end tag sequencing (ChIA-PET) strategy to comprehensively map higher-order chromosome folding and specific chromatin interactions mediated by CCCTC-binding factor (CTCF) and RNA polymerase II (RNAPII) with haplotype specificity and nucleotide resolution in different human cell lineages. We find that CTCF/cohesin-mediated interaction anchors serve as structural foci for spatial organization of constitutive genes concordant with CTCF-motif orientation, whereas RNAPII interacts within these structures by selectively drawing cell-type-specific genes toward CTCF foci for coordinated transcription. Furthermore, we show that haplotype variants and allelic interactions have differential effects on chromosome configuration, influencing gene expression, and may provide mechanistic insights into functions associated with disease susceptibility. 3D genome simulation suggests a model of chromatin folding around chromosomal axes, where CTCF is involved in defining the interface between condensed and open compartments for structural regulation. Our 3D genome strategy thus provides unique insights in the topological mechanism of human variations and diseases.
机译:空间基因组的组织及其对转录的影响仍然是一个基本问题。我们应用了通过配对末端标记测序(ChIA-PET)策略进行的高级染色质相互作用分析来全面绘制高倍染色体折叠和CCCTC结合因子(CTCF)和RNA聚合酶II(RNAPII)介导的具有单倍型特异性的特定染色质相互作用和不同人类细胞谱系中的核苷酸分辨率。我们发现CTCF / cohesin介导的相互作用锚作为与CTCF-基序方向一致的组成基因的空间组织的结构焦点,而RNAPII通过选择性地向CTCF焦点绘制细胞类型特异性基因以协调转录而在这些结构内相互作用。此外,我们显示单倍型变体和等位基因相互作用对染色体构型有不同的影响,影响基因表达,并可能为与疾病易感性相关的功能提供机制的见解。 3D基因组模拟显示了围绕染色体轴的染色质折叠模型,其中CTCF参与定义冷凝和开放隔室之间的界面以进行结构调节。因此,我们的3D基因组策略可提供有关人类变异和疾病的拓扑机制的独特见解。

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