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Index and biological spectrum of human DNase I hypersensitive sites

机译:人DNA酶I过敏位点的指数和生物谱

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摘要

DNase I hypersensitive sites (DHSs) are generic markers of regulatory DNA(1-5)and contain genetic variations associated with diseases and phenotypic traits(6-8). We created high-resolution maps of DHSs from 733 human biosamples encompassing 438 cell and tissue types and states, and integrated these to delineate and numerically index approximately 3.6 million DHSs within the human genome sequence, providing a common coordinate system for regulatory DNA. Here we show that these maps highly resolve thecis-regulatory compartment of the human genome, which encodes unexpectedly diverse cell- and tissue-selective regulatory programs at very high density. These programs can be captured comprehensively by a simple vocabulary that enables the assignment to each DHS of a regulatory barcode that encapsulates its tissue manifestations, and global annotation of protein-coding and non-coding RNA genes in a manner orthogonal to gene expression. Finally, we show that sharply resolved DHSs markedly enhance the genetic association and heritability signals of diseases and traits. Rather than being confined to a small number of distal elements or promoters, we find that genetic signals converge on congruently regulated sets of DHSs that decorate entire gene bodies. Together, our results create a universal, extensible coordinate system and vocabulary for human regulatory DNA marked by DHSs, and provide a new global perspective on the architecture of human gene regulation.High-resolution maps of DNase I hypersensitive sites from 733 human biosamples are used to identify and index regulatory DNA within the human genome.
机译:DNase I过敏位点(DHSS)是调控DNA(1-5)的通用标记,含有与疾病和表型特征相关的遗传变异(6-8)。我们创建了来自733名人体生物素的DHSS的高分辨率地图,包括438个细胞和组织类型和组织类型,并将其整合到描绘中,并在数值上指定人类基因组序列中的约360万DHS,为调节DNA提供共同的坐标系。在这里,我们表明这些地图高度解析了人类基因组的Thecis-Concematory隔间,其在非常高的密度下编码意外不同的细胞和组织选择性调节程序。可以通过简单的词汇全面捕获这些程序,使得能够分配给调节条形码的每个DHS,其在与基因表达正交的方式中封装其组织表现的蛋白质编码和非编码RNA基因的全局注释。最后,我们表明急剧解决的DHSS显着提高了疾病和特征的遗传关联和可遗传性信号。我们发现遗传信号融合了全部受监管的DHS,而不是被限制在少数少数远端元素或启动子上。我们的结果在一起创造了由DHSS标志的人类调节DNA的普遍,可扩展的坐标系和词汇,并提供了一种关于人类基因调节结构的全球性观点。使用来自733个人生物素的DNase I过敏位点的高分辨率映射鉴定人类基因组内的调节性DNA。

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  • 来源
    《Nature》 |2020年第7820期|244-251|共8页
  • 作者单位

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA;

    Altius Inst Biomed Sci Seattle WA 98121 USA|Univ Washington Dept Genome Sci Seattle WA 98195 USA|Univ Washington Dept Med Div Oncol Seattle WA 98195 USA;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
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  • 关键词

  • 入库时间 2022-08-18 22:15:27

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