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Characterizing the strand-specific distribution of non-CpG methylation in human pluripotent cells

机译:表征人多能细胞中非CpG甲基化的股线特异性分布

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摘要

DNA methylation is an important defense and regulatory mechanism. In mammals, most DNA methylation occurs at CpG sites, and asymmetric non-CpG methylation has only been detected at appreciable levels in a few cell types. We are the first to systematically study the strand-specific distribution of non-CpG methylation. With the divide-and compare strategy, we show that CHG and CHH methylation are not intrinsically different in human embryonic stem cells (ESCs) and induced pluripotent stem cells (iPSCs). We also find that non-CpG methylation is skewed between the two strands in introns, especially at intron boundaries and in highly expressed genes. Controlling for the proximal sequences of non-CpG sites, we show that the skew of non-CpG methylation in introns is mainly guided by sequence skew. By studying subgroups of transposable elements, we also found that non-CpG methylation is distributed in a strand-specific manner in both short interspersed nuclear elements (SINE) and long interspersed nuclear elements (LINE), but not in long terminal repeats (LTR). Finally, we show that on the antisense strand of Alus, a non-CpG site just downstream of the A-box is highly methylated. Together, the divide-and-compare strategy leads us to identify regions with strand-specific distributions of non-CpG methylation in humans.
机译:DNA甲基化是一种重要的防御和调节机制。在哺乳动物中,大多数DNA甲基化发生在CpG位点,并且在几种细胞类型中仅在可观的水平下检测到不对称的非CpG甲基化。我们是第一个系统地研究非CpG甲基化的股线特异性分布。随着划分和比较策略,我们表明CHG和CHH甲基化在人胚胎干细胞(ESC)和诱导多能干细胞(IPSC)中没有本质上。我们还发现非CpG甲基化在内含子的两条股线之间倾斜,特别是在内含子边界和高表达的基因。控制非CpG位点的近端序列,我们表明内含子中非CpG甲基化的偏差主要是由序列偏斜引导的。通过研究可转换元素的亚组,我们还发现非CpG甲基化以短时间核心(正弦)和长三个核心(线)以绞合特异性方式分布,但不在长终端重复(LTR)中。最后,我们表明,在Anus的反义链上,刚刚下游的非CPG位点高度甲基化。划分和比较策略在一起导致我们识别人类中非CpG甲基化的股线特异性分布的地区。

著录项

  • 来源
    《Nucleic Acids Research》 |2014年第5期|共8页
  • 作者单位

    Bioinformatics Division and Center for Synthetic &

    Systems Biology TNLIST Tsinghua University Beijing 100084 China;

    Department of Molecular and Cell Biology Center for Systems Biology The University of Texas at Dallas Richardson TX 75080 USA;

    LMAM School of Mathematical Sciences Peking University Beijing 100871 China;

    Department of Molecular Cell and Developmental Biology University of California Los Angeles CA 90095 USA;

    Bioinformatics Division and Center for Synthetic &

    Systems Biology TNLIST Tsinghua University Beijing 100084 China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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