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Two waves of de novo methylation during mouse germ cell development

机译:小鼠生殖细胞发育过程中的两次从头甲基化

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摘要

During development, mammalian germ cells reprogram their epigenomes via a genome-wide erasure and de novo rewriting of DNA methylation marks. We know little of how methylation patterns are specifically determined. The piRNA pathway is thought to target the bulk of retrotransposon methylation. Here we show that most retrotransposon sequences are modified by default de novo methylation. However, potentially active retrotransposon copies evade this initial wave, likely mimicking features of protein-coding genes. These elements remain transcriptionally active and become targets of piRNA-mediated methylation. Thus, we posit that these two waves play essential roles in resetting germ cell epigenomes at each generation.
机译:在发育过程中,哺乳动物生殖细胞通过全基因组擦除和DNA甲基化标记的从头重写来重新编程其表观基因组。我们对如何具体确定甲基化模式知之甚少。 piRNA途径被认为靶向大量的反转录转座子甲基化。在这里,我们显示大多数逆转录转座子序列默认情况下是从头甲基化修饰的。但是,潜在活跃的反转录转座子复制规避了这一最初的浪潮,可能模仿了蛋白质编码基因的特征。这些元件保持转录活性,并成为piRNA介导的甲基化的目标。因此,我们假设这两个波在每一代的生殖细胞表观基因组重置中都起着至关重要的作用。

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