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MIWI2 靶向来源于 piRNA 依赖区域的 RNA 以驱动小鼠精原干细胞中的 DNA 甲基化。

MIWI2 targets RNAs transcribed from piRNA-dependent regions to drive DNA methylation in mouse prospermatogonia.

机构信息

Yale Stem Cell Center and Department of Cell Biology, Yale University School of Medicine, New Haven, CT, USA

Yale Stem Cell Center and Department of Cell Biology, Yale University School of Medicine, New Haven, CT, USA.

出版信息

EMBO J. 2018 Sep 14;37(18). doi: 10.15252/embj.201695329. Epub 2018 Aug 14.

Abstract

Argonaute/Piwi proteins can regulate gene expression via RNA degradation and translational regulation using small RNAs as guides. They also promote the establishment of suppressive epigenetic marks on repeat sequences in diverse organisms. In mice, the nuclear Piwi protein MIWI2 and Piwi-interacting RNAs (piRNAs) are required for DNA methylation of retrotransposon sequences and some other sequences. However, its underlying molecular mechanisms remain unclear. Here, we show that piRNA-dependent regions are transcribed at the stage when piRNA-mediated DNA methylation takes place. MIWI2 specifically interacts with RNAs from these regions. In addition, we generated mice with deletion of a retrotransposon sequence either in a representative piRNA-dependent region or in a piRNA cluster. Both deleted regions were required for the establishment of DNA methylation of the piRNA-dependent region, indicating that piRNAs determine the target specificity of MIWI2-mediated DNA methylation. Our results indicate that MIWI2 affects the chromatin state through base-pairing between piRNAs and nascent RNAs, as observed in other organisms possessing small RNA-mediated epigenetic regulation.

摘要

Argonaute/Piwi 蛋白可通过小 RNA 作为向导调控基因表达,包括 RNA 降解和翻译调控。它们还能促进多种生物中重复序列上抑制性表观遗传标记的建立。在小鼠中,核 Piwi 蛋白 MIWI2 和 Piwi 相互作用 RNA(piRNA)对于逆转录转座子序列和其他一些序列的 DNA 甲基化是必需的。然而,其潜在的分子机制尚不清楚。在这里,我们发现当 piRNA 介导的 DNA 甲基化发生时,piRNA 依赖区被转录。MIWI2 特异性地与来自这些区域的 RNA 相互作用。此外,我们生成了在代表性 piRNA 依赖区或 piRNA 簇中缺失逆转录转座子序列的小鼠。这两个缺失区域都需要建立 piRNA 依赖区的 DNA 甲基化,表明 piRNAs 决定了 MIWI2 介导的 DNA 甲基化的靶标特异性。我们的结果表明,MIWI2 通过 piRNAs 与新生 RNA 之间的碱基配对来影响染色质状态,这在其他具有小 RNA 介导的表观遗传调控的生物中也观察到。

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