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ICR 非编码 RNA 表达控制着 Dlk1-Dio3 区域的印迹和 DNA 复制。

ICR noncoding RNA expression controls imprinting and DNA replication at the Dlk1-Dio3 domain.

机构信息

Institute of Molecular Genetics (IGMM), CNRS UMR5535 and University of Montpellier, 1919 Route de Mende, Montpellier 34293, France.

Institute of Functional Genomics (IGF), CNRS and University of Montpellier, 141 rue de la Cardonille, Montpellier 34090, France.

出版信息

Dev Cell. 2014 Oct 13;31(1):19-33. doi: 10.1016/j.devcel.2014.08.009. Epub 2014 Sep 25.

Abstract

Imprinted genes play essential roles in development, and their allelic expression is mediated by imprinting control regions (ICRs). The Dlk1-Dio3 locus is among the few imprinted domains controlled by a paternally methylated ICR. The unmethylated maternal copy activates imprinted expression early in development through an unknown mechanism. We find that in mouse embryonic stem cells (ESCs) and in blastocysts, this function is linked to maternal, bidirectional expression of noncoding RNAs (ncRNAs) from the ICR. Disruption of ICR ncRNA expression in ESCs affected gene expression in cis, led to acquisition of aberrant histone and DNA methylation, delayed replication timing along the domain on the maternal chromosome, and changed its subnuclear localization. The epigenetic alterations persisted during differentiation and affected the neurogenic potential of the stem cells. Our data indicate that monoallelic expression at an ICR of enhancer RNA-like ncRNAs controls imprinted gene expression, epigenetic maintenance processes, and DNA replication in embryonic cells.

摘要

印记基因在发育中发挥着重要作用,其等位基因的表达受印记控制区(ICR)调控。Dlk1-Dio3 基因座是少数由父源甲基化 ICR 控制的印记区域之一。未甲基化的母源拷贝通过未知机制在早期发育中激活印记表达。我们发现,在小鼠胚胎干细胞(ESCs)和囊胚中,这种功能与 ICR 来自母源的双向非编码 RNA(ncRNA)表达有关。ESCs 中 ICR ncRNA 表达的破坏会影响顺式基因表达,导致异常的组蛋白和 DNA 甲基化,沿母染色体上的结构域延迟复制时间,并改变其亚核定位。这些表观遗传改变在分化过程中持续存在,并影响干细胞的神经生成潜能。我们的数据表明,ICR 上的单等位基因表达增强子 RNA 样 ncRNA 控制着印记基因表达、表观遗传维持过程和胚胎细胞中的 DNA 复制。

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