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Imprinting control regions (ICRs) are marked by mono-allelic bivalent chromatin when transcriptionally inactive

机译:当转录无活性时,印记控制区(ICR)以单等位基因二价染色质标记

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摘要

Parental allele-specific expression of imprinted genes is mediated by imprinting control regions (ICRs) that are constitutively marked by DNA methylation imprints on the maternal or paternal allele. Mono-allelic DNA methylation is strictly required for the process of imprinting and has to be faithfully maintained during the entire life-span. While the regulation of DNA methylation itself is well understood, the mechanisms whereby the opposite allele remains unmethylated are unclear. Here, we show that in the mouse, at maternally methylated ICRs, the paternal allele, which is constitutively associated with H3K4me2/3, is marked by default by H3K27me3 when these ICRs are transcriptionally inactive, leading to the formation of a bivalent chromatin signature. Our data suggest that at ICRs, chromatin bivalency has a protective role by ensuring that DNA on the paternal allele remains unmethylated and protected against spurious and unscheduled gene expression. Moreover, they provide the proof of concept that, beside pluripotent cells, chromatin bivalency is the default state of transcriptionally inactive CpG island promoters, regardless of the developmental stage, thereby contributing to protect cell identity.
机译:印迹基因的父母等位基因特异性表达是由印迹控制区域(ICR)介导的,该区域由母体或父亲等位基因上的DNA甲基化印迹组成性地标记。单等位基因DNA甲基化是印迹过程中严格要求的,并且必须在整个生命周期中如实地进行维护。尽管人们对DNA甲基化的调控本身已广为人知,但相对的等位基因保持未甲基化的机理尚不清楚。在这里,我们显示在小鼠中,在母亲甲基化的ICR处,与这些H3K4me2 / 3组成型相关的父亲等位基因默认情况下被这些ICR转录失活的H3K27me3标记,从而导致二价染色质签名的形成。我们的数据表明,通过确保父本等位基因上的DNA保持未甲基化并防止虚假和计划外的基因表达,染色质双价具有保护作用。此外,它们提供了概念证明,即除多能细胞外,染色质双价性是转录失活的CpG岛启动子的默认状态,而与发育阶段无关,从而有助于保护细胞身份。

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