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Strand-specific CpG hemimethylation, a novel epigenetic modification functional for genomic imprinting

机译:股线特异性CpG六甲基化,一种新型外膜遗传学函数因基因组印记

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摘要

Imprinted genes are regulated by allele-specific differentially DNA-methylated regions (DMRs). Epigenetic methylation of the CpGs constituting these DMRs is established in the germline, resulting in a 5-methylcytosine-specific pattern that is tightly maintained in somatic tissues. Here, we show a novel epigenetic mark, characterized by strand-specific hemimethylation of contiguous CpG sites affecting the germline DMR of the murine Peg3, but not Snrpn, imprinted domain. This modification is enriched in tetraploid cortical neurons, a cell type where evidence for a small proportion of formylmethylated CpG sites within the Peg3-controlling DMR is also provided. Single nucleotide polymorphism (SNP)based transcriptional analysis indicated that these epigenetic modifications participate in the maintainance of the monoallelic expression pattern of the Peg3 imprinted gene. Our results unexpectedly demonstrate that the methylation pattern observed in DMRs controlling defined imprinting regions can be modified in somatic cells, resulting in a novel epigenetic modification that gives rise to strand-specific hemimethylated domains functional for genomic imprinting. We anticipate the existence of a novel molecular mechanism regulating the transition from fully methylated CpGs to strand-specific hemimethylated CpGs.
机译:印迹基因由等位基因特异性差异DNA-甲基化区(DMR)调节。构成这些DMRS的CPG的表观甲基化是在种系中建立的,得到5-甲基胞嘧啶特异性图案,其在体细胞组织中紧密维持。在这里,我们展示了一种新颖的表观遗传标记,其特征在于,其特征是影响鼠PEG3的种系DMR的连续CPG位点的束特异性血管基,但不是SNRPN,印迹结构域。该修饰在四倍体皮质神经元中富集,还提供了一种细胞类型,其中还提供了PEG3控制DMR内少比例的甲醛甲基化的CPG位点的证据。基于单核苷酸多态性(SNP)的转录分析表明,这些表观遗传学修饰参与了PEG3印迹基因的单相连表达模式的维护。我们的结果意外地证明,在控制定义的压印区域的DMRS中观察到的甲基化模式可以在体细胞中进行改性,导致新的表观遗传学改性,其产生用于基因组印记的股线特异性的半甲基化结构域。我们预计将一种调节从完全甲基化CpG转变为股线特异性血氧化CpG的新分子机制的存在。

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