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首页> 外文期刊>Epigenetics: official journal of the DNA Methylation Society >Autonomous silencing of the imprinted Cdkn1c gene in stem cells
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Autonomous silencing of the imprinted Cdkn1c gene in stem cells

机译:干细胞中印记的Cdkn1c基因的自主沉默

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摘要

Parent-of-origin specific expression of imprinted genes relies on the differential DNA methylation of specific genomic regions. Differentially methylated regions (DMrs) acquire DNA methylation either during gametogenesis (primary DMr) or after fertilization when allele-specific expression is established (secondary DMr). Little is known about the function of these secondary DMrs. We investigated the DMr spanning Cdkn1c in mouse embryonic stem cells, androgenetic stem cells and embryonic germ stem cells. in all cases, expression of Cdkn1c was appropriately repressed in in vitro differentiated cells. However, stem cells failed to de novo methylate the silenced gene even after sustained differentiation. in the absence of maintained DNA methylation (Dnmt1 -/-), Cdkn1c escapes silencing demonstrating the requirement for DNA methylation in long term silencing in vivo. We propose that post-fertilization differential methylation reflects the importance of retaining single gene dosage of a subset of imprinted loci in the adult.
机译:印迹基因的起源亲本特异性表达依赖于特定基因组区域的差异DNA甲基化。差异甲基化区域(DMrs)在配子发生期间(初级DMr)或受精后建立等位基因特异性表达时(次级DMr)获得DNA甲基化。这些二级DMrs的功能知之甚少。我们研究了在小鼠胚胎干细胞,雄激素干细胞和胚胎生殖干细胞中跨越Cdkn1c的DMr。在所有情况下,体外分化的细胞中Cdkn1c的表达均被适当抑制。然而,即使在持续分化后,干细胞也无法使被沉默的基因重新甲基化。在没有维持DNA甲基化(Dnmt1-/-)的情况下,Cdkn1c逃避了沉默,这表明了体内长期沉默对DNA甲基化的需求。我们建议,受精后差异甲基化反应反映了在成年人中保留一个基因位点子集的单一基因剂量的重要性。

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