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首页> 美国卫生研究院文献>Cell Research >The p53-induced lincRNA-p21 derails somatic cell reprogramming by sustaining H3K9me3 and CpG methylation at pluripotency gene promoters
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The p53-induced lincRNA-p21 derails somatic cell reprogramming by sustaining H3K9me3 and CpG methylation at pluripotency gene promoters

机译:通过在多能基因启动子处维持H3K9me3和CpG甲基化p53诱导的lincRNA-p21破坏了体细胞重编程。

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摘要

Recent studies have boosted our understanding of long noncoding RNAs (lncRNAs) in numerous biological processes, but few have examined their roles in somatic cell reprogramming. Through expression profiling and functional screening, we have identified that the large intergenic noncoding RNA p21 (lincRNA-p21) impairs reprogramming. Notably, lincRNA-p21 is induced by p53 but does not promote apoptosis or cell senescence in reprogramming. Instead, lincRNA-p21 associates with the H3K9 methyltransferase SETDB1 and the maintenance DNA methyltransferase DNMT1, which is facilitated by the RNA-binding protein HNRNPK. Consequently, lincRNA-p21 prevents reprogramming by sustaining H3K9me3 and/or CpG methylation at pluripotency gene promoters. Our results provide insight into the role of lncRNAs in reprogramming and establish a novel link between p53 and heterochromatin regulation.
机译:最近的研究提高了我们对许多生物过程中长非编码RNA(lncRNA)的了解,但很少有人检查它们在体细胞重编程中的作用。通过表达谱分析和功能筛选,我们发现大型的基因间非编码RNA p21(lincRNA-p21)损害了重编程。值得注意的是,lincRNA-p21由p53诱导,但在重编程中不会促进细胞凋亡或细胞衰老。相反,lincRNA-p21与H3K9甲基转移酶SETDB1和维持DNA甲基转移酶DNMT1缔合,这由RNA结合蛋白HNRNPK促进。因此,lincRNA-p21通过在多能基因启动子处维持H3K9me3和/或CpG甲基化来防止重编程。我们的结果提供了有关lncRNAs在重编程中的作用的见解,并在p53和异染色质调节之间建立了新的联系。

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