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Selective termination of lncRNA transcription promotes heterochromatin silencing and cell differentiation

机译:选择性lncRNA终止转录促进异染色质沉默和细胞分化

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Long non-coding RNAs (lncRNAs) regulating gene expression at the chromatin level are widespread among eukaryotes. However, their functions and the mechanisms by which they act are not fully understood. Here, we identify new fission yeast regulatory lncRNAs that are targeted, at their site of transcription, by the YTH domain of the RNA-binding protein Mmi1 and degraded by the nuclear exosome. We uncover that one of them, nam1, regulates entry into sexual differentiation. Importantly, we demonstrate that Mmi1 binding to this lncRNA not only triggers its degradation but also mediates its transcription termination, thus preventing lncRNA transcription from invading and repressing the downstream gene encoding a mitogen-activated protein kinase kinase kinase (MAPKKK) essential to sexual differentiation. In addition, we show that Mmi1-mediated termination of lncRNA transcription also takes place at pericentromeric regions where it contributes to heterochromatin gene silencing together with RNA interference (RNAi). These findings reveal an important role for selective termination of lncRNA transcription in both euchromatic and heterochromatic lncRNA-based gene silencing processes.
机译:长非编码rna (lncRNAs)调节基因表达式在染色质水平普遍存在在真核生物中。他们的行为的机制并不完全理解。监管lncRNAs是有针对性的,在他们网站的转录,从技术上说,云天化领域的rna结合蛋白Mmi1和退化核外来体。nam1,调节进入性分化。这不仅lncRNA触发其Mmi1绑定退化也介导转录终止,从而防止lncRNA转录从入侵和抑制下游基因编码一个增殖蛋白激酶激酶激酶(MAPKKK)性的关键分化。Mmi1-mediated lncRNA终止转录也发生在pericentromeric地区它导致异染色质基因沉默核糖核酸干扰(RNAi)在一起。发现揭示选择性的重要作用终止lncRNA转录的常染色质的和异色的lncRNA-based基因沉默的过程。

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