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首页> 外文期刊>Biochimica et Biophysica Acta. Gene Regulatory Mechanisms >Transcriptional regulation mechanism mediated by miRNA-DNA?DNA triplex structure stabilized by Argonaute
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Transcriptional regulation mechanism mediated by miRNA-DNA?DNA triplex structure stabilized by Argonaute

机译:Argonaute稳定的miRNA-DNA?DNA三链体结构介导的转录调控机制

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摘要

Transcription regulation depends on interactions between repressor or activator proteins with promoter sequences, while post-transcriptional regulation typically relies on microRNA (miRNA) interaction with sequences in 5' and 3'-Untranslated regions (UTRs) of messenger RNA (mRNA). However, several pieces of evidence suggest that miRNA:Argonaute (AGO) complexes may also suppress transcription through RNA interference (RNAi) components and epigenetic mechanisms. However, recent observations suggest that miRNA-induced transcriptional silencing could be exerted by an unknown mechanism independent of chromatin modifiers. The RNA-DNA?DNA triplex structure has emerged as an important RNA tertiary motif in which successive non-canonical base pairs form between a DNA-DNA duplex and a third strand. Frequently, promoters have Purine (PU)-rich tracts, and some Triplex-forming oligonucleotides (TFOs) targeting these regulatory regions have been shown to inhibit transcription selectively. Here, we summarize observations suggesting that miRNAs exert regulation over promoter regions through miRNA-DNA?DNA triplex structure formation stabilized by AGO proteins which represents a plausible model of RNA-mediated Transcriptional gene silencing (TGS).
机译:转录调控取决于阻遏蛋白或激活蛋白与启动子序列之间的相互作用,而转录后调控通常依赖于microRNA(miRNA)与Messenger RNA(mRNA)5'和3'-非翻译区(UTR)中的序列相互作用。但是,一些证据表明,miRNA:Argonaute(AGO)复合物也可能通过RNA干扰(RNAi)成分和表观遗传机制抑制转录。但是,最近的观察结果表明,miRNA诱导的转录沉默可能是由未知机制独立于染色质修饰剂发挥的。 RNA-DNA→DNA三链体结构已作为一种重要的RNA叔基序出现,其中在DNA-DNA双链体和第三条链之间形成连续的非规范碱基对。通常,启动子具有富含嘌呤(PU)的区域,并且一些靶向这些调控区的三链形成寡核苷酸(TFO)已显示选择性抑制转录。在这里,我们总结了观察结果,提示miRNA通过AGO蛋白稳定的miRNA-DNA?DNA三链体结构形成对启动子区域进行调控,这代表了RNA介导的转录基因沉默(TGS)的合理模型。

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