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Pri-miR-17-92a transcript folds into a tertiary structure and autoregulates its processing

机译:Pri-miR-17-92a转录本折叠成三级结构并自动调节其加工

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MicroRNAs control gene expression either by RNA transcript degradation or translational repression. Expressions of miRNAs are highly regulated in tissues, disruption of which leads to disease. How this regulation is achieved and maintained is still largely unknown. MiRNAs that reside on clustered or polycistronic transcripts represent a more complex case where individual miRNAs from a cluster are processed with different efficiencies despite being cotranscribed. To shed light on the regulatory mechanisms that might be operating in these cases, we considered the long polycistronic primary miRNA transcript pri-miR-17-92a that contains six miRNAs with diverse functions. The six miRNA domains on this cluster are differentially processed to produce varying amounts of resultant mature miRNAs in different tissues. How this is achieved is not known. We show, using various biochemical and biophysical methods coupled with mutational studies, that pri-miR-17-92a adopts a specific three-dimensional architecture that poses a kinetic barrier to its own processing. This tertiary structure could create suboptimal protein recognition sites on the pri-miRNA cluster due to higher-order structure formation.
机译:MicroRNA通过RNA转录物降解或翻译抑制来控制基因表达。 miRNA的表达在组织中受到高度调节,破坏会导致疾病。如何实现和维持该法规仍然很大程度上未知。驻留在簇状或多顺反子转录物上的miRNA代表了一个更为复杂的情况,尽管来自簇中的单个miRNA尽管被共转录,但仍以不同的效率进行处理。为了阐明在这些情况下可能起作用的调节机制,我们考虑了长的多顺反子一级miRNA转录本pri-miR-17-92a,其中包含六个功能多样的miRNA。对该簇上的六个miRNA结构域进行差异处理,以在不同组织中产生不同数量的所得成熟miRNA。如何实现这一点尚不清楚。我们显示,使用各种生化和生物物理方法以及突变研究,pri-miR-17-92a采用了特定的三维结构,对其自身的加工构成了动力学障碍。由于较高阶结构的形成,这种三级结构可能会在pri-miRNA簇上产生次优的蛋白质识别位点。

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