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Argonaute proteins regulate microRNA stability

机译:Argonaute蛋白调节microRNA的稳定性

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摘要

Argonaute proteins are key players in microRNA (miRNA) processing and function. Next to their role as RISC effector proteins mediating target silencing, they actively participate in miRNA biogenesis and increase miRNA abundance by a yet unidentified mechanism. It has been hypothesized that this increase in steady-state miRNA levels might be due to a stabilizing effect of Argonaute proteins, but this has not been analyzed so far due to a lack of test systems. Here, we provide two approaches to estimate miRNA stability and factors affecting it: in cells lacking Ago2, endogenous miRNA guide strand degradation and half-lives can be assessed using Actinomycin D or α-Amanitin. In turn, miRNA passenger strands can serve as a model in wildtype cells to ascertain the impact of miRNA stability factors. We provide evidence that Argonaute proteins stabilize mature miRNAs in a slicing-independent manner. Transcriptional inhibition reveals reduced half-lives of multiple endogenous miRNA guide strands in cells lacking Ago2. This effect is reversible upon the reconstitution of Argonaute expression. Correspondingly, overexpression of Argonaute proteins decelerates miRNA degradation and increases miRNA half-life. Taken together, this study employs two model systems to identify factors altering miRNA stability and provides evidence how Argonaute proteins post-transcriptionally elevate mature miRNA levels via increasing miRNA stability.
机译:Argonaute蛋白是microRNA(miRNA)加工和功能的关键参与者。除了作为介导靶标沉默的RISC效应蛋白外,它们还通过未知的机制积极参与miRNA的生物发生并增加miRNA的丰度。据推测,稳态miRNA水平的增加可能是由于Argonaute蛋白的稳定作用所致,但由于缺乏测试系统,至今尚未对此进行分析。在这里,我们提供了两种方法来评估miRNA的稳定性和影响其的因素:在缺乏Ago2的细胞中,可以使用放线菌素D或α-甘露聚糖来评估内源性miRNA指导链降解和半衰期。反过来,miRNA过客链可以充当野生型细胞中的模型,以确定miRNA稳定性因子的影响。我们提供的证据表明,Argonaute蛋白以独立于切片的方式稳定了成熟的miRNA。转录抑制显示缺乏Ago2的细胞中多个内源性miRNA引导链的半衰期缩短。这种作用在重组Argonaute表达时是可逆的。相应地,Argonaute蛋白的过度表达可减缓miRNA降解并延长miRNA半衰期。总而言之,这项研究采用两个模型系统来识别影响miRNA稳定性的因素,并提供证据证明Argonaute蛋白如何通过转录后通过增加miRNA稳定性来提高成熟miRNA的水平。

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