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On the availability of microRNA-induced silencing complexes saturation of microRNA-binding sites and stoichiometry

机译:关于microRNA诱导沉默复合物的可用性microRNA结合位点的饱和度和化学计量

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摘要

Several authors have suggested or inferred that modest changes in microRNA expression can potentiate or impinge on their capacity to mediate gene repression, and that doing so could play a significant role in diseases. Such interpretations are based on several assumptions, namely: (i) changes in microRNA expression correlate with changes in the availability of mature, functional miRISC, (ii) changes in microRNA expression can significantly alter the stoichiometry of miRISC populations with their cognate targets, (iii) and this, in turn, can result in changes in miRISC silencing output. Here, we experimentally challenge those assumptions by quantifying and altering the availability of miRISC across several families of microRNAs. Doing so revealed a surprising fragmentation in the miRISC functional pool, striking differences in the availability of miRNA families and saturability of miRNA-mediated silencing. Furthermore, we provide direct experimental evidence that only a limited subset of miRNAs, defined by a conjuncture of expression threshold, miRISC availability and low target site abundance, is susceptible to competitive effects through microRNA-binding sites.
机译:一些作者建议或推断,微小RNA表达的适度变化会增强或影响其介导基因阻遏的能力,并且这样做可能在疾病中发挥重要作用。此类解释基于几个假设,即:(i)microRNA表达的变化与成熟的功能性miRISC的可用性的变化相关;(ii)microRNA表达的变化可以显着改变miRISC人群及其相关靶标的化学计量,( iii),进而会导致miRISC沉默输出的变化。在这里,我们通过量化和改变多个microRNA家族中miRISC的可用性来对这些假设进行实验性挑战。这样做揭示了miRISC功能池中令人惊讶的碎片化,显着改变了miRNA家族的可用性和miRNA介导的沉默的饱和性。此外,我们提供了直接的实验证据,证明只有miRNA的有限子集(由表达阈值,miRISC可用性和低目标位点丰度共同决定)易受微小RNA结合位点的竞争影响。

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