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Robust differential microRNA targeting driven by supplementary interactions in vitro

机译:由辅助相互作用驱动的鲁棒差异微小RNA靶向

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Complementarity to the microRNA (miRNA) seed region has long been recognized as the primary determinant in target recognition by the Argonaute-miRNA complex. Recently, we reported that pairing to miRNA 3'-supplementary region (nucleotides 13-16) can increase target affinity by more than an order of magnitude beyond seed-pairing alone. Here, we present biochemical evidence that supplementary interactions can drive robust differential targeting between equivalently seed-matched target RNAs in vitro. When mixed together, Ago2-miRNA complexes initially bind seed-matched targets equally but then redistribute between targets based on the strength of supplementary interactions. Thus, while initial target recognition was driven by seed-pairing, the distribution of Ago2-miRNA complexes between targets was determined by retention of Ago2 on target RNAs via supplementary interactions. Mathematical modeling and biochemical data predict that targets with strong supplementary interactions could be more strongly repressed than seed-only matched targets, even when vastly outnumbered by seed-only targets. The combined results raise the possibility that supplementary interactions could play a role in specifying specific miRNA targets for enhanced repression.
机译:对MicroRNA(miRNA)种子区域的互补性被认为是Argonaute-miRNA复合物的目标识别中的主要决定因素。最近,我们报道了对miRNA 3'-补充区域(核苷酸13-16)的配对可以通过单独的种子配对超出多个数量级的目标亲和力。在这里,我们提出了生物化学证据,即补充相互作用可以在体外促进等效的种子匹配的靶RNA之间的鲁棒差异靶向。当混合在一起时,Ago2-miRNA复合物最初初始结合种子匹配的靶标,然后基于补充相互作用的强度在目标之间重新分配。因此,虽然通过种子配对驱动初始目标识别,但是通过弃权通过补充相互作用在靶RNA上保留靶标之间的AgO2- miRNA复合物的分布。数学建模和生物化学数据预测,即使仅被种子的靶标大大数量超过种子匹配的靶,也可以更强烈地压抑辅助相互作用的目标。合并的结果提高了补充相互作用的可能性在指定针对增强的抑制的特定miRNA靶标中可能发挥作用。

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