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A role for human Dicer in pre-RISC loading of siRNAs

机译:人类Dicer在RISC之前siRNA加载中的作用

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摘要

RNA interference is a powerful mechanism for sequence-specific inhibition of gene expression. It is widely known that small interfering RNAs (siRNAs) targeting the same region of a target-messenger RNA can have widely different efficacies. In efforts to better understand the siRNA features that influence knockdown efficiency, we analyzed siRNA interactions with a high-molecular weight complex in whole cell extracts prepared from two different cell lines. Using biochemical tools to study the nature of the complex, our results demonstrate that the primary siRNA-binding protein in the whole cell extracts is Dicer. We find that Dicer is capable of discriminating highly functional versus poorly functional siRNAs by recognizing the presence of 2-nt 3′ overhangs and the thermodynamic properties of 2–4 bp on both ends of effective siRNAs. Our results suggest a role for Dicer in pre-selection of effective siRNAs for handoff to Ago2. This initial selection is reflective of the overall silencing potential of an siRNA.
机译:RNA干扰是基因表达的序列特异性抑制的强大机制。众所周知,靶向靶信使RNA相同区域的小干扰RNA(siRNA)可能具有广泛不同的功效。为了更好地理解影响敲低效率的siRNA特征,我们分析了由两种不同细胞系制备的全细胞提取物中siRNA与高分子量复合物的相互作用。使用生化工具研究复合物的性质,我们的结果表明,全细胞提取物中的主要siRNA结合蛋白是Dicer。我们发现Dicer通过识别有效siRNA两端的2 -nt 3'突出端和2–4 bp的热力学性质,能够区分高功能和低功能的siRNA。我们的结果表明Dicer在预选有效siRNA以便向Ago2交接中的作用。最初的选择反映了siRNA的整体沉默潜力。

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