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Dicer-1而非Loquacious对于微小RNA诱导沉默复合体的组装至关重要。

Dicer-1, but not Loquacious, is critical for assembly of miRNA-induced silencing complexes.

作者信息

Liu Xiang, Park Joseph K, Jiang Feng, Liu Ying, McKearin Dennis, Liu Qinghua

机构信息

Department of Biochemistry, University of Texas Southwestern Medical Center, Dallas, Texas 75390, USA.

出版信息

RNA. 2007 Dec;13(12):2324-9. doi: 10.1261/rna.723707. Epub 2007 Oct 10.

Abstract

Double-stranded RNA-binding proteins (dsRBPs), such as R2D2 and Loquacious (Loqs), function in tandem with Dicer (Dcr) enzymes in RNA interference (RNAi). In Drosophila, Dcr-1/Loqs and Dcr-2/R2D2 complexes generate microRNAs (miRNAs) and small interfering RNAs (siRNAs), respectively. Although R2D2 does not regulate siRNA production, R2D2 and Dcr-2 coordinately bind siRNAs to promote assembly of the siRNA-induced silencing (siRISC) complexes. Conversely, Loqs enhances miRNA production. It is uncertain if Dcr-1 and Loqs facilitate miRNA loading onto the miRISC complexes. Here we used loqs knockout (KO) flies to characterize the physiological functions of Loqs in the miRNA pathway. Northern analysis revealed consistent accumulation of precursor (pre)-miRNAs in loqs(KO) flies. However, the lack of Loqs had differential effects on mature miRNAs: some are diminished, whereas others maintain wild-type levels. Importantly, the data suggest that miRNA production is not the rate-limiting step of the miRNA pathway. We show that Dcr-1, but not Loqs, is critical for assembly of miRISCs by using dcr-1 or loqs null egg extract. Consistent with this, recombinant Dcr-1 could efficiently interact with miRNA duplex in the absence of Loqs. Together, our results indicate that Loqs plays a prominent role in miRNA biogenesis, but is largely dispensable for miRISC assembly. Thus, Loqs and R2D2 represent two distinct functional modes for dsRBPs in the RNAi pathways.

摘要

双链RNA结合蛋白(dsRBPs),如R2D2和Loquacious(Loqs),在RNA干扰(RNAi)中与Dicer(Dcr)酶协同发挥作用。在果蝇中,Dcr-1/Loqs和Dcr-2/R2D2复合物分别产生微小RNA(miRNA)和小干扰RNA(siRNA)。虽然R2D2不调节siRNA的产生,但R2D2和Dcr-2协同结合siRNA以促进siRNA诱导沉默(siRISC)复合物的组装。相反,Loqs增强miRNA的产生。目前尚不清楚Dcr-1和Loqs是否促进miRNA加载到miRISC复合物上。在这里,我们使用loqs基因敲除(KO)果蝇来表征Loqs在miRNA途径中的生理功能。Northern分析显示,在loqs(KO)果蝇中前体(pre)-miRNA持续积累。然而,Loqs的缺失对成熟miRNA有不同的影响:一些减少,而另一些维持野生型水平。重要的是,数据表明miRNA的产生不是miRNA途径的限速步骤。我们通过使用dcr-1或loqs缺失的卵提取物表明,Dcr-1而非Loqs对miRISC的组装至关重要。与此一致的是,在没有Loqs的情况下,重组Dcr-1可以有效地与miRNA双链体相互作用。总之,我们的结果表明,Loqs在miRNA生物合成中起重要作用,但在很大程度上对于miRISC组装是可有可无的。因此,Loqs和R2D2代表了RNAi途径中dsRBPs的两种不同功能模式。

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