首页> 外文期刊>Molecular cell >The developmental timing regulator AIN-1 interacts with miRISCs and may target the argonaute protein ALG-1 to cytoplasmic P bodies in C. elegans
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The developmental timing regulator AIN-1 interacts with miRISCs and may target the argonaute protein ALG-1 to cytoplasmic P bodies in C. elegans

机译:发育时间调节器AIN-1与miRISC相互作用,并可能将argonaute蛋白ALG-1靶向秀丽隐杆线虫的胞质P体

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摘要

In metazoans, microRNAs (miRNAs) carry out various regulatory functions through association with multiprotein miRNA-induced silencing complexes (miRISCs) that contain Dicer and Argonaute proteins. How miRNAs regulate the expression of their mRNA targets remains a major research question. We have identified the C. elegrans ain-1 gene through a genetic suppressor screen and shown that it functions with the heterochronic genetic pathway that regulates developmental timing. Biochemical analysis indicates that AIN-1 interacts with protein complexes containing an Argonaute protein, Dicer, and miRNAs. AIN-1 shares homology with the candidate human neurological disease protein GW182, shown to localize in cytoplasmic processing bodies that are sites of mRNA degradation and storage. A functional AIN-1::GFP also localizes at the likely worm processing bodies. When coexpressed from transgenes, AIN-1 targets ALG-1 to the foci. These results suggest a model where AIN-1 regulates a subset of miRISCs by localization to the processing bodies, facilitating degradation or translational inhibition of mRNA targets.
机译:在后生动物中,microRNA(miRNA)通过与包含Dicer和Argonaute蛋白的多蛋白miRNA诱导的沉默复合物(miRISC)结合而执行各种调节功能。 miRNA如何调节其mRNA靶标的表达仍是一个主要的研究问题。我们已经通过遗传抑制物筛选鉴定了C. elegrans ain-1基因,并显示了它与调控发育时间的异时遗传途径一起起作用。生化分析表明,AIN-1与包含Argonaute蛋白,Dicer和miRNA的蛋白复合物相互作用。 AIN-1与人类神经疾病候选蛋白GW182具有同源性,后者被证明位于mRNA降解和储存位点的细胞质加工体中。功能性AIN-1 :: GFP也位于可能的蠕虫加工体上。当从转基因中共表达时,AIN-1将ALG-1靶向到病灶。这些结果表明了一种模型,其中AIN-1通过定位到加工体来调节miRISC的子集,从而促进mRNA靶标的降解或翻译抑制。

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