首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Coexpression of Argonaute-2 enhances RNA interference toward perfect match binding sites
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Coexpression of Argonaute-2 enhances RNA interference toward perfect match binding sites

机译:Argonaute-2的共表达增强了对完美匹配结合位点的RNA干扰

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RNAi is widely applied to inhibit expression of specific genes, but it is limited by variable efficiency and specificity of empirically designed siRNA or shRNA constructs. This complicates studies targeting individual genes and significantly impairs large-scale screens using genome-wide knockdown libraries. Here, we show that ectopic expression of the RISC slicer Argonaute-2 (Ago2, elF2C2) dramatically enhances RNAi specifically for mRNA targets with perfectly matched binding sites. This effect depends on its endonuclease activity and is uncoupled from its regulation of microRNA expression. To model the application of Ago2 coexpression with shRNA knockdown, we targeted the EGF receptor (EGFR) in lung cancer cells exhibiting oncogene addiction to EGFR. Whereas multiple empirically designed shRNA constructs exhibited highly divergent efficiencies in mediating EGFR knockdown and cell killing, coexpression of Ago2 resulted in uniform and highly specific target gene suppression and apoptosis in EGFR-dependent cells. Codelivery of Ago2 with shRNA constructs or siRNA duplexes thus provides a strategy to enhance the efficacy and the specificity of RNAi in experimental and potentially therapeutic settings.
机译:RNAi被广泛应用于抑制特定基因的表达,但是它受到经验设计的siRNA或shRNA构建体可变效率和特异性的限制。这使针对单个基因的研究变得复杂,并严重损害了使用全基因组敲除文库的大规模筛选。在这里,我们显示RISC切片机Argonaute-2(Ago2,elF2C2)的异位表达显着增强了RNAi,专门针对具有完全匹配的结合位点的mRNA靶标。该作用取决于其核酸内切酶活性,并与其对microRNA表达的调节无关。为了模拟shRNA敲低的Ago2共表达的应用,我们针对表现出对EGFR致癌基因成瘾的肺癌细胞靶向EGF受体(EGFR)。尽管多个根据经验设计的shRNA构建体在介导EGFR敲低和细胞杀伤方面显示出高度不同的效率,但Ago2的共表达导致EGFR依赖性细胞中均匀且高度特异性的靶基因抑制和凋亡。因此,具有shRNA构建体或siRNA双链体的Ago2的代码传递提供了一种在实验和潜在治疗环境中增强RNAi的功效和特异性的策略。

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