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首页> 外文期刊>Molecular cell >Systematic identification of C. elegans miRISC proteins, miRNAs, and mRNA targets by their interactions with GW182 proteins AIN-1 and AIN-2
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Systematic identification of C. elegans miRISC proteins, miRNAs, and mRNA targets by their interactions with GW182 proteins AIN-1 and AIN-2

机译:通过秀丽隐杆线虫miRISC蛋白,miRNA和mRNA靶标与GW182蛋白AIN-1和AIN-2的相互作用进行系统鉴定

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摘要

MicroRNAs (miRNAs) regulate gene expression for diverse functions, but only a limited number of mRNA targets have been experimentally identified. We show that GW182 family proteins AIN-1 and AIN-2 act redundantly to regulate the expression of miRNA targets, but not miRNA biogenesis. Immunoprecipitation (IP)and mass spectrometry indicate that AIN-1 and AIN-2 interact only with miRNA-specific Argonaute proteins ALG-1 and ALG-2 and with components of the core translational initiation complex. Known miRNA targets are enriched in AIN-2 complexes, correlating with the expression of corresponding miRNAs. Combining IP with pyrosequencing and microarray analysis of RNAs associated with AIN-1/AIN-2, we identified 106 previously annotated miRNAs plus nine new candidate miRNAs, but nearly no siRNAs, and more than 3500 potential miRNA targets, including nearly all known ones. Our results demonstrate an effective biochemical approach to systematically identify miRNA targets and provide valuable insights regarding the properties of miRNA effector complexes.
机译:MicroRNA(miRNA)调节基因表达的多种功能,但实验中仅鉴定了有限数量的mRNA靶标。我们显示,GW182家族蛋白AIN-1和AIN-2冗余地发挥作用,以调节miRNA靶标的表达,而不是miRNA生物发生。免疫沉淀(IP)和质谱分析表明AIN-1和AIN-2仅与miRNA特定的Argonaute蛋白ALG-1和ALG-2以及核心翻译起始复合物的成分相互作用。已知的miRNA靶标富含AIN-2复合物,与相应miRNA的表达相关。将IP与焦磷酸测序和与AIN-1 / AIN-2相关的RNA的微阵列分析相结合,我们确定了106个先前注释的miRNA,外加9个新的候选miRNA,但几乎没有siRNA,还有3500多个潜在的miRNA目标,包括几乎所有已知的miRNA目标。我们的结果证明了一种有效的生化方法可以系统地识别miRNA靶标,并提供有关miRNA效应子复合物特性的宝贵见解。

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