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The Microprocessor complex mediates the genesis of microRNAs

机译:微处理器复合体介导microRNA的起源

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MicroRNAs (miRNAs) are a growing family of small non-protein-coding regulatory genes that regulate the expression of homologous target-gene transcripts. They have been implicated in the control of cell death and proliferation in flies(1,2), haematopoietic lineage differentiation in mammals(3), neuronal patterning in nematodes(4) and leaf and flower development in plants(5-8). miRNAs are processed by the RNA-mediated interference machinery. Drosha is an RNase III enzyme that was recently implicated in miRNA processing. Here we show that human Drosha is a component of two multi-protein complexes. The larger complex contains multiple classes of RNA-associated proteins including RNA helicases, proteins that bind double-stranded RNA, novel heterogeneous nuclear ribonucleoproteins and the Ewing's sarcoma family of proteins. The smaller complex is composed of Drosha and the double-stranded-RNA-binding protein, DGCR8, the product of a gene deleted in DiGeorge syndrome. In vivo knock-down and in vitro reconstitution studies revealed that both components of this smaller complex, termed Microprocessor, are necessary and sufficient in mediating the genesis of miRNAs from the primary miRNA transcript.
机译:微小RNA(miRNA)是一个不断增长的小型非蛋白质编码调节基因家族,它们调节同源靶基因转录本的表达。它们与果蝇细胞死亡和增殖的控制(1,2),哺乳动物的造血谱系分化(3),线虫的神经元模式(4)以及植物的叶和花发育(5-8)有关。 miRNA由RNA介导的干扰机制处理。 Drosha是一种RNase III酶,最近与miRNA加工有关。在这里,我们显示了人类Drosha是两种多蛋白复合物的组成部分。较大的复合物包含多类与RNA相关的蛋白,包括RNA解旋酶,结合双链RNA的蛋白,新型异质核糖核蛋白和尤文氏肉瘤蛋白家族。较小的复合物由Drosha和双链RNA结合蛋白DGCR8组成,DGCR8是DiGeorge综合征中缺失的基因的产物。体内敲除和体外重建研究表明,这种较小的复合体(称为微处理器)的两个组件在介导主要miRNA转录本产生miRNA的过程中都是必要且充分的。

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