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TRBP将Dicer复合物招募至Ago2以进行微小RNA加工和基因沉默。

TRBP recruits the Dicer complex to Ago2 for microRNA processing and gene silencing.

作者信息

Chendrimada Thimmaiah P, Gregory Richard I, Kumaraswamy Easwari, Norman Jessica, Cooch Neil, Nishikura Kazuko, Shiekhattar Ramin

机构信息

The Wistar Institute, 3601 Spruce Street, Philadelphia, Pennsylvania 19104, USA.

出版信息

Nature. 2005 Aug 4;436(7051):740-4. doi: 10.1038/nature03868. Epub 2005 Jun 22.

Abstract

MicroRNAs (miRNAs) are generated by a two-step processing pathway to yield RNA molecules of approximately 22 nucleotides that negatively regulate target gene expression at the post-transcriptional level. Primary miRNAs are processed to precursor miRNAs (pre-miRNAs) by the Microprocessor complex. These pre-miRNAs are cleaved by the RNase III Dicer to generate mature miRNAs that direct the RNA-induced silencing complex (RISC) to messenger RNAs with complementary sequence. Here we show that TRBP (the human immunodeficiency virus transactivating response RNA-binding protein), which contains three double-stranded, RNA-binding domains, is an integral component of a Dicer-containing complex. Biochemical analysis of TRBP-containing complexes revealed the association of Dicer-TRBP with Argonaute 2 (Ago2), the catalytic engine of RISC. The physical association of Dicer-TRBP and Ago2 was confirmed after the isolation of the ternary complex using Flag-tagged Ago2 cell lines. In vitro reconstitution assays demonstrated that TRBP is required for the recruitment of Ago2 to the small interfering RNA (siRNA) bound by Dicer. Knockdown of TRBP results in destabilization of Dicer and a consequent loss of miRNA biogenesis. Finally, depletion of the Dicer-TRBP complex via exogenously introduced siRNAs diminished RISC-mediated reporter gene silencing. These results support a role of the Dicer-TRBP complex not only in miRNA processing but also as a platform for RISC assembly.

摘要

微小RNA(miRNA)通过两步加工途径产生,产生约22个核苷酸的RNA分子,这些分子在转录后水平负向调节靶基因表达。初级miRNA由微处理器复合体加工成前体miRNA(pre-miRNA)。这些pre-miRNA被核糖核酸酶III Dicer切割,产生成熟的miRNA,后者将RNA诱导沉默复合体(RISC)导向具有互补序列的信使RNA。我们在此表明,含有三个双链RNA结合结构域的TRBP(人类免疫缺陷病毒反式激活应答RNA结合蛋白)是含Dicer复合体的一个组成部分。对含TRBP复合体的生化分析揭示了Dicer-TRBP与RISC的催化引擎AGO2的关联。在使用带有Flag标签的AGO2细胞系分离三元复合体后,证实了Dicer-TRBP与AGO2的物理关联。体外重组试验表明,TRBP是将AGO2招募到与Dicer结合的小干扰RNA(siRNA)所必需的。敲低TRBP会导致Dicer不稳定,进而导致miRNA生物合成丧失。最后,通过外源引入的siRNA消耗Dicer-TRBP复合体会减少RISC介导的报告基因沉默。这些结果支持了Dicer-TRBP复合体不仅在miRNA加工中起作用,而且作为RISC组装平台的作用。

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