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微小RNA如何调控基因表达?

How do microRNAs regulate gene expression?

作者信息

Jackson Richard J, Standart Nancy

机构信息

Department of Biochemistry, University of Cambridge, 80 Tennis Court Road, Cambridge CB2 1GA, UK.

出版信息

Sci STKE. 2007 Jan 2;2007(367):re1. doi: 10.1126/stke.3672007re1.

DOI:10.1126/stke.3672007re1
PMID:17200520
Abstract

Several thousand human genes, amounting to about one-third of the whole genome, are potential targets for regulation by the several hundred microRNAs (miRNAs) encoded in the genome. The regulation occurs posttranscriptionally and involves the approximately 21-nucleotide miRNA interacting with a target site in the mRNA that generally has imperfect complementarity to the miRNA. The target sites are almost invariably in the 3'-untranslated region of the messenger RNA (mRNA), often in multiple copies. Metazoan miRNAs were previously thought to down-regulate protein expression by inhibiting target mRNA translation at some stage after the translation initiation step, without much effect on mRNA abundance. However, recent studies have questioned these suppositions. With some targets, an increase in the rate of mRNA degradation by the normal decay pathway contributes to the decrease in protein expression. miRNAs can also inhibit translation initiation, specifically the function of the cap-binding initiation factor, eIF4E. Repressed target mRNAs as well as miRNAs themselves accumulate in cytoplasmic foci known as P-bodies, where many enzymes involved in mRNA degradation are concentrated. However, P-bodies may also serve as repositories for the temporary and reversible storage of untranslated mRNA, and reducing the expression (knockdown) of several distinct P-body protein components can alleviate miRNA-mediated repression of gene expression.

摘要

几千个人类基因,约占整个基因组的三分之一,是基因组中编码的几百种微小RNA(miRNA)进行调控的潜在靶点。这种调控发生在转录后,涉及大约21个核苷酸的miRNA与mRNA中的靶位点相互作用,该靶位点通常与miRNA具有不完全互补性。靶位点几乎总是位于信使RNA(mRNA)的3'非翻译区,且常常有多个拷贝。后生动物的miRNA以前被认为是通过在翻译起始步骤后的某个阶段抑制靶mRNA的翻译来下调蛋白质表达,而对mRNA丰度影响不大。然而,最近的研究对这些假设提出了质疑。对于一些靶标,正常降解途径导致的mRNA降解速率增加也会导致蛋白质表达下降。miRNA还可以抑制翻译起始,特别是帽结合起始因子eIF4E的功能。被抑制的靶mRNA以及miRNA本身会在称为P小体的细胞质聚集体中积累,许多参与mRNA降解的酶都集中在那里。然而,P小体也可能作为未翻译mRNA的临时和可逆储存库,减少几种不同的P小体蛋白成分的表达(敲低)可以减轻miRNA介导的基因表达抑制。

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