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Inverted Alu dsRNA structures do not affect localization but can alter translation efficiency of human mRNAs independent of RNA editing

机译:倒置的Alu dsRNA结构不影响定位,但可以独立于RNA编辑而改变人类mRNA的翻译效率

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With over one million copies, Alu elements are the most abundant repetitive elements in the human genome. When transcribed, interaction between two Alus that are in opposite orientation gives rise to double-stranded RNA (dsRNA). Although the presence of dsRNA in the cell was previously thought to only occur during viral infection, it is now known that cells express many endogenous small dsRNAs, such as short interfering RNA (siRNAs) and microRNA (miRNAs), which regulate gene expression. It is possible that long dsRNA structures formed from Alu elements influence gene expression. Here, we report that human mRNAs containing inverted Alu elements are present in the mammalian cytoplasm. The presence of these long intramolecular dsRNA structures within 3′-UTRs decreases translational efficiency, and although the structures undergo extensive editing in vivo, the effects on translation are independent of the presence of inosine. As inverted Alus are predicted to reside in 5% of human protein-coding genes, these intramolecular dsRNA structures are important regulators of gene expression.
机译:拥有超过一百万个拷贝的Alu元素是人类基因组中最丰富的重复元素。转录后,两个方向相反的Alus之间的相互作用会产生双链RNA(dsRNA)。尽管以前认为细胞中仅存在dsRNA,但现在知道细胞表达许多内源性小dsRNA,例如调节基因表达的短干扰RNA(siRNA)和microRNA(miRNA)。由Alu元素形成的长dsRNA结构可能会影响基因表达。在这里,我们报告哺乳动物细胞质中存在包含反向Alu元素的人类mRNA。这些长的分子内dsRNA结构在3'-UTR中的存在会降低翻译效率,尽管该结构在体内会进行广泛的编辑,但对翻译的影响与肌苷的存在无关。由于预计倒置的Alus会存在于> 5%的人类蛋白质编码基因中,因此这些分子内dsRNA结构是基因表达的重要调节剂。

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