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A transfer-RNA-derived small RNA regulates ribosome biogenesis

核糖核酸 核糖体生物发生 转移RNA 核糖体RNA 核糖体 5.8S核糖体RNA 细胞生物学 小核仁RNA 翻译(生物学) 生物 信使核糖核酸 非编码RNA 分子生物学 基因 遗传学
作者
Hak Kyun Kim,Gabriele Fuchs,Shengchun Wang,Wei Wei,Yue Zhang,Hyesuk Park,Biswajoy Roy‐Chaudhuri,Pan Li,Jianpeng Xu,Kirk Chu,Feijie Zhang,Mei‐Sze Chua,Samuel So,Qiangfeng Cliff Zhang,Peter Sarnow,Mark A. Kay
出处
期刊:Nature [Nature Portfolio]
卷期号:552 (7683): 57-62 被引量:463
标识
DOI:10.1038/nature25005
摘要

Transfer-RNA-derived small RNAs (tsRNAs; also called tRNA-derived fragments) are an abundant class of small non-coding RNAs whose biological roles are not well understood. Here we show that inhibition of a specific tsRNA, LeuCAG3′tsRNA, induces apoptosis in rapidly dividing cells in vitro and in a patient-derived orthotopic hepatocellular carcinoma model in mice. This tsRNA binds at least two ribosomal protein mRNAs (RPS28 and RPS15) to enhance their translation. A decrease in translation of RPS28 mRNA blocks pre-18S ribosomal RNA processing, resulting in a reduction in the number of 40S ribosomal subunits. These data establish a post-transcriptional mechanism that can fine-tune gene expression during different physiological states and provide a potential new target for treating cancer. A 22-nucleotide fragment of a transfer RNA regulates translation by binding to the mRNA of a ribosomal protein and increasing its expression, and downregulation of the fragment in patient-derived liver tumour cells reduces tumour growth in mice. The functional roles of small RNA fragments derived from tRNAs are not well known, but evidence is growing that some play a part in various cellular processes. Mark Kay and colleagues show that a 22-nucleotide fragment from the 3′ end of leucine tRNA can regulate translation. The fragment binds to the mRNA of a ribosomal protein to upregulate its expression. When this interaction is suppressed in human cells in culture, cell death occurs. Decreasing the levels of the tRNA fragment with an antisense oligonucleotide can slow the growth of liver tumours in mice. Technologies aimed at reducing expression of this tRNA fragment might have utility in treating cancer.
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