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一类新型小RNA:tRNA衍生RNA片段(tRFs)。

A novel class of small RNAs: tRNA-derived RNA fragments (tRFs).

作者信息

Lee Yong Sun, Shibata Yoshiyuki, Malhotra Ankit, Dutta Anindya

机构信息

Department of Biochemistry and Molecular Genetics, University of Virginia, Charlottesville, Virginia 22908, USA.

出版信息

Genes Dev. 2009 Nov 15;23(22):2639-49. doi: 10.1101/gad.1837609.

Abstract

New types of small RNAs distinct from microRNAs (miRNAs) are progressively being discovered in various organisms. In order to discover such novel small RNAs, a library of 17- to 26-base-long RNAs was created from prostate cancer cell lines and sequenced by ultra-high-throughput sequencing. A significant number of the sequences are derived from precise processing at the 5' or 3' end of mature or precursor tRNAs to form three series of tRFs (tRNA-derived RNA fragments): the tRF-5, tRF-3, and tRF-1 series. These sequences constitute a class of short RNAs that are second most abundant to miRNAs. Northern hybridization, quantitative RT-PCR, and splinted ligation assays independently measured the levels of at least 17 tRFs. To demonstrate the biological importance of tRFs, we further investigated tRF-1001, derived from the 3' end of a Ser-TGA tRNA precursor transcript that is not retained in the mature tRNA. tRF-1001 is expressed highly in a wide range of cancer cell lines but much less in tissues, and its expression in cell lines was tightly correlated with cell proliferation. siRNA-mediated knockdown of tRF-1001 impaired cell proliferation with the specific accumulation of cells in G2, phenotypes that were reversed specifically by cointroducing a synthetic 2'-O-methyl tRF-1001 oligoribonucleotide resistant to the siRNA. tRF-1001 is generated in the cytoplasm by tRNA 3'-endonuclease ELAC2, a prostate cancer susceptibility gene. Our data suggest that tRFs are not random by-products of tRNA degradation or biogenesis, but an abundant and novel class of short RNAs with precise sequence structure that have specific expression patterns and specific biological roles.

摘要

在各种生物体中,与微小RNA(miRNA)不同的新型小RNA正逐渐被发现。为了发现这类新型小RNA,从前列腺癌细胞系构建了一个长度为17至26个碱基的RNA文库,并通过超高通量测序进行测序。大量序列源自成熟或前体tRNA 5'或3'端的精确加工,形成了三个系列的tRF(tRNA衍生RNA片段):tRF-5、tRF-3和tRF-1系列。这些序列构成了一类短RNA,其丰度仅次于miRNA。Northern杂交、定量RT-PCR和夹板连接试验分别测定了至少17种tRF的水平。为了证明tRF的生物学重要性,我们进一步研究了tRF-1001,它源自Ser-TGA tRNA前体转录本的3'端,该转录本在成熟tRNA中不保留。tRF-1001在多种癌细胞系中高表达,但在组织中表达较少,其在细胞系中的表达与细胞增殖密切相关。siRNA介导的tRF-1001敲低损害细胞增殖,导致细胞在G2期特异性积累,通过共导入对siRNA有抗性的合成2'-O-甲基tRF-1001寡核糖核苷酸可特异性逆转这些表型。tRF-1001由前列腺癌易感基因tRNA 3'-核酸内切酶ELAC2在细胞质中产生。我们的数据表明,tRF不是tRNA降解或生物合成的随机副产物,而是一类丰富的新型短RNA,具有精确的序列结构,具有特定的表达模式和特定的生物学作用。

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