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Global analysis of biogenesis stability and sub-cellular localization of lncRNAs mapping to intragenic regions of the human genome

机译:映射到人类基因组内源区域的lncRNA的生物发生稳定性和亚细胞定位的全局分析

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摘要

Long noncoding RNAs (lncRNAs) that map to intragenic regions of the human genome with the same (intronic lncRNAs) or opposite orientation (antisense lncRNAs) relative to protein-coding mRNAs have been largely dismissed from biochemical and functional characterization due to the belief that they are mRNA precursors, byproducts of RNA splicing or simply transcriptional noise. In this work, we used a custom microarray to investigate aspects of the biogenesis, processing, stability, evolutionary conservation, and cellular localization of ∼6,000 intronic lncRNAs and ∼10,000 antisense lncRNAs. Most intronic (2,903 of 3,427, 85%) and antisense lncRNAs (4,945 of 5,214, 95%) expressed in HeLa cells showed evidence of 5′ cap modification, compatible with their transcription by RNAP II. Antisense lncRNAs (median t1/2 = 3.9 h) were significantly (p < 0.0001) more stable than mRNAs (median t1/2 = 3.2 h), whereas intronic lncRNAs (median t1/2 = 2.1 h) comprised a more heterogeneous class that included both stable (t1/2 > 3 h) and unstable (t1/2 < 1 h) transcripts. Intragenic lncRNAs display evidence of evolutionary conservation, have littleo coding potential and were ubiquitously detected in the cytoplasm. Notably, a fraction of the intronic and antisense lncRNAs (13 and 15%, respectively) were expressed from loci at which the corresponding host mRNA was not detected. The abundances of a subset of intronic/antisense lncRNAs were correlated (r ≥ |0.8|) with those of genes encoding proteins involved in cell division and DNA replication. Taken together, the findings of this study contribute novel biochemical and genomic information regarding intronic and antisense lncRNAs, supporting the notion that these classes include independently transcribed RNAs with potentials for exerting regulatory functions in the cell.
机译:相对于蛋白质编码mRNA映射到具有相同(内含子lncRNA)或相反方向(反义lncRNA)的人类基因组的基因内区域的长非编码RNA(lncRNA)已被人们从生化和功能表征中大为摒弃是mRNA前体,RNA剪接的副产物或简单的转录噪声。在这项工作中,我们使用定制的微阵列研究了约6,000个内含子lncRNA和约10,000个反义lncRNA的生物发生,加工,稳定性,进化保守性和细胞定位等方面。在HeLa细胞中表达的大多数内含子(2,903个,占3,427个,占85%)和反义lncRNA(4,945个,占5,214,占95%)表现出5'帽修饰的证据,与其通过RNAP II的转录相容。反义lncRNA(中位数t1 / 2 = 3.9小时)显着(p <0.0001)比mRNA(中位数t1 / 2 = 3.2小时)稳定,而内含子lncRNA(中位数t1 / 2 = 2.1小时)包含的异质性更高。包括稳定(t1 / 2> 3小时)和不稳定(t1 / 2 <1小时)成绩单。内源性lncRNAs显示出进化保守性的证据,几乎没有/没有编码潜能,并且在细胞质中被普遍检测到。值得注意的是,从未检测到相应宿主mRNA的基因座表达了一部分内含子和反义lncRNA(分别为13%和15%)。内含子/反义lncRNA子集的丰度与编码参与细胞分裂和DNA复制的蛋白质的基因的丰度相关(r≥| 0.8 |)。综上所述,这项研究的发现为内含子和反义lncRNA提供了新的生化和基因组信息,支持了以下观点:这些类别包括独立转录的RNA,具有在细胞中发挥调控功能的潜力。

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