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MicroRNA Genes Derived from Repetitive Elements and Expanded by Segmental Duplication Events in Mammalian Genomes

机译:MicroRNA基因来源于重复元件,并通过 哺乳动物基因组中的节段复制事件。

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摘要

MicroRNAs (miRNAs) are a class of small noncoding RNAs that regulate gene expression by targeting mRNAs for translation repression or mRNA degradation. Many miRNAs are being discovered and studied, but in most cases their origin, evolution and function remain unclear. Here, we characterized miRNAs derived from repetitive elements and miRNA families expanded by segmental duplication events in the human, rhesus and mouse genomes. We applied a comparative genomics approach combined with identifying miRNA paralogs in segmental duplication pair data in a genome-wide study to identify new homologs of human miRNAs in the rhesus and mouse genomes. Interestingly, using segmental duplication pair data, we provided credible computational evidence that two miRNA genes are located in the pseudoautosomal region of the human Y chromosome. We characterized all the miRNAs whether they were derived from repetitive elements or not and identified significant differences between the repeat-related miRNAs (RrmiRs) and non-repeat-derived miRNAs in (1) their location in protein-coding and intergenic regions in genomes, (2) the minimum free energy of their hairpin structures, and (3) their conservation in vertebrate genomes. We found some lineage-specific RrmiR families and three lineage-specific expansion families, and provided evidence indicating that some RrmiR families formed and expanded during evolutionary segmental duplication events. We also provided computational and experimental evidence for the functions of the conservative RrmiR families in the three species. Together, our results indicate that repetitive elements contribute to the origin of miRNAs, and large segmental duplication events could prompt the expansion of some miRNA families, including RrmiR families. Our study is a valuable contribution to the knowledge of evolution and function of non-coding region in genome.
机译:微小RNA(miRNA)是一类小的非编码RNA,它们通过将mRNA靶向翻译抑制或mRNA降解来调节基因表达。许多miRNA被发现和研究,但在大多数情况下,其起源,进化和功能尚不清楚。在这里,我们表征了人类,恒河猴和小鼠基因组中通过片段重复事件扩展的重复元件和miRNA家族衍生的miRNA。我们在全基因组研究中应用了比较基因组学方法,并结合了分段复制对数据中的miRNA旁系同源物来识别恒河猴和小鼠基因组中人类miRNA的新同源物。有趣的是,使用分段复制对数据,我们提供了可靠的计算证据,表明两个miRNA基因位于人Y染色体的假常染色体区域。我们对所有miRNA进行了表征,无论它们是否源自重复元件,并在以下方面确定了重复相关的miRNA(RrmiRs)和非重复的miRNA之间的显着差异:(1)它们在基因组中蛋白质编码和基因间区域的位置, (2)它们发夹结构的最小自由能,以及(3)在脊椎动物基因组中的保守性。我们发现了一些特定于谱系的RrmiR家族和三个特定于谱系的扩展家族,并提供了证据表明某些RrmiR家族在进化性节段复制事件中形成和扩展。我们还提供了三种物种中保守RrmiR家族功能的计算和实验证据。在一起,我们的结果表明重复元件有助于miRNA的起源,并且大的节段性复制事件可能促使某些miRNA家族(包括RrmiR家族)的扩张。我们的研究对基因组非编码区的进化和功能的知识做出了宝贵的贡献。

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