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ADAR2 induces reproducible changes in sequence and abundance of mature microRNAs in the mouse brain

机译:ADAR2诱导小鼠脑中成熟微稻草的序列和丰度的可重复变化

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摘要

Adenosine deaminases that act on RNA (ADARs) deaminate adenosines to inosines in double-stranded RNAs including miRNA precursors. A to I editing is widespread and required for normal life. By comparing deep sequencing data of brain miRNAs from wild-type and ADAR2 deficient mouse strains, we detect editing sites and altered miRNA processing at high sensitivity. We detect 48 novel editing events in miRNAs. Some editing events reach frequencies of up to 80%. About half of all editing events depend on ADAR2 while some miRNAs are preferentially edited by ADAR1. Sixty-four percent of all editing events are located within the seed region of mature miRNAs. For the highly edited miR-3099, we experimentally prove retargeting of the edited miRNA to novel 3'-UTRs. We show further that an abundant editing event in miR-497 promotes processing by Drosha of the corresponding pri-miRNA. We also detect reproducible changes in the abundance of specific miRNAs in ADAR2-deficient mice that occur independent of adjacent A to I editing events. This indicates that ADAR2 binding but not editing of miRNA precursors may influence their processing. Correlating with changes in miRNA abundance we find misregulation of putative targets of these miRNAs in the presence or absence of ADAR2.
机译:在RNA(ADARS)上作用的腺苷脱氨酶将腺苷延长到包括miRNA前体的双链RNA中的毒液中。 A对我的编辑普遍存在,正常生活所需。通过比较来自野生型和ADAR2缺乏小鼠菌株的脑miRNA的深度测序数据,我们检测编辑位点并以高灵敏度改变miRNA处理。我们在MiRNA中检测到48个新颖的编辑事件。一些编辑事件达到高达80%的频率。大约一半的所有编辑事件都依赖于ADAR2,而一些MIRNA优先由ADAR1编辑。所有编辑事件中的六十四个百分之六十四个位于成熟MiRNA的种子区域内。对于高度编辑的miR-3099,我们通过实验证明编辑的miRNA重新定位为新的3'-UTR。我们进一步展示MIR-497中的丰富编辑事件促进了相应的PRI-miRNA的DROSHA的处理。我们还检测到缺陷的小鼠中特定miRNA的丰度的可重复变化,该小鼠与I邻近A与I编辑事件不同。这表明ADAR2结合但未对miRNA前体进行编辑可能影响其处理。与miRNA丰富的变化相关,我们在存在或不存在ADAR2中找到了这些miRNA的推定靶标的靶向的错误化。

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  • 来源
    《Nucleic Acids Research》 |2014年第19期|共14页
  • 作者单位

    Univ Vienna Max F Perutz Labs Dept Chromosome Biol A-1030 Vienna Austria;

    Univ Vienna Max F Perutz Labs Ctr Integrat Bioinformat Vienna A-1030 Vienna Austria;

    Univ Vienna Max F Perutz Labs Ctr Integrat Bioinformat Vienna A-1030 Vienna Austria;

    Univ Vienna Max F Perutz Labs Dept Chromosome Biol A-1030 Vienna Austria;

    Univ Vienna Max F Perutz Labs Ctr Integrat Bioinformat Vienna A-1030 Vienna Austria;

    Univ Vienna Max F Perutz Labs Dept Chromosome Biol A-1030 Vienna Austria;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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