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In-cell SHAPE uncovers dynamic interactions between the untranslated regions of the foot-and-mouth disease virus RNA

机译:细胞形状揭示了脚口病病毒RNA的未翻译区之间的动态相互作用

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摘要

The genome of RNA viruses folds into 3D structures that include long-range RNA-RNA interactions relevant to control critical steps of the viral cycle. In particular, initiation of translation driven by the IRES element of foot-and-mouth disease virus is stimulated by the 3'UTR. Here we sought to investigate the RNA local flexibility of the IRES element and the 3'UTR in living cells. The SHAPE reactivity observed in vivo showed statistically significant differences compared to the free RNA, revealing protected or exposed positions within the IRES and the 3'UTR. Importantly, the IRES local flexibility was modified in the presence of the 3'UTR, showing significant protections at residues upstream from the functional start codon. Conversely, presence of the IRES element in cis altered the 3'UTR local flexibility leading to an overall enhanced reactivity. Unlike the reactivity changes observed in the IRES element, the SHAPE differences of the 3'UTR were large but not statistically significant, suggesting multiple dynamic RNA interactions. These results were supported by covariation analysis, which predicted IRES-3'UTR conserved helices in agreement with the protections observed by SHAPE probing. Mutational analysis suggested that disruption of one of these interactions could be compensated by alternative base pairings, providing direct evidences for dynamic long-range interactions between these distant elements of the viral genome.
机译:RNA病毒的基因组折叠成3D结构,其包括与控制病毒循环的关键步骤相关的远程RNA-RNA相互作用。特别是,由3'UTR刺激由脚口病病毒的IRES元素驱动的翻译引发。在这里,我们试图研究IRES元素和3'UTR在活细胞中的RNA局部灵活性。与游离RNA相比,体内观察到的形状反应性显示出统计学上的显着差异,在IRE和3'UTR内露出保护或暴露的位置。重要的是,在3'UTR的存在下修改了IRES局部灵活性,显示出在功能起始密码子上游的残留物中的显着保护。相反,CIS中的IRE元素的存在改变了3'UTR局部灵活性,导致整体增强的反应性。与在IRES元件中观察到的反应性变化不同,3'UTR的形状差异大而不是统计学意义,表明多种动态RNA相互作用。这些结果得到了协变量分析,其预测IRES-3'UTR保守的螺旋与形状探测所观察到的保护。突变分析表明,可以通过替代碱基配对来补偿这些相互作用之一的破坏,从而为病毒基因组的这些远距离元件之间的动态远程相互作用提供直接证据。

著录项

  • 来源
    《Nucleic Acids Research》 |2017年第3期|共17页
  • 作者单位

    Univ Autonoma Madrid CSIC Centro Biol Mol Severo Ochoa Nicolas Cabrera 1 E-28049 Madrid Spain;

    Univ Autonoma Madrid CSIC Centro Biol Mol Severo Ochoa Nicolas Cabrera 1 E-28049 Madrid Spain;

    Univ Autonoma Madrid CSIC Centro Biol Mol Severo Ochoa Nicolas Cabrera 1 E-28049 Madrid Spain;

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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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