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Probing the Structures of Viral RNA Regulatory Elements with SHAPE and Related Methodologies

机译:用SHAPE和相关方法探索病毒RNA调控元件的结构

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摘要

Viral RNAs were selected by evolution to possess maximum functionality in a minimal sequence. Depending on the classification of the virus and the type of RNA in question, viral RNAs must alternately be replicated, spliced, transcribed, transported from the nucleus into the cytoplasm, translated and/or packaged into nascent virions, and in most cases, provide the sequence and structural determinants to facilitate these processes. One consequence of this compact multifunctionality is that viral RNA structures can be exquisitely complex, often involving intermolecular interactions with RNA or protein, intramolecular interactions between sequence segments separated by several thousands of nucleotides, or specialized motifs such as pseudoknots or kissing loops. The fluidity of viral RNA structure can also present a challenge when attempting to characterize it, as genomic RNAs especially are likely to sample numerous conformations at various stages of the virus life cycle. Here we review advances in chemoenzymatic structure probing that have made it possible to address such challenges with respect to cis-acting elements, full-length viral genomes and long non-coding RNAs that play a major role in regulating viral gene expression.
机译:通过进化选择病毒RNA以最小的序列具有最大的功能。根据病毒的分类和相关RNA的类型,病毒RNA必须交替复制,剪接,转录,从细胞核转运到细胞质中,翻译和/或包装成新生的病毒体,并且在大多数情况下,必须提供序列和结构决定因素,以促进这些过程。这种紧凑的多功能性的一个结果是病毒RNA结构可能非常复杂,通常涉及与RNA或蛋白质的分子间相互作用,由数千个核苷酸分隔的序列段之间的分子内相互作用或特殊的基序,例如假结或亲吻环。试图对其进行表征时,病毒RNA结构的流动性也可能带来挑战,因为基因组RNA尤其可能在病毒生命周期的各个阶段采样众多构象。在这里,我们回顾了化学酶促结构探测的进展,这些进展使得应对顺式作用元件,全长病毒基因组和长非编码RNA在调控病毒基因表达中起主要作用的此类挑战成为可能。

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