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Functionally conserved architecture of hepatitis C virus RNA genomes

机译:丙型肝炎病毒RNA基因组的功能保守结构

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摘要

Hepatitis C virus (HCV) infects over 170 million people worldwide and is a leading cause of liver disease and cancer. The virus has a 9,650-nt, single-stranded, messenger-sense RNA genome that is infectious as an independent entity. The RNA genome has evolved in response to complex selection pressures, including the need to maintain structures that facilitate replication and to avoid clearance by cell-intrinsic immune processes. Here we used high-throughput, single-nucleotide resolution information to generate and functionally test data-driven structural models for three diverse HCV RNA genomes. We identified, de novo, multiple regions of conserved RNA structure, including all previously characterized cis-acting regulatory elements and also multiple novel structures required for optimal viral fitness. Well-defined RNA structures in the central regions of HCV genomes appear to facilitate persistent infection by masking the genome from RNase L and double-stranded RNA-induced innate immune sensors. This work shows how structure-first comparative analysis of entire genomes of a pathogenic RNA virus enables comprehensive and concise identification of regulatory elements and emphasizes the extensive interrelationships among RNA genome structure, viral biology, and innate immune responses.
机译:丙型肝炎病毒(HCV)感染全球超过1亿7千万人,是肝脏疾病和癌症的主要原因。该病毒具有9,650 nt的单链信使感知RNA基因组,可作为独立实体进行感染。 RNA基因组已经响应复杂的选择压力而进化,包括需要维持有利于复制的结构并避免通过细胞内免疫过程清除。在这里,我们使用了高通量的单核苷酸分辨率信息来生成和功能测试三个不同的HCV RNA基因组的数据驱动的结构模型。我们从头确定了保守RNA结构的多个区域,包括所有先前表征的顺式调控元件,以及最佳病毒适应性所需的多个新颖结构。 HCV基因组中心区域中定义良好的RNA结构似乎可以通过掩盖RNase L和双链RNA诱导的先天性免疫传感器的基因组来促进持续感染。这项工作显示了对致病性RNA病毒整个基因组的结构优先比较分析如何能够全面,简明地鉴定调控元件,并强调了RNA基因组结构,病毒生物学和先天免疫反应之间广泛的相互关系。

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