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Structure mapping of dengue and Zika viruses reveals functional long-range interactions

机译:登革热和寨卡病毒的结构图揭示了功能性的远程相互作用

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摘要

Dengue (DENV) and Zika (ZIKV) viruses are clinically important members of the Flaviviridae family with an 11 kb positive strand RNA genome that folds to enable virus function. Here, we perform structure and interaction mapping on four DENV and ZIKV strains inside virions and in infected cells. Comparative analysis of SHAPE reactivities across serotypes nominates potentially functional regions that are highly structured, conserved, and contain low synonymous mutation rates. Interaction mapping by SPLASH identifies many pair-wise interactions, 40% of which form alternative structures, suggesting extensive structural heterogeneity. Analysis of shared interactions between serotypes reveals a conserved macro-organization whereby interactions can be preserved at physical locations beyond sequence identities. We further observe that longer-range interactions are preferentially disrupted inside cells, and show the importance of new interactions in virus fitness. These findings deepen our understanding of Flavivirus genome organization and serve as a resource for designing therapeutics in targeting RNA viruses.
机译:登革热(DENV)和寨卡(ZIKV)病毒是黄病毒科的临床重要成员,具有11 kb的正链RNA基因组,该基因组可折叠以实现病毒功能。在这里,我们对病毒体内部和感染细胞中的四种DENV和ZIKV菌株进行结构和相互作用的定位。跨血清型的SHAPE反应性的比较分析可提名高度结构化,保守且包含低同义突变率的潜在功能区域。 SPLASH的相互作用图谱鉴定了许多成对相互作用,其中40%形成了替代结构,表明存在广泛的结构异质性。对血清型之间共享相互作用的分析揭示了一个保守的宏观组织,由此可以在序列同一性以外的物理位置保留相互作用。我们进一步观察到,较长距离的相互作用优先在细胞内部被破坏,并显示出新的相互作用对病毒适应性的重要性。这些发现加深了我们对黄病毒基因组组织的了解,并为设计针对RNA病毒的治疗药物提供了资源。

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