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特化 - 作用 RNA 元件平衡基因组环化以确保黄热病病毒的有效复制。

Specialized -Acting RNA Elements Balance Genome Cyclization to Ensure Efficient Replication of Yellow Fever Virus.

机构信息

The Centre for Infection and Immunity Studies, School of Medicine, Sun Yat-sen University, Shenzhen, Guangdong, China.

Department of Virology, State Key Laboratory of Pathogen and Biosecurity, Beijing Institute of Microbiology and Epidemiology, Academy of Military Medical Sciences, Beijing, China.

出版信息

J Virol. 2023 Apr 27;97(4):e0194922. doi: 10.1128/jvi.01949-22. Epub 2023 Apr 5.

Abstract

Genome cyclization is essential for viral RNA (vRNA) replication of the vertebrate-infecting flaviviruses, and yet its regulatory mechanisms are not fully understood. Yellow fever virus (YFV) is a notorious pathogenic flavivirus. Here, we demonstrated that a group of -acting RNA elements in YFV balance genome cyclization to govern efficient vRNA replication. It was shown that the ownstream of the 5'-yclization equence airin (DCS-HP) is conserved in the YFV clade and is important for efficient YFV propagation. By using two different replicon systems, we found that the function of the DCS-HP is determined primarily by its secondary structure and, to a lesser extent, by its base-pair composition. By combining RNA binding and chemical probing assays, we found that the DCS-HP orchestrates the balance of genome cyclization through two different mechanisms, as follows: the DCS-HP assists the correct folding of the 5' end in a linear vRNA to promote genome cyclization, and it also limits the overstabilization of the circular form through a potential crowding effect, which is influenced by the size and shape of the DCS-HP structure. We also provided evidence that an A-rich sequence downstream of the DCS-HP enhances vRNA replication and contributes to the regulation of genome cyclization. Interestingly, diversified regulatory mechanisms of genome cyclization, involving both the downstream of the 5'-cyclization sequence (CS) and the upstream of the 3'-CS elements, were identified among different subgroups of the mosquito-borne flaviviruses. In summary, our work highlighted how YFV precisely controls the balance of genome cyclization to ensure viral replication. Yellow fever virus (YFV), the prototype of the genus, can cause devastating yellow fever disease. Although it is preventable by vaccination, there are still tens of thousands of yellow fever cases per year, and no approved antiviral medicine is available. However, the understandings about the regulatory mechanisms of YFV replication are obscure. In this study, by a combination of bioinformatics, reverse genetics, and biochemical approaches, it was shown that the ownstream of the 5'-yclization equence airin (DCS-HP) promotes efficient YFV replication by modulating the conformational balance of viral RNA. Interestingly, we found specialized combinations for the downstream of the 5'-cyclization sequence (CS) and upstream of the 3'-CS elements in different groups of the mosquito-borne flaviviruses. Moreover, possible evolutionary relationships among the various downstream of the 5'-CS elements were implied. This work highlighted the complexity of RNA-based regulatory mechanisms in the flaviviruses and will facilitate the design of RNA structure-targeted antiviral therapies.

摘要

基因组环化对于脊椎动物感染的黄病毒的病毒 RNA(vRNA)复制至关重要,但调控机制尚不完全清楚。黄热病毒(YFV)是一种臭名昭著的致病性黄病毒。在这里,我们证明了一组在 YFV 中的 - 作用 RNA 元件平衡基因组环化以控制有效的 vRNA 复制。结果表明,5'-环化序列 airin(DCS-HP)的下游在黄病毒属中是保守的,对于有效的 YFV 繁殖很重要。通过使用两种不同的复制子系统,我们发现 DCS-HP 的功能主要由其二级结构决定,其次是由其碱基对组成决定。通过结合 RNA 结合和化学探测测定,我们发现 DCS-HP 通过两种不同的机制协调基因组环化的平衡,如下所示:DCS-HP 协助线性 vRNA 中 5' 端的正确折叠以促进基因组环化,并且它还通过潜在的拥挤效应限制环状形式的过度稳定,这受 DCS-HP 结构的大小和形状影响。我们还提供了证据表明,DCS-HP 下游的富含 A 的序列增强了 vRNA 复制并有助于调节基因组环化。有趣的是,在不同的蚊媒黄病毒亚群中,发现了涉及 5'-CS 下游和 3'-CS 元件上游的基因组环化的多样化调控机制。总之,我们的工作强调了 YFV 如何精确控制基因组环化的平衡以确保病毒复制。黄热病毒(YFV)是该属的原型,可以引起毁灭性的黄热病。尽管可以通过疫苗预防,但每年仍有数千例黄热病病例,并且没有批准的抗病毒药物。然而,对 YFV 复制的调控机制的理解还不清楚。在这项研究中,通过生物信息学、反向遗传学和生化方法的结合,表明 5'-环化序列 airin(DCS-HP)的下游通过调节病毒 RNA 的构象平衡促进有效的 YFV 复制。有趣的是,我们发现不同蚊媒黄病毒群中的 5'-CS 下游和 3'-CS 元件上游有专门的组合。此外,暗示了各种 5'-CS 下游之间的可能进化关系。这项工作突出了黄病毒中基于 RNA 的调控机制的复杂性,并将有助于设计针对 RNA 结构的抗病毒疗法。

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