Long noncoding RNA #61 exerts a broad anti-influenza a virus effect by its long arm rings

生物 病毒复制 甲型流感病毒 病毒 病毒学 聚合酶 H5N1亚型流感病毒 病毒生命周期 核出口信号 RNA聚合酶 病毒进入 核糖核酸 长非编码RNA 细胞生物学 基因 遗传学
作者
Jiao Hu,Lei Zhang,Xinxin Zheng,Guoqing Wang,Xia Chen,Zenglei Hu,Yu Chen,Xiaoquan Wang,Min Gu,Shunlin Hu,Xiaowen Liu,Xinan Jiao,Daxin Peng,Xiufan Liu
出处
期刊:Antiviral Research [Elsevier]
卷期号:215: 105637-105637 被引量:1
标识
DOI:10.1016/j.antiviral.2023.105637
摘要

Emerging evidence has demonstrated the critical role of long noncoding RNAs (lncRNAs) in regulating gene expression. However, the functional significance and mechanisms underlying influenza A virus (IAV)-host lncRNA interactions are still elusive. Here, we identified a functional lncRNA, LncRNA#61, as a broad anti-IAV factor. LncRNA#61 is highly upregulated by different subtypes of IAV, including human H1N1 virus and avian H5N1 and H7N9 viruses. Furthermore, nuclear-enriched LncRNA#61 can translocate from the nucleus to the cytoplasm soon after IAV infection. Forced LncRNA#61 expression dramatically impedes viral replication of various subtypes of IAV, including human H1N1 virus and avian H3N2/N8, H4N6, H5N1, H6N2/N8, H7N9, H8N4, H10N3, H11N2/N6/N9 viruses. Conversely, abolishing LncRNA#61 expression substantially favored viral replication. More importantly, LncRNA#61 delivered by the lipid nanoparticle (LNP)-encapsulated strategy shows good performance in restraining viral replication in mice. Interestingly, LncRNA#61 is involved in multiple steps of the viral replication cycle, including virus entry, viral RNA synthesis and the virus release period. Mechanistically, the four long ring arms of LncRNA#61 mainly mediate its broad antiviral effect and contribute to its inhibition of viral polymerase activity and nuclear aggregation of key polymerase components. Therefore, we defined LncRNA#61 as a potential broad-spectrum antiviral factor for IAV. Our study further extends our understanding of the stunning and unanticipated biology of lncRNAs as well as their close interaction with IAV, providing valuable clues for developing novel broad anti-IAV therapeutics targeting host lncRNAs.
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