Wellcome-Wolfson Institute for Experimental Medicine, Queen's University Belfast, Belfast, United Kingdom.
PLoS Pathog. 2024 May 16;20(5):e1012231. doi: 10.1371/journal.ppat.1012231. eCollection 2024 May.
Utilisation of RNA-binding proteins (RBPs) is an important aspect of post-transcriptional regulation of viral RNA. Viruses such as influenza A viruses (IAV) interact with RBPs to regulate processes including splicing, nuclear export and trafficking, while also encoding RBPs within their genomes, such as NP and NS1. But with almost 1000 RBPs encoded within the human genome it is still unclear what role, if any, many of these proteins play during viral replication. Using the RNA interactome capture (RIC) technique, we isolated RBPs from IAV infected cells to unravel the RBPome of mRNAs from IAV infected human cells. This led to the identification of one particular RBP, MKRN2, that associates with and positively regulates IAV mRNA. Through further validation, we determined that MKRN2 is involved in the nuclear-cytoplasmic trafficking of IAV mRNA potentially through an association with the RNA export mediator GLE1. In the absence of MKRN2, IAV mRNAs accumulate in the nucleus of infected cells, which may lead to their degradation by the nuclear RNA exosome complex. MKRN2, therefore, appears to be required for the efficient nuclear export of IAV mRNAs in human cells.
RNA 结合蛋白(RBPs)的利用是病毒 RNA 转录后调控的一个重要方面。流感 A 病毒(IAV)等病毒与 RBPs 相互作用,调节包括剪接、核输出和运输在内的过程,同时在其基因组中编码 RBPs,如 NP 和 NS1。但是,人类基因组中编码了近 1000 个 RBPs,目前仍不清楚这些蛋白质中的许多在病毒复制过程中扮演着什么角色,如果有的话。我们使用 RNA 互作组捕获(RIC)技术,从感染了 IAV 的细胞中分离出 RBPs,以揭示感染了 IAV 的人类细胞中 mRNAs 的 RBP 组。这导致鉴定出一种特定的 RBP,MKRN2,它与 IAV mRNA 结合并正向调节 IAV mRNA。通过进一步验证,我们确定 MKRN2 参与 IAV mRNA 的核质转运,可能通过与 RNA 输出介质 GLE1 相关联。在没有 MKRN2 的情况下,IAV mRNAs 在感染细胞的核内积累,这可能导致它们被核 RNA 外切酶复合物降解。因此,MKRN2 似乎是人类细胞中 IAV mRNAs 有效核输出所必需的。
