乙酰基转移酶 8 通过增加肠道病毒 71 非结构蛋白的稳定性促进病毒复制。
-Acetyltransferase 8 Promotes Viral Replication by Increasing the Stability of Enterovirus 71 Nonstructural Proteins.
机构信息
Department of Pathogen Biology and Immunology, Xi'an Jiaotong University Health Science Center, Xi'an, China.
Key Laboratory of Environment and Genes Related to Diseases, Xi'an Jiaotong University, Xi'an, China.
出版信息
J Virol. 2022 Mar 23;96(6):e0011922. doi: 10.1128/jvi.00119-22. Epub 2022 Feb 16.
Enterovirus 71 (EV71) is deemed a reemergent pathogen, with recent outbreaks worldwide. EV71 infection causes hand, foot, and mouth disease (HFMD) and has been associated with severe cardiac and central nervous system complications and even death. Viruses need host factors to complete their life cycle; therefore, the identification of the host factors for EV71 infection is pivotal to new antiviral research. Emerging evidence has highlighted the importance of protein acetylation during infection by various human viruses. The endoplasmic reticulum (ER), as the prominent organelle of EV71 replication, also has a unique acetylation regulation mechanism. However, the pathogenesis of EV71 and its relationship with the ER-based acetylation machinery are not fully understood. In this study, we demonstrated for the first time that the ER-resident acetyltransferase -acetyltransferase 8 (NAT8) is a host factor for EV71 infection. Inhibiting NAT8 with CRISPR or a small compound significantly suppressed EV71 infection in SK-N-SH cells. NAT8 promoted EV71 replication in an acetyltransferase-activity-dependent manner. Additionally, we found that NAT8 facilitates EV71 infection by interacting with EV71 2B, 3AB, and 3C proteins and increasing the stability of these proteins. These results uncovered a novel function of NAT8 and elucidated a new mechanism underlying the regulation of EV71 replication. EV71 is one of the most common pathogens causing HFMD in young children, and some patients experience severe or fatal neurological consequences. To ensure efficient replication, the virus must hijack multiple host factors for its own benefit. Here, we show that the ER-resident acetyltransferase NAT8 is a host factor for EV71 infection. EV71 fails to complete its infection in various cells in the absence of NAT8. We further show that NAT8 benefits EV71 replication in an acetyltransferase-activity-dependent manner. Finally, we show that NAT8 facilitates EV71 infection by interacting with EV71 2B, 3AB, and 3C proteins and increasing the stability of these proteins. These results uncovered a novel function of NAT8 in EV71 infection and elucidated a new mechanism underlying the regulation of EV71 replication.
肠道病毒 71 型(EV71)被认为是一种重新出现的病原体,最近在全球范围内爆发。EV71 感染会引起手足口病(HFMD),并与严重的心脏和中枢神经系统并发症甚至死亡有关。病毒需要宿主因素来完成其生命周期;因此,鉴定 EV71 感染的宿主因素对于新的抗病毒研究至关重要。新出现的证据强调了各种人类病毒感染过程中蛋白质乙酰化的重要性。内质网(ER)作为 EV71 复制的主要细胞器,也具有独特的乙酰化调节机制。然而,EV71 的发病机制及其与 ER 基础乙酰化机制的关系尚未完全阐明。在这项研究中,我们首次证明内质网驻留乙酰转移酶乙酰转移酶 8(NAT8)是 EV71 感染的宿主因子。用 CRISPR 或小分子化合物抑制 NAT8 可显著抑制 SK-N-SH 细胞中的 EV71 感染。NAT8 以乙酰转移酶活性依赖性方式促进 EV71 复制。此外,我们发现 NAT8 通过与 EV71 2B、3AB 和 3C 蛋白相互作用并增加这些蛋白的稳定性来促进 EV71 感染。这些结果揭示了 NAT8 的新功能,并阐明了 EV71 复制调控的新机制。EV71 是引起幼儿手足口病的最常见病原体之一,一些患者会出现严重或致命的神经后果。为了确保有效的复制,病毒必须为自身利益劫持多种宿主因素。在这里,我们表明内质网驻留乙酰转移酶 NAT8 是 EV71 感染的宿主因子。在没有 NAT8 的情况下,病毒无法在各种细胞中完成感染。我们进一步表明,NAT8 以乙酰转移酶活性依赖性方式促进 EV71 复制。最后,我们表明 NAT8 通过与 EV71 2B、3AB 和 3C 蛋白相互作用并增加这些蛋白的稳定性来促进 EV71 感染。这些结果揭示了 NAT8 在 EV71 感染中的新功能,并阐明了 EV71 复制调控的新机制。
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