Fish Snx27 promotes viral products by modulating the innate immune response and exosomal machinery

生物 石斑鱼 病毒复制 先天免疫系统 干扰素 病毒学 病毒 细胞生物学 免疫学 免疫系统 渔业
作者
Yepin Yu,Jiaxin Liu,Zhiwen Zhao,Xiaoming Lan,Linmiao Li,Junjie Hu,Zang Ying-an,Xiujuan Zhang,Jin‐Ping Chen
出处
期刊:Journal of Virology [American Society for Microbiology]
卷期号:98 (12): e0097424-e0097424
标识
DOI:10.1128/jvi.00974-24
摘要

ABSTRACT Viral nervous necrosis caused by the nervous necrosis virus (NNV) poses a significant threat to the global aquaculture industry. Developing preventive methods to minimize economic losses due to NNV infections is crucial. This study explored the role of the sorting nexin 27 ( Snx27 ) gene, encoded by the orange-spotted grouper ( Epinephelus coioides ) and referred to as EcSnx27 , as an immune regulator affecting red-spotted grouper nervous necrosis virus (RGNNV) infection in vitro . Our findings revealed that EcSnx27 negatively regulates interferon (IFN)-related cytokines and the promoter activities of fish ISRE and NF-κB. Furthermore, we identified the SNX-FERM and SNX-FERM-like domains as responsible for the interaction between EcSnx27 and RGNNV coat protein. Through the detection of viable virions associated with EcSnx27 -containing exosomes, we propose that EcSnx27 may contribute to the release process of RGNNV by influencing the apoptosis-linked gene 2-interacting protein X (ALIX)-associated exosomal pathway. Consequently, our study suggests that EcSnx27 promotes RGNNV replication by inhibiting the IFN immune response and facilitating virus production and release through ALIX-mediated exosomal machinery. IMPORTANCE Red grouper nervous necrosis virus (RGNNV), a member of the Nodaviridae family, has emerged as a significant cause of fish diseases worldwide, leading to high morbidity and mortality rates. This study investigated the sorting nexin 27 ( Snx27 ) gene encoded by the orange-spotted grouper ( Epinephelus coioides ) on RGNNV infection in grouper kidney cells. Our findings revealed that EcSnx27 negatively regulated the interferon pathway, resulting in the promotion of RGNNV replication. Additionally, we observed that EcSnx27 could interact with apoptosis-linked gene 2-interacting protein X (ALIX) and the RGNNV coat protein, suggesting its potential involvement in viral release processes through modulation of the exosomal pathway. Our study identified EcSnx27 as a key target that RGNNV exploits to enhance viral production. This finding offers valuable insights into the immune evasion and viral release mechanisms of non-enveloped RNA viruses.
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