TRIM56 impairs HBV infection and replication by inhibiting HBV core promoter activity

cccDNA 乙型肝炎病毒 乙型肝炎病毒β前体 病毒学 病毒复制 生物 先天免疫系统 抄写(语言学) HBeAg 效应器 病毒 分子生物学 免疫系统 细胞生物学 乙型肝炎病毒DNA聚合酶 免疫学 乙型肝炎表面抗原 哲学 语言学
作者
Xing Tian,Huijun Dong,Xinyuan Lai,Guomin Ou,Junning Cao,Jihang Shi,Chengang Xiang,Lei Wang,Xuechao Zhang,Kai Zhang,Ji Soo Song,Juan Deng,Hongkui Deng,Shichun Lu,Hui Zhuang,Tong Li,Kuanhui Xiang
出处
期刊:Antiviral Research [Elsevier BV]
卷期号:207: 105406-105406 被引量:33
标识
DOI:10.1016/j.antiviral.2022.105406
摘要

Members of the tripartite motif (TRIM) protein family strongly induced by interferons (IFNs) are parts of the innate immune system with antiviral activity. However, it is still unclear which TRIMs could play important roles in hepatitis B virus (HBV) inhibition. Here, we identified that TRIM56 expression responded in IFN-treated HepG2-NTCP cells and HBV-infected liver tissues, which was a potent IFN-inducible inhibitor of HBV replication. Mechanistically, TRIM56 suppressed HBV replication via its Ring and C-terminal domain. C-terminal domain was essential for TRIM56 translocating from cytoplasm to nucleus during HBV infection. Further analysis revealed that TRIM56's Ring domain targeted IκBα for ubiquitination. This modification induced phosphorylation of p65, which subsequently inhibited HBV core promoter activity, resulting in the inhibition of HBV replication. The p65 was found to be necessary for NF-κB signal pathway to inhibit HBV replication. We verified our findings using HepG2-NTCP and primary human hepatocytes. Our findings reveal that TRIM56 is a critical antiviral immune effector and exerts an anti-HBV activity via NF-κB signal pathway, which is essential for inhibiting transcription of HBV covalently closed circular DNA.
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