Department of Virology II, National Institute of Infectious Diseases, Tokyo, Japan.
Department of Microbial Biotechnology, Division of Genetic Engineering and Biotechnology Research, National Research Centre, Giza, Egypt.
J Virol. 2021 Jul 12;95(15):e0076721. doi: 10.1128/JVI.00767-21.
Hepatitis B virus (HBV) is a stealth virus that exhibits only minimal induction of the interferon system, which is required for both innate and adaptive immune responses. However, 90% of acutely infected adults can clear the virus, suggesting the presence of additional mechanisms that facilitate viral clearance. Here, we report that Maf bZIP transcription factor F (MafF) promotes host defense against infection with HBV. Using a small interfering RNA (siRNA) library and an HBV/NanoLuc (NL) reporter virus, we screened to identify anti-HBV host factors. Our data showed that silencing of led to a 6-fold increase in luciferase activity after HBV/NL infection. Overexpression of MafF reduced HBV core promoter transcriptional activity, which was relieved upon mutation of the putative MafF binding region. Loss of MafF expression through CRISPR/Cas9 editing (in HepG2-hNTCP-C4 cells) or siRNA silencing (in primary hepatocytes [PXB cells]) induced HBV core RNA and HBV pregenomic RNA (pgRNA) levels, respectively, after HBV infection. MafF physically binds to the HBV core promoter and competitively inhibits HNF-4α binding to an overlapping sequence in the HBV enhancer II sequence (EnhII), as seen by chromatin immunoprecipitation (ChIP) analysis. MafF expression was induced by interleukin-1β (IL-1β) or tumor necrosis factor alpha (TNF-α) treatment in both HepG2 and PXB cells, in an NF-κB-dependent manner. Consistently, expression levels were significantly enhanced and positively correlated with the levels of these cytokines in patients with chronic HBV infection, especially in the immune clearance phase. HBV is a leading cause of chronic liver diseases, infecting about 250 million people worldwide. HBV has developed strategies to escape interferon-dependent innate immune responses. Therefore, the identification of other anti-HBV mechanisms is important for understanding HBV pathogenesis and developing anti-HBV strategies. MafF was shown to suppress transcription from the HBV core promoter, leading to significant suppression of the HBV life cycle. Furthermore, MafF expression was induced in chronic HBV patients and in primary human hepatocytes (PXB cells). This induction correlated with the levels of inflammatory cytokines (IL-1β and TNF-α). These data suggest that the induction of MafF contributes to the host's antiviral defense by suppressing transcription from selected viral promoters. Our data shed light on a novel role for MafF as an anti-HBV host restriction factor.
乙型肝炎病毒(HBV)是一种隐匿性病毒,仅能轻微诱导干扰素系统,这是固有和适应性免疫反应所必需的。然而,90%的急性感染成年人可以清除病毒,这表明存在促进病毒清除的其他机制。在这里,我们报告 Maf bZIP 转录因子 F(MafF)促进宿主对乙型肝炎病毒感染的防御。我们使用小干扰 RNA(siRNA)文库和乙型肝炎病毒/NanoLuc(NL)报告病毒进行筛选,以鉴定抗乙型肝炎病毒的宿主因子。我们的数据表明,沉默 可导致乙型肝炎病毒/NL 感染后荧光素酶活性增加 6 倍。MafF 的过表达降低了乙型肝炎病毒核心启动子的转录活性,而突变假定的 MafF 结合区域则缓解了该活性。通过 CRISPR/Cas9 编辑(在 HepG2-hNTCP-C4 细胞中)或 siRNA 沉默(在原代肝细胞[PXB 细胞]中)丧失 MafF 表达,分别在乙型肝炎病毒感染后诱导乙型肝炎病毒核心 RNA 和乙型肝炎病毒前基因组 RNA(pgRNA)水平升高。MafF 通过染色质免疫沉淀(ChIP)分析,物理结合到乙型肝炎病毒核心启动子上,并竞争性抑制 HNF-4α与乙型肝炎病毒增强子 II 序列(EnhII)中的重叠序列结合。白细胞介素-1β(IL-1β)或肿瘤坏死因子-α(TNF-α)处理可在 HepG2 和 PXB 细胞中诱导 MafF 表达,这是一种 NF-κB 依赖性方式。一致的是,在慢性乙型肝炎病毒感染患者中, 表达水平显著增强,并与这些细胞因子的水平呈正相关,尤其是在免疫清除阶段。 乙型肝炎病毒是导致慢性肝病的主要原因,全世界约有 2.5 亿人感染。乙型肝炎病毒已经开发出逃避干扰素依赖的先天免疫反应的策略。因此,鉴定其他抗乙型肝炎病毒的机制对于了解乙型肝炎病毒的发病机制和开发抗乙型肝炎病毒的策略非常重要。MafF 被证明可抑制乙型肝炎病毒核心启动子的转录,从而显著抑制乙型肝炎病毒的生命周期。此外,MafF 在慢性乙型肝炎病毒患者和原代人肝细胞(PXB 细胞)中表达诱导。这种诱导与炎症细胞因子(IL-1β 和 TNF-α)的水平相关。这些数据表明,MafF 的诱导通过抑制选定的病毒启动子的转录,有助于宿主的抗病毒防御。我们的数据揭示了 MafF 作为一种抗乙型肝炎病毒宿主限制因子的新作用。
