乙型肝炎病毒核心蛋白对于共价闭合环状 DNA 的转录调控并非必需。
Hepatitis B Virus Core Protein Is Not Required for Covalently Closed Circular DNA Transcriptional Regulation.
机构信息
State Key Laboratory of Virology and Hubei Province Key Laboratory of Allergy and Immunology, Institute of Medical Virology, TaiKang Center for Life and Medical Sciences, TaiKang Medical School, Wuhan Universitygrid.49470.3e, Wuhan, China.
Department of Laboratory Medicine, The People's Hospital of Guangxi Zhuang Autonomous Region, Nanning, China.
出版信息
J Virol. 2022 Nov 9;96(21):e0136222. doi: 10.1128/jvi.01362-22. Epub 2022 Oct 13.
Hepatitis B virus (HBV) infection is a major health burden worldwide, and currently there is no cure. The persistence of HBV covalently closed circular DNA (cccDNA) is the major obstacle for antiviral trement. HBV core protein (HBc) has emerged as a promising antiviral target, as it plays important roles in critical steps of the viral life cycle. However, whether HBc could regulate HBV cccDNA transcription remains under debate. In this study, different approaches were used to address this question. In synthesized HBV cccDNA and HBVcircle transfection assays, lack of HBc showed no effect on transcription of HBV RNA as well as HBV surface antigen (HBsAg) production in a hepatoma cell line and primary human hepatocytes. Reconstitution of HBc did not alter the expression of cccDNA-derived HBV markers. Similar results were obtained from an mouse model harboring cccDNA. Chromatin immunoprecipitation (ChIP) or ChIP sequencing assays revealed transcription regulation of HBc-deficient cccDNA chromatin similar to that of wild-type cccDNA. Furthermore, treatment with capsid assembly modulators (CAMs) dramatically reduced extracellular HBV DNA but could not alter viral RNA and HBsAg. Our results demonstrate that HBc neither affects histone modifications and transcription factor binding of cccDNA nor directly influences cccDNA transcription. Although CAMs could reduce HBc binding to cccDNA, they do not suppress cccDNA transcriptional activity. Thus, therapeutics targeting capsid or HBc should not be expected to sufficiently reduce cccDNA transcription. Hepatitis B virus (HBV) core protein (HBc) has emerged as a promising antiviral target. However, whether HBc can regulate HBV covalently closed circular DNA (cccDNA) transcription remains elusive. This study illustrated that HBc has no effect on epigenetic regulation of cccDNA, and it does not participate in cccDNA transcription. Given that HBc is dispensable for cccDNA transcription, novel cccDNA-targeting therapeutics are needed for an HBV cure.
乙型肝炎病毒 (HBV) 感染是全球范围内的一个主要健康负担,目前尚无治愈方法。HBV 共价闭合环状 DNA (cccDNA) 的持续存在是抗病毒治疗的主要障碍。HBV 核心蛋白 (HBc) 已成为一种有前途的抗病毒靶点,因为它在病毒生命周期的关键步骤中发挥重要作用。然而,HBc 是否可以调节 HBV cccDNA 转录仍存在争议。在这项研究中,使用了不同的方法来解决这个问题。在合成的 HBV cccDNA 和 HBVcircle 转染实验中,在肝癌细胞系和原代人肝细胞中,缺乏 HBc 对 HBV RNA 转录以及 HBV 表面抗原 (HBsAg) 的产生没有影响。HBc 的重建并没有改变 cccDNA 衍生的 HBV 标志物的表达。从携带 cccDNA 的小鼠模型中也获得了类似的结果。染色质免疫沉淀 (ChIP) 或 ChIP 测序实验表明,HBc 缺陷型 cccDNA 染色质的转录调控与野生型 cccDNA 相似。此外,衣壳组装调节剂 (CAMs) 的治疗显著降低了细胞外 HBV DNA,但不能改变病毒 RNA 和 HBsAg。我们的结果表明,HBc 既不影响 cccDNA 染色质的组蛋白修饰和转录因子结合,也不直接影响 cccDNA 转录。虽然 CAMs 可以减少 HBc 与 cccDNA 的结合,但它们不能抑制 cccDNA 的转录活性。因此,针对衣壳或 HBc 的治疗剂不应期望足以降低 cccDNA 转录。乙型肝炎病毒 (HBV) 核心蛋白 (HBc) 已成为一种有前途的抗病毒靶点。然而,HBc 是否可以调节 HBV 共价闭合环状 DNA (cccDNA) 的转录仍不清楚。本研究表明,HBc 对 cccDNA 的表观遗传调控没有影响,也不参与 cccDNA 转录。鉴于 HBc 对于 cccDNA 转录是可有可无的,需要新的靶向 cccDNA 的治疗方法来治愈 HBV。
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