永生化小鼠肝细胞中乙型肝炎病毒的病毒DNA依赖性先天免疫反应诱导
Viral DNA-Dependent Induction of Innate Immune Response to Hepatitis B Virus in Immortalized Mouse Hepatocytes.
作者信息
Cui Xiuji, Clark Daniel N, Liu Kuancheng, Xu Xiao-Dong, Guo Ju-Tao, Hu Jianming
机构信息
Department of Microbiology and Immunology, Penn State University College of Medicine, Hershey, Pennsylvania, USA.
Department of Experimental Therapeutics, Baruch S. Blumberg Institute, Doylestown, Pennsylvania, USA.
出版信息
J Virol. 2015 Oct 21;90(1):486-96. doi: 10.1128/JVI.01263-15. Print 2016 Jan 1.
UNLABELLED
Hepatitis B virus (HBV) infects hundreds of millions of people worldwide and causes acute and chronic hepatitis, cirrhosis, and hepatocellular carcinoma. HBV is an enveloped virus with a relaxed circular (RC) DNA genome. In the nuclei of infected human hepatocytes, conversion of RC DNA from the incoming virion or cytoplasmic mature nucleocapsid (NC) to the covalently closed circular (CCC) DNA, which serves as the template for producing all viral transcripts, is essential to establish and sustain viral replication. A prerequisite for CCC DNA formation is the uncoating (disassembly) of NCs to expose their RC DNA content for conversion to CCC DNA. We report here that in an immortalized mouse hepatocyte cell line, AML12HBV10, in which RC DNA exposure is enhanced, the exposed viral DNA could trigger an innate immune response that was able to modulate viral gene expression and replication. When viral gene expression and replication were low, the innate response initially stimulated these processes but subsequently acted to shut off viral gene expression and replication after they reached peak levels. Inhibition of viral DNA synthesis or cellular DNA sensing and innate immune signaling diminished the innate response. These results indicate that HBV DNA, when exposed in the host cell cytoplasm, can function to trigger an innate immune response that, in turn, modulates viral gene expression and replication.
IMPORTANCE
Chronic infection by hepatitis B virus (HBV) afflicts hundreds of millions worldwide and is sustained by the episomal covalently closed circular (CCC) DNA in the nuclei of infected hepatocytes. Release of viral genomic DNA from cytoplasmic nucleocapsids (NCs) (NC disassembly or uncoating) is a prerequisite for its conversion to CCC DNA, which can also potentially expose the viral DNA to host DNA sensors and trigger an innate immune response. We have found that in an immortalized mouse hepatocyte cell line in which efficient CCC DNA formation was associated with enhanced exposure of nucleocapsid-associated DNA, the exposed viral DNA indeed triggered host cytoplasmic DNA sensing and an innate immune response that was able to modulate HBV gene expression and replication. Thus, HBV can, under select conditions, be recognized by the host innate immune response through exposed viral DNA, which may be exploited therapeutically to clear viral persistence.
未标记
乙肝病毒(HBV)感染了全球数亿人,可导致急性和慢性肝炎、肝硬化及肝细胞癌。HBV是一种具有松弛环状(RC)DNA基因组的包膜病毒。在受感染的人类肝细胞的细胞核中,将来自进入的病毒粒子或细胞质成熟核衣壳(NC)的RC DNA转化为共价闭合环状(CCC)DNA对于建立和维持病毒复制至关重要,CCC DNA是产生所有病毒转录本的模板。CCC DNA形成的一个先决条件是NC的脱壳(解体),以暴露其RC DNA内容物以便转化为CCC DNA。我们在此报告,在一种永生化小鼠肝细胞系AML12HBV10中,RC DNA暴露增强,暴露的病毒DNA可触发一种能够调节病毒基因表达和复制的先天免疫反应。当病毒基因表达和复制水平较低时,先天反应最初会刺激这些过程,但在它们达到峰值水平后,随后会抑制病毒基因表达和复制。抑制病毒DNA合成或细胞DNA传感及先天免疫信号传导会减弱先天反应。这些结果表明,HBV DNA在宿主细胞质中暴露时,可触发一种先天免疫反应,进而调节病毒基因表达和复制。
重要性
乙肝病毒(HBV)的慢性感染困扰着全球数亿人,并且由受感染肝细胞细胞核中的游离共价闭合环状(CCC)DNA维持。从细胞质核衣壳(NC)释放病毒基因组DNA(NC解体或脱壳)是其转化为CCC DNA的先决条件,这也可能使病毒DNA暴露于宿主DNA传感器并触发先天免疫反应。我们发现,在一种永生化小鼠肝细胞系中,有效的CCC DNA形成与核衣壳相关DNA的暴露增强有关,暴露的病毒DNA确实触发了宿主细胞质DNA传感和一种能够调节HBV基因表达和复制的先天免疫反应。因此,在特定条件下HBV可通过暴露的病毒DNA被宿主先天免疫反应识别,这可用于治疗以清除病毒持续性感染。
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