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Hepatitis B Virus X Protein Colocalizes to Mitochondria with a Human Voltage-Dependent Anion Channel, HVDAC3, and Alters Its Transmembrane Potential

机译:乙型肝炎病毒X蛋白与人类电压依赖性阴离子通道HVDAC3共定位于线粒体,并改变其跨膜电位

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摘要

Understanding the mechanism(s) of action of the hepatitis B virus (HBV)-encoded protein HBx is fundamental to elucidating the underlying mechanisms of chronic liver disease and hepatocellular carcinoma caused by HBV infection. In our continued attempts to identify cellular targets of HBx, we have previously reported the identification of a novel cellular protein with the aid of a yeast two-hybrid assay. This cellular gene was identified as a third member of the family of human genes that encode the voltage-dependent anion channel (HVDAC3). In the present study, physical interaction between HBx and HVDAC3 was established by standard in vitro and in vivo methods. Confocal laser microscopy of transfected cells with respective expression vectors colocalized HVDAC3 and HBx to mitochondria. This novel, heretofore unreported subcellular distribution of HBx in mitochondria implies a functional role of HBx in functions associated with mitochondria. Using a stable cationic fluorophore dye, CMXRos, we show that HBx expression in cultured human hepatoma cells leads to alteration of mitochondrial transmembrane potential. Such functional roles of HBx in affecting mitochondrial physiology have implications for HBV-induced liver injury and the development of hepatocellular carcinoma.
机译:了解乙型肝炎病毒(HBV)编码蛋白HBx的作用机制对于阐明由HBV感染引起的慢性肝病和肝细胞癌的潜在机制至关重要。在我们继续尝试鉴定HBx的细胞靶标中,我们先前已经报道了借助酵母双杂交测定法鉴定新型细胞蛋白的方法。该细胞基因被鉴定为编码电压依赖性阴离子通道(HVDAC3)的人类基因家族的第三个成员。在本研究中,通过标准的体外和体内方法建立了HBx和HVDAC3之间的物理相互作用。用各自的表达载体对转染的细胞进行共聚焦激光显微镜检查,将HVDAC3和HBx共定位于线粒体。线粒体中迄今为止尚未报道的这种新的HBx亚细胞分布暗示着HBx在与线粒体相关的功能中的功能性作用。使用稳定的阳离子荧光染料CMXRos,我们显示培养的人肝癌细胞中HBx表达导致线粒体跨膜电位改变。 HBx在影响线粒体生理中的这种功能性作用对HBV诱导的肝损伤和肝细胞癌的发展有影响。

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