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首页> 外文期刊>ACS Omega >Hepatitis B Virus Oncoprotein HBx Is Not an ATPase
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Hepatitis B Virus Oncoprotein HBx Is Not an ATPase

机译:乙型肝炎病毒癌蛋白HBX不是ATP酶

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HBx is the smallest gene product of the Hepatitis B virus (HBV) and an oncogenic stimulus in chronic infections leading to liver disease. HBx interacts and interferes with numerous cellular processes, but its modes of action remain poorly understood. It has been invoked that HBx employs nucleotide hydrolysis to regulate molecular pathways or protein–protein interactions. In the present study, we reinvestigate the (d)NTP hydrolysis of recombinant HBx to explore its potential as a biochemical probe for antiviral studies. For our investigations, we employed existing soluble constructs (i.e., GST-HBx, MBP-HBx) and engineered new fusion proteins (i.e., DsbC-HBx, NusA-HBx), which are shown to serve as better systems for in vitro research. We performed mutational scanning of the computationally predicted NTP-binding domain, which includes residues associated with clinical cases. Steady-state and end-point activity assays, in tandem with mass-spectrometric analyses, reveal that the observed hydrolysis of all alleged HBx substrates, ATP, dATP, and GTP, is contingent on the presence of the GroEL chaperone, which preferentially copurifies as a contaminant with GST-HBx and MBP-HBx. Collectively, our findings provide new technical standards for recombinant HBx studies and reveal that nucleotide hydrolysis is not an operant mechanism by which HBx contributes to viral HBV carcinogenesis.
机译:HBX是乙型肝炎病毒(HBV)的最小基因产物和慢性感染的致癌刺激,导致肝病。 HBX与许多细胞过程相互作用并干扰,但其作用方式仍然明白很差。已经调用HBX使用核苷酸水解以调节分子途径或蛋白质 - 蛋白质相互作用。在本研究中,我们将重组HBX的(d)NTP水解加强(d)NTP水解,以探讨其作为抗病毒研究的生化探针的潜力。对于我们的研究,我们使用现有的可溶性构建体(即GST-HBX,MBP-HBX)和工程化的新融合蛋白(即DSBC-HBX,NUSA-HBX),其被证明为更好的系统体外研究。我们对计算预期的NTP结合结构域进行了突变扫描,其包括与临床病例相关的残基。稳态和终点活性测定,串联具有质谱分析,揭示了所谓的HBX底物,ATP,DATP和GTP的检测到的水解在腹股沟伴侣的存在下,其优先将其共用具有GST-HBX和MBP-HBX的污染物。集体,我们的研究结果为重组HBX研究提供了新的技术标准,并揭示了核苷酸水解不是一种操作机制,通过该方法,HBX对病毒HBV致癌作用。

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