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乙型肝炎前核心/核心相关抗原的表征
作者:Xupeng Hong https://orcid.org/0000-0002-7091-6108、Laurie Luckenbaugh、Megan Mendenhall、Renae Walsh、Liza Cabuang、Sally Soppe、Peter A. Revill、Dara Burdette、Becket Feierbach、William Delaney、Jianming胡 https://orcid.org/0000-0002-3967-2133Authors Info & AffiliationsAuthors Info & Affiliations
DOI:https://doi.org/10.1128/JVI.01695-20
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    合资公司
    第 95 卷,第 3 期
    2021 年 1 月 13 日
        抽象的
        介绍
        结果
        讨论
        材料和方法
        致谢
        参考

抽象的
目前的疗法很少治愈慢性乙型肝炎病毒 (HBV) 感染,因为肝细胞中存在病毒附加体,即共价闭合环状 DNA (cccDNA)。乙型肝炎病毒核心相关抗原 (HBcrAg) 是病毒前核心/核心基因产物的混合物,已成为监测肝内 cccDNA 水平和活性的一种潜在标志物。在这项研究中,对前核心/核心基因产物的综合表征表明,HBcrAg 成分包括经典的乙型肝炎病毒核心抗原 (HBc) 和 e 抗原 (HBeAg),此外,前核心相关抗原 PreC,保留了 N-末端信号肽。 HBeAg 和 PreC 抗原在其 C 末端均表现出异质蛋白水解加工,从而导致多种物种,这些物种因病毒基因型而异。 HBeAg 是 HBeAg 阳性患者中 HBcrAg 的主要形式。 HBcrAg 与 PreC 之间、HBcrAg 与 HBeAg 之间、PreC 与 HBeAg 之间均存在正相关,但 HBcrAg 与 HBc 之间不存在正相关。血清 HBeAg 和 PreC 具有相似的浮力密度和大小分布,并且都表现出密度和大小的异质性。 HBc,但不是 HBeAg 或 PreC 抗原,被发现是含 DNA 或空病毒体中衣壳的主要成分。在生理条件下,HBeAg 和 PreC 蛋白都不能在细胞内或体外形成衣壳。总之,我们的研究提供了关于前核心/核心基因产物各组分水平及其生化和生物物理特征的重要新定量信息,这意味着每个组分在反映肝内病毒活性方面可能具有不同的功能和应用。
重要性 慢性乙型肝炎病毒 (HBV) 感染折磨着大约 2.57 亿人,他们极有可能发展为慢性肝病,包括纤维化、肝硬化和肝细胞癌。由于 HBV 附加体,即共价闭合环状 DNA (cccDNA) 在受感染肝细胞的细胞核中的持续存在,目前的疗法很少能治愈 HBV 感染。迫切需要cccDNA水平和转录活性的外周标志物来指导抗病毒治疗和药物开发。血清乙型肝炎核心相关抗原 (HBcrAg) 就是这样一种新兴的外周标志物。我们已经对 HBV 感染患者以及细胞培养物中的 HBcrAg 成分进行了表征。我们的结果提供了关于每种 HBcrAg 成分水平及其生化和生物物理特征的重要新定量信息。我们的研究结果表明,每种 HBcrAg 成分在反映肝内病毒活性方面可能具有不同的功能和应用。

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Characterization of Hepatitis B Precore/Core-Related Antigens
Authors: Xupeng Hong https://orcid.org/0000-0002-7091-6108, Laurie Luckenbaugh, Megan Mendenhall, Renae Walsh, Liza Cabuang, Sally Soppe, Peter A. Revill, Dara Burdette, Becket Feierbach, William Delaney, Jianming Hu https://orcid.org/0000-0002-3967-2133Authors Info & AffiliationsAuthors Info & Affiliations
DOI: https://doi.org/10.1128/JVI.01695-20
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    JVI
    Volume 95, Number 3
    13 January 2021
        ABSTRACT
        INTRODUCTION
        RESULTS
        DISCUSSION
        MATERIALS AND METHODS
        ACKNOWLEDGMENTS
        REFERENCES

ABSTRACT
Current therapies rarely cure chronic hepatitis B virus (HBV) infection due to the persistence of the viral episome, the covalently closed circular DNA (cccDNA), in hepatocytes. The hepatitis B virus core-related antigen (HBcrAg), a mixture of the viral precore/core gene products, has emerged as one potential marker to monitor the levels and activities of intrahepatic cccDNA. In this study, a comprehensive characterization of precore/core gene products revealed that HBcrAg components included the classical hepatitis B virus core antigen (HBc) and e antigen (HBeAg) and, additionally, the precore-related antigen, PreC, retaining the N-terminal signal peptide. Both HBeAg and PreC antigens displayed heterogeneous proteolytic processing at their C termini resulting in multiple species, which varied with viral genotypes. HBeAg was the predominant form of HBcrAg in HBeAg-positive patients. Positive correlations were found between HBcrAg and PreC, between HBcrAg and HBeAg, and between PreC and HBeAg but not between HBcrAg and HBc. Serum HBeAg and PreC shared similar buoyant density and size distributions, and both displayed density and size heterogeneity. HBc, but not HBeAg or PreC antigen, was found as the main component of capsids in DNA-containing or empty virions. Neither HBeAg nor PreC protein was able to form capsids in cells or in vitro under physiological conditions. In conclusion, our study provides important new quantitative information on levels of each component of precore/core gene products as well as their biochemical and biophysical characteristics, implying that each component may have distinct functions and applications in reflecting intrahepatic viral activities.
IMPORTANCE Chronic hepatitis B virus (HBV) infection afflicts approximately 257 million people, who are at high risk of progressing to chronic liver diseases, including fibrosis, cirrhosis, and hepatocellular carcinoma. Current therapies rarely achieve cure of HBV infection due to the persistence of the HBV episome, the covalently closed circular DNA (cccDNA), in the nuclei of infected hepatocytes. Peripheral markers of cccDNA levels and transcriptional activities are urgently required to guide antiviral therapy and drug development. Serum hepatitis B core-related antigen (HBcrAg) is one such emerging peripheral marker. We have characterized the components of HBcrAg in HBV-infected patients as well as in cell cultures. Our results provide important new quantitative information on levels of each HBcrAg component, as well as their biochemical and biophysical characteristics. Our findings suggest that each HBcrAg component may have distinct functions and applications in reflecting intrahepatic viral activities.

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