Effects of amino acid substitutions in hepatitis B virus surface protein on virion secretion, antigenicity, HBsAg and viral DNA

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Effects of amino acid substitutions in hepatitis B virus surface protein on virion secretion, antigenicity, HBsAg and viral DNA

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作者：Kuan-hui Xiang¹ ; ² ; Eleftherios Michailidis² ; Hai Ding¹ ; Ya-qin Peng¹ ; ³ ; Ming-ze Su¹ ; Yao Li¹ ; Xue-en Liu¹ ; Viet Loan Dao Thi² ; Xian-fang Wu² ; William M. Schneider² ; Charles M. Rice² ; Hui Zhuang¹ ; ^{zhuangbmu@126.com} ; Tong Li¹ ; ^{tongli08@vip.sina.com}
关键词：HBV ; HBsAg mutation ; Virion secretion ; Antigenicity ; &lsquo ; a&rsquo ; determinant ; Hepatitis B surface antigens ; Amino acid substitution ; DNA ; Viral ; Membrane proteins
刊名：Journal of Hepatology
出版年：2017
出版时间：February 2017
年：2017
卷：66
期：2
页码：288-296
全文大小：1193 K
卷排序：66

文摘

As important virological markers, serum hepatitis B surface antigen (HBsAg) and hepatitis B virus (HBV) DNA levels show large fluctuations among chronic hepatitis B patients. The aim of this study was to reveal the potential impact and mechanisms of amino acid substitutions in small hepatitis B surface proteins (SHBs) on serum HBsAg and HBV DNA levels.MethodsSerum samples from 230 untreated chronic hepatitis B patients with genotype C HBV were analyzed in terms of HBV DNA levels, serological markers of HBV infection and SHBs sequences. In vitro functional analysis of the identified SHBs mutants was performed.ResultsAmong 230 SHBs sequences, there were 39 (16.96%) sequences with no mutation detected (wild-type) and 191 (83.04%) with single or multiple mutations. SHBs consist of 226 amino acids, of which 104 (46.02%) had mutations in our study. Some mutations (e.g., sE2G, sL21S, sR24K, sT47A/K, sC69stop (sC69∗), sL95W, sL98V, and sG145R) negatively correlated with serum HBsAg levels. HBsAg and HBV DNA levels from this group of patients had a positive correlation (r = 0.61, p <0.001). In vitro analysis showed that these mutations reduced extracellular HBsAg and HBV DNA levels by restricting virion secretion and antibody binding capacity. Virion secretion could be rescued for sE2G, sC69∗, and sG145R by co-expression of wild-type HBsAg.ConclusionThe serum HBsAg levels were lower in untreated CHB patients with novel SHBs mutations outside the major antigenic region than those without mutations. Underlying mechanisms include impairment of virion secretion and lower binding affinity to antibodies used for HBsAg measurements.Lay summaryThe hepatitis B surface antigen (HBsAg) is a major viral protein of the hepatitis B virus (HBV) secreted into patient blood serum and its quantification value serves as an important marker for the evaluation of chronic HBV infection and antiviral response. We found a few new amino acid substitutions in HBsAg associated with lower serum HBsAg and HBV DNA levels. These different substitutions might impair virion secretion, change the ability of HBsAg to bind to antibodies, or impact HBV replication. These could all result in decreased detectable levels of serum HBsAg. The factors affecting circulating HBsAg level and HBsAg detection are varied and caution is needed when interpreting clinical significance of serum HBsAg levels.Clinical trial number: NCT01088009.