Belnap D M, Watts N R, Conway J F, Cheng N, Stahl S J, Wingfield P T, Steven A C
Laboratory of Structural Biology and Protein Expression Laboratory, National Institute of Arthritis, Musculoskeletal, and Skin Diseases, National Institutes of Health, Bethesda, MD 20892, USA.
Proc Natl Acad Sci U S A. 2003 Sep 16;100(19):10884-9. doi: 10.1073/pnas.1834404100. Epub 2003 Sep 3.
Core antigen (cAg), the viral capsid, is one of the three major clinical antigens of hepatitis B virus. cAg has been described as presenting either one or two conformational epitopes involving the "immunodominant loop." We have investigated cAg antigenicity by cryo-electron microscopy at approximately 11-A resolution of capsids labeled with monoclonal Fabs, combined with molecular modeling, and describe here two conformational epitopes. Both Fabs bind to the dimeric external spikes, and each epitope has contributions from the loops on both subunits, explaining their discontinuous nature: however, their binding aspects and epitopes differ markedly. To date, four cAg epitopes have been characterized: all are distinct. Although only two regions of the capsid surface are accessible to antibodies, local clustering of the limited number of exposed peptide loops generates a potentially extensive set of discontinuous epitopes. This diversity has not been evident from competition experiments because of steric interference effects. These observations suggest an explanation for the distinction between cAg and e-antigen (an unassembled form of capsid protein) and an approach to immunodiagnosis, exploiting the diversity of cAg epitopes.
核心抗原(cAg),即病毒衣壳,是乙肝病毒的三种主要临床抗原之一。cAg被描述为呈现涉及“免疫显性环”的一个或两个构象表位。我们通过冷冻电子显微镜在约11埃分辨率下对用单克隆Fab标记的衣壳进行研究,并结合分子建模来研究cAg的抗原性,在此描述两个构象表位。两种Fab均与二聚体外部刺突结合,且每个表位都有来自两个亚基上的环的贡献,这解释了它们的不连续性质:然而,它们的结合方式和表位明显不同。迄今为止,已鉴定出四个cAg表位:均不相同。尽管衣壳表面只有两个区域可被抗体识别,但有限数量暴露肽环的局部聚集产生了一组潜在广泛的不连续表位。由于空间位阻干扰效应,这种多样性在竞争实验中并不明显。这些观察结果为cAg与e抗原(衣壳蛋白的未组装形式)之间的区别提供了解释,并提出了一种利用cAg表位多样性进行免疫诊断的方法。
