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树鼩肝细胞培养物的前S1抗原依赖性人乙型肝炎病毒感染

Pre-s1 antigen-dependent infection of Tupaia hepatocyte cultures with human hepatitis B virus.

作者信息

Glebe Dieter, Aliakbari Mehriar, Krass Peter, Knoop Eva V, Valerius Klaus P, Gerlich Wolfram H

机构信息

Institute of Medical Virology. Institute of Anatomy and Cell Biology, Justus Liebig University Giessen, 35392 Giessen, Germany.

出版信息

J Virol. 2003 Sep;77(17):9511-21. doi: 10.1128/jvi.77.17.9511-9521.2003.

Abstract

The susceptibility of the tree shrew Tupaia belangeri to human hepatitis B virus (HBV) has been demonstrated both in vivo and in vitro. In this study, we show that purified HBV infects primary T. belangeri hepatocyte cultures in a very specific manner, as detected by HBV covalently closed circular DNA, mRNA, HBV e antigen, and HBsAg production. A monoclonal antibody (MAb), MA18/7, directed against the pre-S1 domain of the large HBs protein, which has been shown to neutralize infectivity of HBV for primary human hepatocytes, also blocked infection of primary Tupaia hepatocytes. MAbs against the pre-S2 domain of HBs inhibited infection only partially, whereas an S MAb and polyvalent anti-HBs antibodies neutralized infection completely. Thus, both pre-S1 and S antigens are necessary for infection in the tupaia. Using subviral particles, >70% of primary Tupaia hepatocytes are capable of specific binding of pre-S1-rich HBsAg, showing localization in distinct membrane areas. The data show that the early steps of HBV infection in Tupaia hepatocyte cultures are comparable to those in the human system.

摘要

树鼩(Tupaia belangeri)对人乙型肝炎病毒(HBV)的易感性已在体内和体外得到证实。在本研究中,我们发现纯化的HBV以非常特异的方式感染原代树鼩肝细胞培养物,这可通过检测HBV共价闭合环状DNA、mRNA、HBV e抗原和HBsAg的产生来证实。一种针对大HBs蛋白前S1结构域的单克隆抗体(MAb)MA18/7已被证明可中和HBV对原代人肝细胞的感染性,它也能阻断原代树鼩肝细胞的感染。针对HBs前S2结构域的单克隆抗体仅部分抑制感染,而一种S单克隆抗体和多价抗HBs抗体可完全中和感染。因此,前S1和S抗原对于树鼩的感染都是必需的。使用亚病毒颗粒,超过70%的原代树鼩肝细胞能够特异性结合富含前S1的HBsAg,显示其定位于不同的膜区域。数据表明,树鼩肝细胞培养物中HBV感染的早期步骤与人类系统中的相似。

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