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阻断单纯疱疹病毒1型免疫球蛋白G Fc受体的免疫策略。

Immunization strategies to block the herpes simplex virus type 1 immunoglobulin G Fc receptor.

作者信息

Lin Xiaoqing, Lubinski John M, Friedman Harvey M

机构信息

Department of Medicine, Division of Infectious Diseases, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania 19104, USA.

出版信息

J Virol. 2004 Mar;78(5):2562-71. doi: 10.1128/jvi.78.5.2562-2571.2004.

Abstract

Herpes simplex virus type 1 (HSV-1) glycoprotein gE functions as an immunoglobulin G (IgG) Fc receptor (FcgammaR) that promotes immune evasion. When an IgG antibody binds by the F(ab')(2) domain to an HSV antigen, the Fc domain of some of the same antibody molecules binds to the FcgammaR, which blocks Fc-mediated functions. gE is a type 1 membrane glycoprotein with a large ectodomain that is expressed on the virion envelope and infected-cell surface. Our goal was to determine if immunizing with gE protein fragments could produce antibodies that bind by the F(ab')(2) domain to gE and block the FcgammaR, as measured by competitively inhibiting nonimmune human IgG binding to the FcgammaR. Three gE peptides were constructed in baculovirus spanning almost the entire ectodomain and used to immunize mice and rabbits. Two fragments were highly effective at producing antibodies that bind by the F(ab')(2) domain and block the FcgammaR. The most potent of these two antibodies was far more effective at blocking the FcgammaR than antibodies that are only capable of binding by the Fc domains to the FcgammaR, including anti-gC, anti-gD, and nonimmune IgG. These results suggest that immunizing with gE fragments has potential for preventing immune evasion by blocking activities mediated by the HSV-1 FcgammaR.

摘要

1型单纯疱疹病毒(HSV-1)糖蛋白gE作为一种免疫球蛋白G(IgG)Fc受体(FcγR)发挥作用,可促进免疫逃逸。当IgG抗体通过F(ab')(2)结构域与HSV抗原结合时,部分相同抗体分子的Fc结构域会与FcγR结合,从而阻断Fc介导的功能。gE是一种1型膜糖蛋白,具有一个大的胞外结构域,在病毒粒子包膜和感染细胞表面表达。我们的目标是确定用gE蛋白片段免疫是否能产生通过F(ab')(2)结构域与gE结合并阻断FcγR的抗体,这通过竞争性抑制非免疫人IgG与FcγR的结合来衡量。在杆状病毒中构建了三种几乎跨越整个胞外结构域的gE肽,并用于免疫小鼠和兔子。其中两个片段在产生通过F(ab')(2)结构域结合并阻断FcγR的抗体方面非常有效。这两种抗体中最有效的一种在阻断FcγR方面比仅能通过Fc结构域与FcγR结合的抗体(包括抗gC、抗gD和非免疫IgG)有效得多。这些结果表明,用gE片段免疫具有通过阻断HSV-1 FcγR介导的活性来预防免疫逃逸的潜力。

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