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单纯疱疹病毒(HSV)的糖蛋白gH-gL复合物可刺激产生中和抗体,并保护小鼠免受1型单纯疱疹病毒的攻击。

The gH-gL complex of herpes simplex virus (HSV) stimulates neutralizing antibody and protects mice against HSV type 1 challenge.

作者信息

Peng T, Ponce-de-Leon M, Jiang H, Dubin G, Lubinski J M, Eisenberg R J, Cohen G H

机构信息

School of Dental Medicine, and Center for Oral Health Research, University of Pennsylvania, Philadelphia 19104, USA.

出版信息

J Virol. 1998 Jan;72(1):65-72. doi: 10.1128/JVI.72.1.65-72.1998.

Abstract

The herpes simplex virus type 1 (HSV-1) gH-gL complex which is found in the virion envelope is essential for virus infectivity and is a major antigen for the host immune system. However, little is known about the precise role of gH-gL in virus entry, and attempts to demonstrate the immunologic or vaccine efficacy of gH and gL separately or as the gH-gL complex have not succeeded. We constructed a recombinant mammalian cell line (HL-7) which secretes a soluble gH-gL complex, consisting of gH truncated at amino acid 792 (gHt) and full-length gL. Purified gHt-gL reacted with gH- and gL-specific monoclonal antibodies, including LP11, which indicates that it retains its proper antigenic structure. Soluble forms of gD (gDt) block HSV infection by interacting with specific cellular receptors. Unlike soluble gD, gHt-gL did not block HSV-1 entry into cells, nor did it enhance the blocking capacity of gD. However, polyclonal antibodies to the complex did block entry even when added after virus attachment. In addition, these antibodies exhibited high titers of complement-independent neutralizing activity against HSV-1. These sera also cross-neutralized HSV-2, albeit at low titers, and cross-reacted with gH-2 present in extracts of HSV-2-infected cells. To test the potential for gHt-gL to function as a vaccine, BALB/c mice were immunized with the complex. As controls, other mice were immunized with gD purified from HSV-infected cells or were sham immunized. Sera from the gD- or gHt-gL-immunized mice exhibited high titers of virus neutralizing activity. Using a zosteriform model of infection, we challenged mice with HSV-1. All animals showed some evidence of infection at the site of virus challenge. Mice immunized with either gD or gHt-gL showed reduced primary lesions and exhibited no secondary zosteriform lesions. The sham-immunized control animals exhibited extensive secondary lesions. Furthermore, mice immunized with either gD or gHt-gL survived virus challenge, while many control animals died. These results suggest that gHt-gL is biologically active and may be a candidate for use as a subunit vaccine.

摘要

单纯疱疹病毒1型(HSV-1)的gH-gL复合物存在于病毒粒子包膜中,对病毒感染性至关重要,是宿主免疫系统的主要抗原。然而,关于gH-gL在病毒进入过程中的精确作用知之甚少,单独或以gH-gL复合物形式证明gH和gL的免疫或疫苗效力的尝试均未成功。我们构建了一种重组哺乳动物细胞系(HL-7),该细胞系分泌一种可溶性gH-gL复合物,由在氨基酸792处截短的gH(gHt)和全长gL组成。纯化的gHt-gL与gH和gL特异性单克隆抗体(包括LP11)发生反应,这表明它保留了其正确的抗原结构。可溶性形式的gD(gDt)通过与特定细胞受体相互作用来阻断HSV感染。与可溶性gD不同,gHt-gL不会阻断HSV-1进入细胞,也不会增强gD的阻断能力。然而,针对该复合物的多克隆抗体即使在病毒附着后添加也能阻断病毒进入。此外,这些抗体对HSV-1表现出高滴度的非补体依赖性中和活性。这些血清也能交叉中和HSV-2,尽管滴度较低,并且与HSV-2感染细胞提取物中存在的gH-2发生交叉反应。为了测试gHt-gL作为疫苗的潜力,用该复合物对BALB/c小鼠进行免疫。作为对照,其他小鼠用从HSV感染细胞中纯化的gD进行免疫或进行假免疫。来自gD或gHt-gL免疫小鼠的血清表现出高滴度的病毒中和活性。使用感染性带状疱疹模型,我们用HSV-1攻击小鼠。所有动物在病毒攻击部位均显示出一些感染迹象。用gD或gHt-gL免疫的小鼠原发性损伤减少,且未出现继发性带状疱疹样损伤。假免疫的对照动物出现广泛的继发性损伤。此外,用gD或gHt-gL免疫的小鼠在病毒攻击中存活下来,而许多对照动物死亡。这些结果表明gHt-gL具有生物学活性,可能是一种亚单位疫苗的候选物。

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