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人疱疹病毒糖蛋白B的增殖性T细胞应答:主要组织相容性复合体及感染顺序对交叉反应模式的影响

Proliferative T-cell response to glycoprotein B of the human herpes viruses: the influence of MHC and sequence of infection on the pattern of cross-reactivity.

作者信息

Chan W L, Tizard M L, Faulkner L

机构信息

Department of Microbiology, Guy's Medical School, UMDS, London, UK.

出版信息

Immunology. 1989 Sep;68(1):96-101.

Abstract

Oligopeptides of the highly conserved herpes virus glycoprotein B (gB) were expressed from DNA fragments of the EBV gB (BALF4) and HSV-2 gB open reading frames as fusion proteins with the lambda CII protein and beta-galactosidase (GZ), respectively, in Escherichia coli. After immunopurification using anti-gB or anti-GZ affinity columns, the fusion proteins were used in vitro to stimulate human peripheral blood lymphocytes (PBL) or murine lymph node cells that have been primed with EBV, HSV-1, HSV-2, VZV or HCMV (all human herpes viruses) to proliferate. Results obtained in BALB/c mice indicate that different herpes viruses induce different levels of T-cell response to each other and to gB, over a range of type-specific and cross-reactive T-cell epitopes. There is a lack of correlation of immunogenicity and antigenicity in the generation of T-cell responses between some of the viruses. Major T-cell epitopes are located at the C terminal half of the gB molecule. The T-cell response to gB in healthy individuals seropositive for various combinations of the five herpes viruses differed markedly from individual to individual, even when they are seropositive to the same set of herpes viruses. However, two individuals with high proliferative T-cell response to VZV and sharing HLA A2, B7, DR2 and DQw1 are also good responders for cross-reactive gB/fragments and for virus antigen of all the five herpes viruses. Therefore the data obtained demonstrated that the MHC and the immune interaction arising from cross-reactive T-cell response evoked by other herpes viruses may determine the pathogenesis of a herpes virus infection.

摘要

高度保守的疱疹病毒糖蛋白B(gB)的寡肽分别从EBV gB(BALF4)和HSV-2 gB开放阅读框的DNA片段表达,作为与λCII蛋白和β-半乳糖苷酶(GZ)的融合蛋白,在大肠杆菌中表达。使用抗gB或抗GZ亲和柱进行免疫纯化后,融合蛋白用于体外刺激已用EBV、HSV-1、HSV-2、VZV或HCMV(所有人类疱疹病毒)致敏的人外周血淋巴细胞(PBL)或小鼠淋巴结细胞增殖。在BALB/c小鼠中获得的结果表明,在一系列型特异性和交叉反应性T细胞表位范围内,不同的疱疹病毒相互之间以及对gB诱导不同水平的T细胞反应。在某些病毒之间T细胞反应的产生中,免疫原性和抗原性缺乏相关性。主要T细胞表位位于gB分子的C末端一半。对五种疱疹病毒各种组合血清学阳性的健康个体中,对gB的T细胞反应个体之间差异显著,即使他们对同一组疱疹病毒血清学阳性。然而,两名对VZV具有高增殖性T细胞反应且共享HLA A2、B7、DR2和DQw1的个体,对交叉反应性gB/片段以及所有五种疱疹病毒的病毒抗原也是良好的反应者。因此,获得的数据表明,MHC以及由其他疱疹病毒诱发的交叉反应性T细胞反应产生的免疫相互作用可能决定疱疹病毒感染的发病机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7571/1385511/618a5fe5ca21/immunology00136-0100-a.jpg

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