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在呼吸道合胞病毒G蛋白保守区域中鉴定出一种常见的HLA-DP4限制性T细胞表位。

Identification of a common HLA-DP4-restricted T-cell epitope in the conserved region of the respiratory syncytial virus G protein.

作者信息

de Waal L, Yüksel S, Brandenburg A H, Langedijk J P M, Sintnicolaas K, Verjans G M G M, Osterhaus A D M E, de Swart R L

机构信息

Department of Virology, Erasmus MC, Rotterdam, The Netherlands.

出版信息

J Virol. 2004 Feb;78(4):1775-81. doi: 10.1128/jvi.78.4.1775-1781.2004.

Abstract

The cellular immune response to respiratory syncytial virus (RSV) is important in both protection and immunopathogenesis. In contrast to HLA class I, HLA class II-restricted RSV-specific T-cell epitopes have not been identified. Here, we describe the generation and characterization of two human RSV-specific CD4(+)-T-cell clones (TCCs) associated with type 0-like cytokine profiles. TCC 1 was specific for the matrix protein and restricted over HLA-DPB11601, while TCC 2 was specific for the attachment protein G and restricted over either HLA-DPB10401 or -0402. Interestingly, the latter epitope is conserved in both RSV type A and B viruses. Given the high allele frequencies of HLA-DPB10401 and -0402 worldwide, this epitope could be widely recognized and boosted by recurrent RSV infections. Indeed, peptide stimulation of peripheral blood mononuclear cells from healthy adults resulted in the detection of specific responses in 8 of 13 donors. Additional G-specific TCCs were generated from three of these cultures, which recognized the identical (n = 2) or almost identical (n = 1) HLA-DP4-restricted epitope as TCC 2. No significant differences were found between the capacities of cell lines obtained from infants with severe (n = 41) or mild (n = 46) RSV lower respiratory tract infections to function as antigen-presenting cells to the G-specific TCCs, suggesting that the severity of RSV disease is not linked to the allelic frequency of HLA-DP4. In conclusion, we have identified an RSV G-specific human T helper cell epitope restricted by the widely expressed HLA class II alleles DPB10401 and -0402. Its putative role in protection and/or immunopathogenesis remains to be determined.

摘要

对呼吸道合胞病毒(RSV)的细胞免疫反应在保护作用和免疫发病机制中都很重要。与HLA I类分子不同,尚未鉴定出HLA II类分子限制的RSV特异性T细胞表位。在此,我们描述了两个与0型细胞因子谱相关的人RSV特异性CD4(+) T细胞克隆(TCC)的产生和特性。TCC 1对基质蛋白具有特异性,并受HLA-DPB11601限制,而TCC 2对附着蛋白G具有特异性,并受HLA-DPB10401或-0402限制。有趣的是,后一个表位在A、B两型RSV病毒中均保守。鉴于HLA-DPB10401和-0402在全球的高等位基因频率,该表位可能会被反复的RSV感染广泛识别和增强。实际上,用肽刺激健康成年人的外周血单个核细胞后,在13名供体中的8名检测到了特异性反应。从这些培养物中的3个又产生了额外的G特异性TCC,它们识别与TCC 2相同(n = 2)或几乎相同(n = 1)的HLA-DP4限制表位。在从患有严重(n = 41)或轻度(n = 46)RSV下呼吸道感染的婴儿中获得的细胞系作为G特异性TCC的抗原呈递细胞的功能能力之间未发现显著差异,这表明RSV疾病的严重程度与HLA-DP4的等位基因频率无关。总之,我们鉴定出了一个受广泛表达的HLA II类等位基因DPB10401和-0402限制的RSV G特异性人辅助性T细胞表位。其在保护和/或免疫发病机制中的假定作用仍有待确定。

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