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外源性抗原在启动人类CD8+ T细胞应答中的重要性:来自EBV核抗原EBNA1的启示。

The importance of exogenous antigen in priming the human CD8+ T cell response: lessons from the EBV nuclear antigen EBNA1.

作者信息

Blake N, Haigh T, Shaka'a G, Croom-Carter D, Rickinson A

机构信息

Cancer Research Campaign Institute for Cancer Studies, and Medical Research Council Centre for Immune Regulation, The Medical School, University of Birmingham, Edgbaston, Birmingham, United Kingdom.

出版信息

J Immunol. 2000 Dec 15;165(12):7078-87. doi: 10.4049/jimmunol.165.12.7078.

Abstract

Mouse models suggest that the processing of exogenous Ag by dendritic cells can be important for priming the CD8(+) CTL response. To study the situation in humans, we have exploited the CTL response to EBV infection. In this context EBV expresses eight latent proteins, of which EBV-encoded nuclear Ag (EBNA) 3A, 3B, and 3C appear to be immunodominant for CTL responses, whereas another nuclear Ag, EBNA1, which is completely protected from endogenous presentation via the MHC class I pathway, is thought to induce responses rarely, if ever. Here, using EBNA1 peptides and/or EBNA1 protein-loaded dendritic cells as in vitro stimuli, we have identified memory CTL responses to HLA-B*3501, -B7, and -B53-restricted EBNA1 epitopes that can be as strong as those seen in immunodominant epitopes from the "conventionally processed"" EBNA3 Ags. Furthermore, we used HLA-peptide tetramers to show that the primary response to one such EBNA1 epitope constituted up to 5% of the CD8(+) T cells in infectious mononucleosis blood, the strongest latent Ag-specific response yet detected in this setting. We conclude that exogenous protein represents a significant source of Ag for priming the human CTL response.

摘要

小鼠模型表明,树突状细胞对外源性抗原的处理对于启动CD8(+)细胞毒性T淋巴细胞(CTL)反应可能很重要。为了研究人类的情况,我们利用了针对EB病毒(EBV)感染的CTL反应。在这种情况下,EBV表达八种潜伏蛋白,其中EBV编码的核抗原(EBNA)3A、3B和3C似乎是CTL反应的免疫显性抗原,而另一种核抗原EBNA1通过MHC I类途径完全免受内源性提呈,被认为很少(如果有的话)诱导反应。在这里,我们使用EBNA1肽和/或负载EBNA1蛋白的树突状细胞作为体外刺激物,鉴定出了对HLA-B*3501、-B7和-B53限制性EBNA1表位的记忆CTL反应,这些反应的强度可与“传统处理”的EBNA3抗原的免疫显性表位相当。此外,我们使用HLA-肽四聚体表明,对一种这样的EBNA1表位的初次反应在传染性单核细胞增多症血液中占CD8(+) T细胞的比例高达5%,这是在这种情况下检测到的最强的潜伏抗原特异性反应。我们得出结论,外源性蛋白质是启动人类CTL反应的重要抗原来源。

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