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用短肽编码组合文库对 CD8+ T 细胞的靶抗原进行无偏鉴定。

Unbiased identification of target antigens of CD8+ T cells with combinatorial libraries coding for short peptides.

机构信息

Institute of Clinical Neuroimmunology, Ludwig-Maximilians-University, Munich, Germany.

出版信息

Nat Med. 2012 May;18(5):824-8. doi: 10.1038/nm.2720.

Abstract

Cytotoxic CD8(+) T cells recognize the antigenic peptides presented by class I major histocompatibility complex (MHC) molecules. These T cells have key roles in infectious diseases, autoimmunity and tumor immunology, but there is currently no unbiased method for the reliable identification of their target antigens. This is because of the low affinities of antigen-specific T cell receptors (TCR) to their target MHC-peptide complexes, the polyspecificity of these TCRs and the requirement that these TCRs recognize protein antigens that have been processed by antigen-presenting cells (APCs). Here we describe a technology for the unbiased identification of the antigenic peptides presented by MHC class I molecules. The technology uses plasmid-encoded combinatorial peptide libraries and a single-cell detection system. We validated this approach using a well-characterized influenza-virus–specific TCR, MHC and peptide combination. Single APCs carrying antigenic peptides can be detected among several million APCs that carry irrelevant peptides. The identified peptide sequences showed a converging pattern of mimotopes that revealed the parent influenza antigen. This technique should be generally applicable to the identification of disease-relevant T cell antigens.

摘要

细胞毒性 CD8(+) T 细胞识别由 I 类主要组织相容性复合体 (MHC) 分子呈递的抗原肽。这些 T 细胞在传染病、自身免疫和肿瘤免疫学中具有关键作用,但目前尚无可靠鉴定其靶抗原的无偏方法。这是因为抗原特异性 T 细胞受体 (TCR) 与它们的靶 MHC-肽复合物的亲和力低,这些 TCR 的多特异性以及这些 TCR 识别已被抗原呈递细胞 (APC) 加工的蛋白质抗原的要求。在这里,我们描述了一种用于鉴定 MHC I 类分子呈递的抗原肽的无偏方法。该技术使用质粒编码的组合肽文库和单细胞检测系统。我们使用一种经过充分表征的流感病毒特异性 TCR、MHC 和肽组合验证了这种方法。可以在携带无关肽的几百万个 APC 中检测到携带抗原肽的单个 APC。鉴定出的肽序列显示出模拟表位的收敛模式,揭示了母体流感抗原。该技术应该普遍适用于鉴定与疾病相关的 T 细胞抗原。

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