Sant Sneha, Grzelak Ludivine, Wang Zhongfang, Pizzolla Angela, Koutsakos Marios, Crowe Jane, Loudovaris Thomas, Mannering Stuart I, Westall Glen P, Wakim Linda M, Rossjohn Jamie, Gras Stephanie, Richards Michael, Xu Jianqing, Thomas Paul G, Loh Liyen, Nguyen Thi H O, Kedzierska Katherine
Department of Microbiology and Immunology, Peter Doherty Institute for Infection and Immunity, University of Melbourne, Melbourne, VIC, Australia.
École Normale Supérieure Paris-Saclay, Université Paris-Saclay, Cachan, France.
Front Immunol. 2018 Jun 27;9:1453. doi: 10.3389/fimmu.2018.01453. eCollection 2018.
CD8 T cells recognizing antigenic peptides derived from conserved internal viral proteins confer broad protection against distinct influenza viruses. As memory CD8 T cells change throughout the human lifetime and across tissue compartments, we investigated how T cell receptor (TCR) composition and diversity relate to memory CD8 T cells across anatomical sites and immunological phases of human life. We used peptide-HLA tetramer magnetic enrichment, single-cell multiplex RT-PCR for both the TCR-alpha (TCRα) and TCR-beta (TCRβ) chains, and new TCRdist and grouping of lymphocyte interactions by paratope hotspots (GLIPH) algorithms to compare TCRs directed against the most prominent human influenza epitope, HLA-A*02:01-M1 (A2M1). We dissected memory TCR repertoires directed toward A2M1 CD8 T cells within human tissues and compared them to human peripheral blood of young and elderly adults. Furthermore, we compared these memory CD8 T cell repertoires to A2M1 CD8 TCRs during acute influenza disease in patients hospitalized with avian A/H7N9 virus. Our study provides the first comparative analysis of paired antigen-specific TCR-α/β clonotypes across different tissues and peripheral blood across different age groups. We show that human A2M1 CD8 T cells can be readily detected in human lungs, spleens, and lymph nodes, and that tissue A2M1 TCRαβ repertoires reflect A2M1 TCRαβ clonotypes derived from peripheral blood in healthy adults and influenza-infected patients. A2M1 TCRαβ repertoires displayed distinct features only in elderly adults, with large private TCRαβ clonotypes replacing the prominent and public TRBV19/TRAV27 TCRs. Our study provides novel findings on influenza-specific TCRαβ repertoires within human tissues, raises the question of how we can prevent the loss of optimal TCRαβ signatures with aging, and provides important insights into the rational design of T cell-mediated vaccines and immunotherapies.
识别源自保守的病毒内部蛋白的抗原肽的CD8 T细胞可对不同的流感病毒提供广泛的保护。由于记忆性CD8 T细胞在人的一生中以及跨组织区室都会发生变化,我们研究了T细胞受体(TCR)的组成和多样性如何与人类生命不同解剖部位和免疫阶段的记忆性CD8 T细胞相关。我们使用肽-HLA四聚体磁珠富集、针对TCR-α(TCRα)和TCR-β(TCRβ)链的单细胞多重逆转录PCR,以及新的TCRdist和通过互补位热点对淋巴细胞相互作用进行分组(GLIPH)算法,来比较针对最突出的人类流感表位HLA-A*02:01-M1(A2M1)的TCR。我们剖析了人类组织中针对A2M1 CD8 T细胞的记忆性TCR库,并将它们与年轻人和老年人的外周血进行比较。此外,我们还将这些记忆性CD8 T细胞库与感染甲型H7N9禽流感病毒住院患者急性流感疾病期间的A2M1 CD8 TCR进行了比较。我们的研究首次对不同组织和不同年龄组外周血中配对的抗原特异性TCR-α/β克隆型进行了比较分析。我们发现,在人类肺、脾和淋巴结中可以很容易地检测到人类A2M1 CD8 T细胞,并且组织中的A2M1 TCRαβ库反映了健康成年人和流感感染患者外周血中的A2M1 TCRαβ克隆型。A2M1 TCRαβ库仅在老年人中表现出不同特征,大量独特的TCRαβ克隆型取代了突出的公共TRBV19/TRAV27 TCR。我们的研究提供了关于人类组织中流感特异性TCRαβ库的新发现,提出了如何预防随着年龄增长而导致最佳TCRαβ特征丧失的问题,并为T细胞介导的疫苗和免疫疗法的合理设计提供了重要见解。
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