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Identification of HLA-E-specific alloreactive T lymphocytes: A cell subset that undergoes preferential expansion in mixed lymphocyte culture and displays a broad cytolytic activity against allogeneic cells

机译:鉴定HLA-E特异性同种异体T淋巴细胞:在混合淋巴细胞培养中经历优先扩增并显示出对同种异体细胞广泛的溶细胞活性的细胞亚群

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摘要

Previous studies showed that a subset of CD8+ cytolytic T lymphocytes expressing HLA class I-specific natural killer inhibitory receptors (iNKR) is characterized by the ability to recognize HLA-E and to mediate T cell receptor-dependent killing of different NK cell-susceptible tumor target cells. In this study, we show that this CD8+ T cell subset can also undergo extensive proliferation in mixed lymphocyte cultures in response to allogeneic cells. Analysis of their cytolytic activity revealed a broad specificity against a panel of allogeneic phytohemagglutinin-induced blasts derived from HLA-unmatched donors. On the other hand, autologous and certain allogeneic phytohemagglutinin blasts were resistant to lysis. We used as target cells the transporter associated with antigen processing (TAP)-2−/− murine RMA-S cell line cotransfected with β2-microglobulin and HLA-E*01033. On loading these cells with different HLA-E-binding peptides derived either from HLA class I leader sequences or viral proteins, we could show that HLA-E-specific cytolytic T lymphocytes recognized many, but not all, peptides analyzed. These data suggest that these cells may recognize, on allogeneic cells, HLA-E with peptides that are not present in the host of origin. In addition to their ability to proliferate in response to allogeneic stimulation and to lyse, most allogeneic cells may have important implications in transplantation and in antitumor immune responses.
机译:先前的研究表明,表达HLA I类特异性自然杀伤抑制受体(iNKR)的CD8 + 细胞溶解性T淋巴细胞的一部分具有识别HLA-E和介导T细胞受体依赖性的能力。杀死不同的NK细胞敏感性肿瘤靶细胞。在这项研究中,我们表明,这种CD8 + T细胞子集也可以在混合淋巴细胞培养物中响应同种异体细胞而广泛增殖。对它们的溶细胞活性的分析表明,它对来自HLA不匹配供体的一组同种异体植物血凝素诱导的胚芽具有广泛的特异性。另一方面,自体和某些同种异体植物血凝素胚芽细胞对裂解具有抗性。我们使用与β2-微球蛋白和HLA-E * 01033共转染的抗原处理(TAP)-2 -/-鼠RMA-S细胞系相关的转运蛋白作为靶细胞。用这些衍生自HLA I类前导序列或病毒蛋白的不同HLA-E结合肽装载这些细胞时,我们可以证明HLA-E特异性的溶细胞性T淋巴细胞可以识别许多但并非全部的肽。这些数据表明,这些细胞可以在同种异体细胞上识别HLA-E和原发宿主中不存在的肽。除了它们能够响应同种异体刺激而增生并裂解之外,大多数同种异体细胞可能在移植和抗肿瘤免疫反应中也具有重要意义。

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