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首页> 外文期刊>The journal of immunology >Characterization of High-Avidity Cytomegalovirus-Specific T Cells with Differential Tetramer Binding Coappearing after Allogeneic Stem Cell Transplantation
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Characterization of High-Avidity Cytomegalovirus-Specific T Cells with Differential Tetramer Binding Coappearing after Allogeneic Stem Cell Transplantation

机译:同种异体干细胞移植后,高抗原性巨细胞病毒特异的T细胞与差异四聚体结合的表征。

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CMV reactivation is a major complication after allogeneic stem cell transplantation (SCT). Immune reconstitution of CMV-specific CTLs (CMV-CTLs) is essential for virus control. During CMV-CTL monitoring using mutated HLA/CMV tetramers selectively detecting high-avidity T cells, we observed coappearance of CMV-CTLs with low (CMV tetlow CTLs) and high tetramer binding (CMV tethigh CTLs) in 53/115 CMV IgG+ patients stem cell transplanted from CMV IgG+ donors. However, the relevance of these coappearing differentially tetramer binding (“dual”) CMV-CTLs was unclear. In this study, we investigated the kinetics, properties, and clinical impact of coappearing CMV tetlow and tethigh CTLs after allogeneic SCT. Patients with dual CMV-CTLs had more CMV tethigh than tetlow CTLs. Chimerism analysis of isolated CMV tetlow and tethigh CTLs revealed their exclusive donor origin. CMV tetlow and tethigh CTLs had an identical effector memory CD45RA?CCR7? and CD45RA+CCR7? T cell distribution, equal differentiation, senescence, and exhaustion marker expression and were negative for regulatory CD8+ T cell markers. Isolated CMV tetlow and tethigh CTLs were equally sensitive to CMV peptides in IFN-γ release and cytotoxicity assays. However, CMV tethigh CTLs proliferated more in response to low CMV peptide concentrations than tetlow CTLs. TCR repertoire analysis revealed that CMV tetlow and tethigh CTLs use different TCRs. Finally, dual CMV-CTLs were not associated with CMV antigenemia. In conclusion, these data show for the first time, to our knowledge, that both CMV tetlow and tethigh CTLs are functional effector T cells differing by proliferation, numbers in peripheral blood, and probably by their precursors without increasing the CMV reactivation risk after allogeneic SCT.
机译:同种异体干细胞移植(SCT)后,CMV重新激活是主要并发症。 CMV特定CTL(CMV-CTL)的免疫重建对于控制病毒至关重要。在使用突变HLA / CMV四聚体选择性检测高存活率T细胞的CMV-CTL监测过程中,我们观察到53/115 CMV IgG +患者茎中具有低(CMV tetlow CTL)和高四聚体结合(CMV tethigh CTL)的CMV-CTL共同出现CMV IgG +供体移植的细胞。但是,这些共同出现的差异四聚体结合(“双重”)CMV-CTL的相关性尚不清楚。在这项研究中,我们调查了异基因SCT后同时出现的CMV小腿和大腿CTL的动力学,特性和临床影响。双重CMV-CTL患者的tethigh CMV多于tetlow CTL。对孤立的CMV小腿和大腿CTL的嵌合分析显示出它们的独家供体来源。 CMV的Tetlow和Tethigh的CTL具有相同的效应记忆CD45RA?CCR7?。和CD45RA + CCR7? T细胞分布,均等分化,衰老和精疲力竭标志物表达,对CD8 + T细胞调节性标志物阴性。在IFN-γ释放和细胞毒性试验中,分离的CMV小腿和大腿CTL对CMV肽同样敏感。但是,对低CMV肽浓度的响应,CMV大腿高CTL的增殖要比大腿CTL高。 TCR曲目库分析显示,CMV小腿和大腿CTL使用不同的TCR。最后,双重CMV-CTL与CMV抗原血症无关。总而言之,据我们所知,这些数据首次表明,CMV tetlow和tethigh CTL都是功能性效应T细胞,它们的增殖,外周血数目以及可能由其前体不同,而不会增加同种异体SCT后的CMV活化风险。

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