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首页> 外文期刊>Clinical and Experimental Immunology: An Official Journal of the British Society for Immunology >Factors involved in the generation of memory CD8 T cells in patients with X-linked lymphoproliferative disease (XLP).
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Factors involved in the generation of memory CD8 T cells in patients with X-linked lymphoproliferative disease (XLP).

机译:X连锁淋巴增生性疾病(XLP)患者的记忆CD8 T细胞生成相关因素。

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Summary We have analysed the phenotype of T lymphocytes in two X-linked lymphoproliferative disease (XLP) patients with the same SH2D1A mutation differing in initial exposure to Epstein-Barr virus (EBV) and treatment. While memory T lymphocytes (with low CCR7 and CD62L expression) prevailed in both XLP patients, in patient 9, who developed acute infectious mononucleosis (AIM) and received B cell ablative treatment, the predominant phenotype was that of late effector CD8 T cells (CD27(-), CD28(-), CCR7(-), CD62L(-), CD45 RA(+), perforin(+)), while in patient 4 (who did not suffer AIM) the prevalent phenotype of CD8 T lymphocytes was similar to that of normal controls (N) or to that of adult individuals who recovered from AIM: CD27(+) , CD28(+), CCR7(-), CD62L(-), CD45 RO(+) and perforin(-). CD57 expression (related to senescence) was also higher in CD8 T cells from patient 9 than in patient 4, AIM or N. Persistently high EBV viral load was observed in patient 9. The results obtained from this limited number of XLP patients suggest that events related to the initial EBV encounter (antigen load, treatment, cytokine environment) may have more weight than lack of SH2D1A in determining the long-term differentiation pattern of CD8 memory T cells.
机译:总结我们已经分析了两名具有相同SH2D1A突变的X连锁淋巴组织增生性疾病(XLP)患者的T淋巴细胞表型,这些患者的初始接触爱泼斯坦-巴尔病毒(EBV)和治疗方法不同。虽然记忆X淋巴细胞(CCR7和CD62L表达低)在这两个XLP患者中都普遍存在,但在9位患者中,其发展为急性传染性单核细胞增多症(AIM),并接受了B细胞消融治疗,但主要表型是晚期效应CD8 T细胞(CD27)。 (-),CD28(-),CCR7(-),CD62L(-),CD45 RA(+),perforin(+)),而在患者4(未患有AIM的患者)中,CD8 T淋巴细胞的普遍表型为与正常对照组(N)或从AIM中恢复的成年个体相似:CD27(+),CD28(+),CCR7(-),CD62L(-),CD45 RO(+)和perforin(-) 。来自患者9的CD8 T细胞中的CD57表达(与衰老相关)也高于患者4,AIM或N中的CD57。在患者9中观察到持久的高EBV病毒载量。从数量有限的XLP患者中获得的结果表明,在确定CD8记忆T细胞的长期分化模式时,与最初的EBV遭遇(抗原负荷,治疗,细胞因子环境)相关的因素可能比缺少SH2D1A更为重要。

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