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CD8+ T细胞上C1.7抗原的表达依赖于激活:在疾病进展的HIV-1感染患者中,C1.7+CD8+ T细胞的比例增加。

C1.7 antigen expression on CD8+ T cells is activation dependent: increased proportion of C1.7+CD8+ T cells in HIV-1-infected patients with progressing disease.

作者信息

Peritt D, Sesok-Pizzini D A, Schretzenmair R, Macgregor R R, Valiante N M, Tu X, Trinchieri G, Kamoun M

机构信息

The Wistar Institute, Philadelphia, PA 19104, USA.

出版信息

J Immunol. 1999 Jun 15;162(12):7563-8.

PMID:10358213
Abstract

The C1.7 Ag is a surface marker previously shown to be expressed on all NK cells and on a subset of CD8+ T cells. We report in this study that C1.7 Ag expression on peripheral blood-derived CD8+ T cells overlaps with activation markers S6F1high and CD29high and is reciprocally expressed with CD62L. C1.7 Ag expression can be induced in vitro on CD8+ T cells by anti-CD3 cross-linking, suggesting that C1.7 Ag is activation dependent. In contrast to NK cells, C1.7 Ag does not signal on CD8+ T cells, nor does it induce redirected lysis upon ligation. The proportion of C1.7 Ag+CD8+ T cells is increased in HIV-infected patients compared with healthy donors. In 69 HIV-infected patients, we observed a significant inverse correlation between the percentage of C1.7 Ag-expressing CD8+ T cells and the absolute CD4+ T cell count. Two-year clinical follow-up of patients with initial CD4+ T cell count of >400 cells/mm3 and a normal proportion of C1.7 Ag+CD8+ T cells revealed that these patients were clinically stable with minimal HIV-associated symptoms. In contrast, 10 of 12 patients with CD4+ T cell counts of >400 cells/mm3 and an elevated proportion of C1.7 Ag+CD8+ T cells were symptomatic. ANOVA analysis of patients indicates that C1.7 Ag is a better predictor of disease progression than CD4 count. Overall, our findings indicate that C1.7 Ag is the first described marker for activated/memory CD8+ T cells and a useful parameter for evaluating the level of CD8+ T cell activation in vivo.

摘要

C1.7抗原是一种表面标志物,先前已证明其在所有自然杀伤(NK)细胞和一部分CD8⁺T细胞上表达。我们在本研究中报告,外周血来源的CD8⁺T细胞上的C1.7抗原表达与激活标志物S6F1高表达和CD29高表达重叠,且与CD62L呈反向表达。通过抗CD3交联可在体外诱导CD8⁺T细胞表达C1.7抗原,这表明C1.7抗原的表达依赖于激活。与NK细胞不同,C1.7抗原在CD8⁺T细胞上不产生信号,也不会在连接时诱导重定向裂解。与健康供体相比,HIV感染患者中C1.7抗原⁺CD8⁺T细胞的比例增加。在69例HIV感染患者中,我们观察到表达C1.7抗原的CD8⁺T细胞百分比与CD4⁺T细胞绝对计数之间存在显著的负相关。对初始CD4⁺T细胞计数>400个细胞/mm³且C1.7抗原⁺CD8⁺T细胞比例正常的患者进行的两年临床随访显示,这些患者临床稳定,HIV相关症状极少。相比之下,12例CD4⁺T细胞计数>400个细胞/mm³且C1.7抗原⁺CD8⁺T细胞比例升高的患者中有10例出现症状。对患者的方差分析表明,C1.7抗原比CD4计数更能预测疾病进展。总体而言,我们的研究结果表明,C1.7抗原是首个被描述的活化/记忆性CD8⁺T细胞标志物,也是评估体内CD8⁺T细胞激活水平的有用参数。

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