HIV-1感染中的淋巴细胞活化。II. CD28阴性T细胞的功能缺陷。

Lymphocyte activation in HIV-1 infection. II. Functional defects of CD28- T cells.

作者信息

Borthwick N J, Bofill M, Gombert W M, Akbar A N, Medina E, Sagawa K, Lipman M C, Johnson M A, Janossy G

机构信息

Department of Clinical Immunology, Royal Free Hospital and School of Medicine, London, UK.

出版信息

AIDS. 1994 Apr;8(4):431-41. doi: 10.1097/00002030-199404000-00004.

DOI:10.1097/00002030-199404000-00004

PMID:8011246

Abstract

OBJECTIVES AND DESIGN

The expression of the accessory molecule CD28 was compared in various populations of T and natural killer (NK) cells from HIV-1-negative and HIV-1-positive individuals and correlated with activation using mitogens in vitro.

METHODS

Multiparameter flow cytometric analysis using combinations of CD3 CD28 and other markers was performed together with absolute cell counting in peripheral blood. Blast transformation and proliferative responses were also quantitated using the Cytoronabsolute after stimulation with phytohaemagglutinin (PHA) and anti-CD3. CD28- cells were also purified to confirm the observations.

RESULTS

In HIV-1-negative individuals > 90% of CD3+ T cells were CD28+ and responded to stimulation, while CD3- CD16+ CD57+ NK-like cells were CD28- and failed to respond. In HIV-1-positive individuals the expression of CD28 was greatly reduced and the proportion of CD3+CD28- T cells expanded. CD8 lymphocytosis was caused entirely by the accumulation of CD28- T cells and many of these expressed activation markers human lymphocyte antigen-DR, CD38 and CD45RO on their membrane and molecules such as TIA-1 and perforin, associated with cytolytic function, in their cytoplasm. The strong positive correlation (r = 0.66) between the lack of CD28 expression and the poor proliferation from HIV-1-positive individuals was confirmed by demonstrating that only CD28+ cells transformed into lymphoblasts and proliferated. Although the CD28- including CD3+ T cells transiently expressed CD25 (interleukin-2R alpha), they did not undergo blastogenesis or activation measured by bromodeoxyuridine uptake and died after 3-4 days in culture. These observations were confirmed in costimulation experiments with anti-CD2 and anti-CD28.

CONCLUSION

In HIV-1 infection activated CD3+CD28- T cells accumulate but are unresponsive to mitogens and anti-CD28. These cells appear to represent terminally differentiated effector cells which fail to respond to further stimuli because of the absence of a CD28 second signal.

摘要

目的与设计

比较了来自HIV - 1阴性和HIV - 1阳性个体的不同T细胞群和自然杀伤（NK）细胞中辅助分子CD28的表达情况，并将其与体外使用丝裂原激活的情况相关联。

方法

使用CD3、CD28和其他标志物组合进行多参数流式细胞术分析，并对外周血中的细胞进行绝对计数。在用植物血凝素（PHA）和抗CD3刺激后，还使用Cytoronabsolute对母细胞转化和增殖反应进行定量。还对CD28阴性细胞进行了纯化以证实观察结果。

结果

在HIV - 1阴性个体中，>90%的CD3 + T细胞为CD28 + ，并对刺激有反应，而CD3 - CD16 + CD57 + NK样细胞为CD28 - ，且无反应。在HIV - 1阳性个体中，CD28的表达大大降低，CD3 + CD28 - T细胞的比例增加。CD8淋巴细胞增多完全是由CD28 - T细胞的积累引起的，其中许多细胞在其细胞膜上表达激活标志物人类淋巴细胞抗原 - DR、CD38和CD45RO，在其细胞质中表达与细胞溶解功能相关的分子如TIA - 1和穿孔素。通过证明只有CD28 + 细胞转化为成淋巴细胞并增殖，证实了HIV - 1阳性个体中CD28表达缺失与增殖不良之间的强正相关（r = 0.66）。尽管包括CD3 + T细胞在内的CD28 - 细胞短暂表达CD25（白细胞介素 - 2Rα），但它们未经历母细胞形成或通过溴脱氧尿苷摄取测量的激活，并且在培养3 - 4天后死亡。这些观察结果在抗CD2和抗CD28的共刺激实验中得到证实。