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激活抗原CD69的表达可预测来自健康供体和HIV感染患者的体外扩增外周血单个核细胞(PBMC)的功能。

Expression of the activation antigen CD69 predicts functionality of in vitro expanded peripheral blood mononuclear cells (PBMC) from healthy donors and HIV-infected patients.

作者信息

Nielsen S D, Afzelius P, Ersbøll A K, Nielsen J O, Hansen J E

机构信息

Department of Infectious Diseases, Hvidovre Hospital, Denmark.

出版信息

Clin Exp Immunol. 1998 Oct;114(1):66-72. doi: 10.1046/j.1365-2249.1998.00685.x.

Abstract

Gene therapy for AIDS necessitates harvest and expansion of PBMC from HIV-infected patients. We expanded PBMC from healthy blood donors and HIV-infected patients for up to 14 days using four expansion protocols: 3 days of phytohaemagglutinin (PHA) stimulation, continuous PHA stimulation, 3 days of stimulation with anti-CD3 and anti-CD28, and continuous stimulation with anti-CD3 and anti-CD28. Functionality of PBMC was evaluated prior to and after expansion using standard proliferation assay. Phenotype and lymphocyte subset activation defined by expression of CD69 and CD25 were determined using flow cytometry. PBMC from healthy donors and HIV-infected patients were readily expanded. The best expansion was obtained using stimulation for 3 days. After expansion, functionality of PBMC measured as proliferative response was partly conserved. PBMC expanded with stimulation for 3 days exhibited more preserved functionality than PBMC stimulated continuously (P < 0.03). The mean proliferative response in each of the four different expansion protocols correlated with the mean values of CD69 expression. The proliferative responses from patients and healthy donors expanded with PHA stimulation for 3 days correlated with CD69 expression on CD4 cells (r = 0.68, P < 0.01) and on CD8 cells (r = 0.59, P < 0.03). Furthermore, expression of CD69 reliably predicted which patients and donors had highly conserved functionality after in vitro expansion. Finally, PBMC expanded with PHA stimulation for 3 days were examined for apoptosis. Only a minor fraction was primed for apoptosis, and this fraction could be significantly reduced by addition of IL-2 to the culture medium (P < 0.05). In conclusion, the feasibility of expanding PBMC from HIV patients was demonstrated. Expanded PBMC had conserved functionality. Finally, after in vitro expansion, expression of the activation antigen CD69 reliably predicted functionality of PBMC.

摘要

艾滋病的基因治疗需要从感染HIV的患者中采集和扩增外周血单核细胞(PBMC)。我们使用四种扩增方案,将健康献血者和感染HIV患者的PBMC扩增长达14天:3天的植物血凝素(PHA)刺激、持续PHA刺激、3天的抗CD3和抗CD28刺激以及抗CD3和抗CD28的持续刺激。在扩增前后,使用标准增殖试验评估PBMC的功能。使用流式细胞术确定由CD69和CD25表达定义的表型和淋巴细胞亚群激活。健康供体和感染HIV患者的PBMC很容易扩增。使用3天刺激获得了最佳扩增效果。扩增后,以增殖反应衡量的PBMC功能部分得以保留。与持续刺激的PBMC相比,经3天刺激扩增的PBMC表现出更多保留的功能(P < 0.03)。四种不同扩增方案中每种方案的平均增殖反应与CD69表达的平均值相关。经PHA刺激3天扩增的患者和健康供体的增殖反应与CD4细胞(r = 0.68,P < 0.01)和CD8细胞(r = 0.59,P < 0.03)上的CD69表达相关。此外,CD69的表达可靠地预测了哪些患者和供体在体外扩增后具有高度保留的功能。最后,对经PHA刺激3天扩增的PBMC进行凋亡检测。只有一小部分细胞处于凋亡准备状态,并且通过向培养基中添加白细胞介素-2可以显著减少这一部分细胞(P < 0.05)。总之,证明了从HIV患者中扩增PBMC的可行性。扩增后的PBMC保留了功能。最后,在体外扩增后,激活抗原CD69的表达可靠地预测了PBMC的功能。

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