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树突状细胞成熟以增强抗HIV-1 CD8(+) T细胞免疫的激活

Maturation of dendritic cells for enhanced activation of anti-HIV-1 CD8(+) T cell immunity.

作者信息

Huang Xiao-Li, Fan Zheng, Borowski LuAnn, Rinaldo Charles R

机构信息

Graduate School of Public Health and School of Medicine, University of Pittsburgh, Pittsburgh, PA 15261, USA.

出版信息

J Leukoc Biol. 2008 Jun;83(6):1530-40. doi: 10.1189/jlb.1107795. Epub 2008 Mar 25.

DOI:10.1189/jlb.1107795
PMID:18364435
Abstract

Maturation of dendritic cells (DC) to enhance their capacity to activate T cell immunity to HIV-1 is a key step in immunotherapy of HIV-1 infection with DC. We compared maturation of DC derived from HIV-1-uninfected subjects and infected subjects on antiretroviral therapy (ART) or ART naïve by CD40 ligand (CD40L) and combinations of TLR3 ligand polyinosinic:polycytidylic acid [poly(I:C)] and inflammatory cytokines IFN-gamma, IFN-alpha, IL-1beta, and TNF-alpha. The greatest levels of virus-specific IFN-gamma production by CD8(+) T cells were stimulated by DC treated with CD40L, followed by DC treated with the poly(I:C)-cytokine combination. The highest levels of IL-12p70 were produced by DC treated with CD40L + IFN-gamma, followed by CD40L and the poly(I:C)-cytokine combination. Neutralization of IL-12p70 indicated that it was only partially involved in direct enhancement of antiviral CD8(+) T cell activity. DC stimulation of antiviral CD8(+) T cell reactivity was enhanced by activated CD4(+) T cells at low concentrations but was suppressed at higher CD4(+) T cell concentrations. Maturation of DC with CD40L obviated the need for CD4(+) T cell help and overcame this suppressive activity. Finally, we showed that DC from HIV-1-infected subjects on ART, which were treated with the poly(I:C)-cytokine combination, retained the capacity to produce IL-12p70 and activate anti-HIV-1 CD8(+) T cell responses after restimulation with CD40L, with or without IFN-gamma. Thus, DC from HIV-1-infected subjects can be engineered with CD40L or a poly(I:C)-cytokine combination for enhancing CD8(+) T cell responses to HIV-1, which has potential applications in HIV-1 immunotherapy.

摘要

使树突状细胞(DC)成熟以增强其激活针对HIV-1的T细胞免疫的能力,是采用DC进行HIV-1感染免疫治疗的关键步骤。我们比较了来自未感染HIV-1的受试者以及接受抗逆转录病毒治疗(ART)或未接受ART的感染受试者的DC,通过CD40配体(CD40L)以及Toll样受体3配体聚肌苷酸:聚胞苷酸[聚(I:C)]与炎性细胞因子IFN-γ、IFN-α、IL-1β和TNF-α的组合来实现成熟。CD8(+) T细胞产生的病毒特异性IFN-γ的最高水平是由用CD40L处理的DC刺激产生的,其次是用聚(I:C)-细胞因子组合处理的DC。IL-12p70的最高水平是由用CD40L + IFN-γ处理的DC产生的,其次是CD40L和聚(I:C)-细胞因子组合。对IL-12p70的中和表明它仅部分参与直接增强抗病毒CD8(+) T细胞活性。低浓度活化的CD4(+) T细胞可增强DC对抗病毒CD8(+) T细胞反应性的刺激,但在较高的CD4(+) T细胞浓度下则受到抑制。用CD40L使DC成熟消除了对CD4(+) T细胞辅助的需求并克服了这种抑制活性。最后,我们表明,接受ART的HIV-1感染受试者的DC,在用聚(I:C)-细胞因子组合处理后,在用CD40L再刺激(无论有无IFN-γ)后仍保留产生IL-12p70和激活抗HIV-1 CD8(+) T细胞反应的能力。因此,HIV-1感染受试者的DC可用CD40L或聚(I:C)-细胞因子组合进行改造,以增强CD8(+) T细胞对HIV-1的反应,这在HIV-1免疫治疗中具有潜在应用价值。

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