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对选定HIV表位的IL-15依赖性CD8 T细胞反应与早期接受治疗的HIV感染受试者的病毒控制有关。

An IL-15 dependent CD8 T cell response to selected HIV epitopes is related to viral control in early-treated HIV-infected subjects.

作者信息

D'Offizi G, Gioia C, Corpolongo A, Martini F, Paganelli R, Volpi I, Sacchi A, Tozzi V, Narciso P, Poccia F

机构信息

National Institute for Infectious Diseases, Lazzaro Spallanzani - I.R.C.C.S., Rome, Italy.

出版信息

Int J Immunopathol Pharmacol. 2007 Jul-Sep;20(3):473-85. doi: 10.1177/039463200702000306.

DOI:10.1177/039463200702000306
PMID:17880761
Abstract

In some early-treated HIV-positive patients, Structured Treatment Interruption (STI) is associated to spontaneous control of viral rebound. Thus, in this clinical setting, we analyzed the immunological parameters associated to viral control. Two groups of early treated patients who underwent STI were retrospectively defined, according to the ability to spontaneously control HIV replication (Controller and Non-controller). Plasma cytokine levels were analyzed by multiplex analysis. CD8 T cell differentiation was determined by polychromatic flow cytometry. Antigen-specific IFN-gamma production was analyzed by ELISpot and intracellular staining after stimulation with HIV-peptides. Long-term Elispot assays were performed in the presence or absence of IL-15. Plasma IL-15 was found decreased over a period of time in Non-Controller patients, whereas a restricted response to Gag (aa.167-202 and 265-279) and Nef (aa.86-100 and 111-138) immunodominant epitopes was more frequently observed in Controller patients. Interestingly, in two Non-Controller patients the CD8-mediated T cells response to immunodominant epitopes could be restored in vitro by IL-15, suggesting a major role of cytokine homeostasis on the generation of protective immunity. In early-treated HIV+ patients undergoing STI, HIV replication control was associated to CD8 T cell maturation and sustained IL-15 levels, leading to HIV-specific CD8 T cell responses against selected Gag and Nef epitopes.

摘要

在一些早期接受治疗的HIV阳性患者中,结构化治疗中断(STI)与病毒反弹的自发控制相关。因此,在这种临床情况下,我们分析了与病毒控制相关的免疫参数。根据自发控制HIV复制的能力(控制者和非控制者),对两组接受STI的早期治疗患者进行了回顾性定义。通过多重分析检测血浆细胞因子水平。通过多色流式细胞术测定CD8 T细胞分化。在用HIV肽刺激后,通过ELISpot和细胞内染色分析抗原特异性IFN-γ的产生。在有或没有IL-15的情况下进行长期ELISpot检测。发现非控制者患者血浆IL-15在一段时间内下降,而在控制者患者中更频繁地观察到对Gag(aa.167 - 202和265 - 279)和Nef(aa.86 - 100和111 - 138)免疫显性表位的受限反应。有趣的是,在两名非控制者患者中,IL-15可在体外恢复CD8介导的T细胞对免疫显性表位的反应,提示细胞因子稳态在保护性免疫产生中起主要作用。在接受STI的早期治疗的HIV +患者中,HIV复制控制与CD8 T细胞成熟和持续的IL-15水平相关,导致针对选定的Gag和Nef表位的HIV特异性CD8 T细胞反应。

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