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免疫衰老的 CD57+CD4+ T 细胞在对 ART 稳定应答的 HIV 患者中积累并有助于干扰素-γ 反应。

Immunosenescent CD57+CD4+ T-cells accumulate and contribute to interferon-γ responses in HIV patients responding stably to ART.

机构信息

School of Pathology and Laboratory Medicine, University of Western Australia and PathWest Laboratory Medicine, Perth, Australia.

出版信息

Dis Markers. 2011;31(6):337-42. doi: 10.3233/DMA-2011-0847.

DOI:10.3233/DMA-2011-0847
PMID:22182806
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3826487/
Abstract

HIV-infected individuals responding to antiretroviral therapy (ART) after severe CD4+ T-cell depletion may retain low responses to recall antigens [eg: cytomegalovirus (CMV)] and altered expression of T-cell co-stimulatory molecules consistent with immunosenescence. We investigated the capacity of phenotypically senescent cells to generate cytokines in HIV patients receiving long-term ART (n = 18) and in healthy controls (n = 10). Memory T-cells were assessed by interferon (IFN)-γ ELISpot assay and flow cytometrically via IFN-γ or IL-2. Proportions of CD57(bright)CD28(null) CD4+ T-cells correlated with IFN-γ responses to CMV (p =0.009) and anti-CD3 (p =0.002) in HIV patients only. Proportions of CD57(bright)CD28(null) CD8+T-cells and CD8+ T-cell IFN-γ responses to CMV peptides correlated in controls but not HIV patients. IL-2 was predominantly produced by CD28+T-cells from all donors, whereas IFN-γ was mostly produced by CD57+ T-cells. The findings provide evidence of an accumulation of immunosenescent T-cells able to make IFN-γ. This may influence the pathogenesis of secondary viral infections in HIV patients receiving ART.

摘要

接受抗逆转录病毒治疗(ART)后严重 CD4+T 细胞耗竭的 HIV 感染者可能对回忆抗原(如巨细胞病毒(CMV))保持低反应,并表现出 T 细胞共刺激分子表达改变,这与免疫衰老一致。我们研究了长期接受 ART(n=18)的 HIV 患者和健康对照者(n=10)中表型衰老细胞产生细胞因子的能力。通过干扰素(IFN)-γ ELISpot 测定和通过 IFN-γ 或 IL-2 的流式细胞术评估记忆 T 细胞。CD57(bright)CD28(null)CD4+T 细胞的比例与 HIV 患者中 CMV(p=0.009)和抗-CD3(p=0.002)的 IFN-γ 反应相关,但与 HIV 患者无关。CD57(bright)CD28(null)CD8+T 细胞的比例和 CD8+T 细胞对 CMV 肽的 IFN-γ 反应在对照组中相关,但在 HIV 患者中不相关。IL-2 主要由所有供体的 CD28+T 细胞产生,而 IFN-γ 主要由 CD57+T 细胞产生。这些发现提供了证据,证明有免疫衰老 T 细胞的积累,能够产生 IFN-γ。这可能会影响接受 ART 的 HIV 患者继发病毒感染的发病机制。