在单细胞水平上检测到特应性疾病患者中产生干扰素-γ和白细胞介素-2的细胞频率降低。
Decreased frequency of interferon-gamma- and interleukin-2-producing cells in patients with atopic diseases measured at the single cell level.
作者信息
Jung T, Lack G, Schauer U, Uberück W, Renz H, Gelfand E W, Rieger C H
机构信息
Department of Dermatology, University of Göttingen, Germany.
出版信息
J Allergy Clin Immunol. 1995 Oct;96(4):515-27. doi: 10.1016/s0091-6749(95)70296-2.
BACKGROUND
Recently, diminished interferon-gamma (IFN-gamma) and increased interleukin (IL-4 production in peripheral blood mononuclear cells (PBMCs) from atopic patients have been described by several groups, measured as total cytokine content in culture supernatants. These studies suggested a predominance of TH2-like cells producing large amounts of IL-4 in atopic patients. It is not clear whether the reported cytokine imbalances are the result of an alteration in the distribution of specific T-cell subsets or whether intrinsic dysregulation in cytokine production is a characteristic of atopic individuals.
OBJECTIVE
This study examined the production of IFN-gamma, and IL-2 in PBMCs from atopic patients at the single cell level with the use of freshly isolated lymphocytes.
METHODS
We recently described a flow cytometric assay in which three-color analysis was used to study the production of a cytokine of interest in a T-cell subpopulation defined by two cell surface markers. PBMCs from 23 atopic patients and 14 control subjects were stimulated with phorbol ester and ionomycin for 5 hours. PBMCs from seven patients and seven control subjects were also cultured with immobilized anti-CD3 antibodies for 24 hours. Cells were fixed, made permeable, and stained for intracellular cytokines in combination with cell surface markers CD3, CD8, and CD45RO. Cytokine-producing cells were analyzed by gating on T-cell subsets.
RESULTS
IFN-gamma-producing cells were significantly decreased (p < 0.05) in CD4+ T cells but not in CD8+ T cells of atopic patients. CD45R0+ and CD45R0-T cells showed a decreased proportion of IFN-gamma-producing cells (p < 0.05 and p < 0.01, respectively). IL-2 production was diminished in all T-cell subsets (p < 0.01). The number of IL-4-producing cells was not elevated, and such cells were exclusively found in the CD45RO+ T cells. Analysis of culture supernatants of sorted CD45RO+ T cells for IL-4 and IFN-gamma production confirmed these results.
CONCLUSION
Our findings provide evidence that a reduced IFN-gamma production in atopic patients is due to an intrinsic defect selectively found in the CD4+ T cells. Because IL-2 production was markedly decreased but IL-4 production was unchanged, our data demonstrate a deficiency in the ability of atopic T cells to produce TH1-like cytokines on stimulation with phorbol ester, ionomycin, or anti-CD3 monoclonal antibodies.
背景
最近,几个研究小组报道了特应性患者外周血单个核细胞(PBMC)中干扰素-γ(IFN-γ)减少,白细胞介素(IL-4)产生增加,以培养上清液中的细胞因子总含量来衡量。这些研究提示特应性患者中产生大量IL-4的TH2样细胞占优势。尚不清楚所报道的细胞因子失衡是特定T细胞亚群分布改变的结果,还是细胞因子产生的内在失调是特应性个体的一个特征。
目的
本研究采用新鲜分离的淋巴细胞,在单细胞水平检测特应性患者PBMC中IFN-γ和IL-2的产生情况。
方法
我们最近描述了一种流式细胞术检测方法,其中利用三色分析来研究由两种细胞表面标志物定义的T细胞亚群中一种感兴趣的细胞因子的产生情况。用佛波酯和离子霉素刺激23例特应性患者和14例对照受试者的PBMC 5小时。7例患者和7例对照受试者的PBMC还用固定化抗CD3抗体培养24小时。细胞固定、通透处理后,结合细胞表面标志物CD3、CD8和CD45RO对细胞内细胞因子进行染色。通过门控T细胞亚群分析产生细胞因子的细胞。
结果
特应性患者的CD4⁺T细胞中产生IFN-γ的细胞显著减少(p<0.05),而CD8⁺T细胞中未减少。CD45R0⁺和CD45R0⁻T细胞中产生IFN-γ的细胞比例均降低(分别为p<0.05和p<0.01)。所有T细胞亚群中IL-2的产生均减少(p<0.01)。产生IL-4的细胞数量未增加,且此类细胞仅在CD45RO⁺T细胞中发现。对分选的CD45RO⁺T细胞培养上清液中IL-4和IFN-γ产生情况的分析证实了这些结果。
结论
我们的研究结果提供了证据,表明特应性患者中IFN-γ产生减少是由于在CD4⁺T细胞中选择性发现的内在缺陷。由于IL-2产生明显减少而IL-4产生未改变,我们的数据表明特应性T细胞在用佛波酯、离子霉素或抗CD3单克隆抗体刺激时产生TH1样细胞因子的能力存在缺陷。
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