首页> 外文期刊>Clinical and experimental allergy : >Inhibition of human allergic T-helper type 2 immune responses by induced regulatory T cells requires the combination of interleukin-10-treated dendritic cells and transforming growth factor-beta for their induction.
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Inhibition of human allergic T-helper type 2 immune responses by induced regulatory T cells requires the combination of interleukin-10-treated dendritic cells and transforming growth factor-beta for their induction.

机译:通过诱导的调节性T细胞抑制人类2型过敏性T辅助免疫应答需要白介素10处理的树突状细胞和转化生长因子β的组合。

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BACKGROUND: In grass pollen-allergic individuals, T cell anergy can be induced by IL-10-treated dendritic cells (IL-10-DC) resulting in the suppression of T helper type 1 (Th1) as well as Th2 cells. This study was performed to analyse whether such IL-10-DC-treated T cells are able to act as regulatory T cells (Treg) suppressing the function of other T cells in the periphery. As transforming growth factor (TGF)-beta is also a potential inducer of Treg, we additionally analysed the inhibitory capacity of TGF-beta-treated T cells in this system. MATERIALS AND METHODS: Freshly isolated CD4+ or CD4+ CD25- T cells from grass pollen-allergic donors were stimulated with autologous mature monocyte-derived allergen-pulsed DC in the presence or absence of T cells previously cultured with IL-10-DC- and/or TGF-beta. RESULTS: Anergic T cells induced by allergen-pulsed IL-10-treated DC or allergen-pulsed DC and TGF-beta enhanced IL-10 production and strongly inhibited IFN-gamma production of freshly prepared peripheral CD4+ or CD4+ CD25- T cells while proliferation and Th2 cytokine production were only slightly reduced. The combination of allergen-pulsed IL-10-treated DC and TGF-beta had an additional effect leading to a significant suppression also of Th2 cytokine production and proliferation. Suppression was not antigen-specific and was mainly mediated by cell-to-cell contact and by the molecule-programmed death-1 and only partially by CTLA-4, TGF-beta and IL-10. CONCLUSION: These data demonstrate that regulatory T cells that also suppress Th2 cytokine production are induced by two signals: TGF-beta and IL-10-DC. This is of importance for the regulation of allergic immune responses and might be exploited for future therapeutic strategies for allergic diseases.
机译:背景:在对花粉过敏的个体中,IL-10处理的树突状细胞(IL-10-DC)可以诱导T细胞无反应性,从而抑制1型T辅助细胞(Th1)和Th2细胞。进行该研究以分析这种经IL-10-DC处理的T细胞是否能够充当调节性T细胞(Treg),从而抑制周围其他T细胞的功能。由于转化生长因子(TGF)-β也是Treg的潜在诱导剂,因此我们另外分析了TGF-β处理的T细胞在该系统中的抑制能力。材料与方法:在存在或不存在先前用IL-10-DC-和/或培养的T细胞的情况下,用自体成熟的单核细胞衍生的变应原刺激的DC刺激从草花粉过敏性供体新鲜分离的CD4 +或CD4 + CD25- T细胞。或TGF-beta。结果:过敏原脉冲的IL-10处理的DC或过敏原脉冲的DC和TGF-β诱导的无能T细胞增强了IL-10的产生,并强烈抑制了新鲜制备的外周CD4 +或CD4 + CD25-T细胞增殖时的IFN-γ产生。 Th2细胞因子的产生仅略有减少。过敏原脉冲处理的IL-10-DC和TGF-β的组合具有额外的作用,导致Th2细胞因子的产生和增殖也受到显着抑制。抑制不是抗原特异性的,主要是通过细胞间接触和分子编程的death-1介导的,仅部分通过CTLA-4,TGF-beta和IL-10介导。结论:这些数据表明,还抑制Th2细胞因子产生的调节性T细胞由两种信号诱导:TGF-β和IL-10-DC。这对于调节过敏性免疫应答非常重要,并可能被用于未来过敏性疾病的治疗策略。

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