首页> 外文期刊>Free Radical Biology and Medicine: The Official Journal of the Oxygen Society >Modulatory effects of low-dose hydrogen peroxide on the function of human plasmacytoid dendritic cells
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Modulatory effects of low-dose hydrogen peroxide on the function of human plasmacytoid dendritic cells

机译:小剂量过氧化氢对人浆细胞样树突状细胞功能的调节作用

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Under normal conditions, plasmacytoid dendritic cells (pDCs) are located in peripheral lymphoid organs or circulate in the blood, from where they can migrate to sites of infection or inflammation. In inflamed tissues, pDCs can be exposed to elevated levels of reactive oxygen species produced by inflammatory cells and we presume that oxidative stress could affect the cellular responses of pDCs to microenvironmental stimuli. To explore this possibility, human pDCs isolated from peripheral blood of healthy donors were treated with H 2O 2 and R837 (a Toll-like receptor 7 ligand), separately and in combination. Our results demonstrate that treatment with a low concentration (0.01 μM) of H 2O 2 resulted in only slight changes in the expression of CD40, CD80, CD86, and CD83; however, low-dose H 2O 2 markedly decreased the expression of HLA-DQ on pDCs. Exposure to H 2O 2 did not trigger the release of IL-6, TNF-α, IL-8, or IFN-α from pDCs. Although addition of H 2O 2 did not modify the capacity of pDCs to activate allogeneic IL-17- or IFN-γ-producing T cells, it significantly increased the ability of pDCs to stimulate IL-4-secreting T cells. Exposure of pDCs to H 2O 2 before cocultivation with na?ve autologous T cells significantly lowered IL-10 production by T cells, but did not affect IL-17 release. It was also observed that H 2O 2-exposed pDCs provided stronger stimuli for Th2 than for Th1 differentiation upon autologous activation, compared to untreated pDCs, possibly because of elevated surface expression of OX40-L. Most importantly, when pDCs were stimulated with R837 in the presence of H 2O 2, decreased phenotypic activation, decreased chemokine and cytokine release, and impaired allo- and autostimulatory functions of pDCs were detected, indicating that pDCs exposed to oxidative stress in vivo may have an anti-inflammatory or tolerogenic role in regulating adaptive immune responses.
机译:在正常情况下,浆细胞样树突状细胞(pDC)位于外周淋巴器官或在血液中循环,从那里它们可以迁移到感染或炎症部位。在发炎的组织中,pDC可能会暴露于炎性细胞产生的活性氧水平升高,我们推测氧化应激可能会影响pDC对微环境刺激的细胞反应。为了探索这种可能性,分别将从H2O 2和R837(Toll样受体7配体)中分离出健康供体外周血中分离出的人pDC。我们的结果表明,用低浓度(0.01μM)的H 2O 2处理只会使CD40,CD80,CD86和CD83的表达发生轻微变化;然而,低剂量的H 2O 2明显降低了pDC上HLA-DQ的表达。暴露于H 2O 2不会触发pDC释放IL-6,TNF-α,IL-8或IFN-α。尽管加入H 2O 2不会改变pDC激活同种异体产生IL-17或IFN-γ的T细胞的能力,但它显着提高了pDC刺激分泌IL-4的T细胞的能力。与未经处理的自体T细胞共培养之前,将pDC暴露于H 2O 2会显着降低T细胞产生IL-10的程度,但不会影响IL-17的释放。还观察到,与未经处理的pDC相比,自体激活后,暴露于H 2O 2的pDC对Th2的刺激要强于Th1的分化,这可能是由于OX40-L的表面表达升高。最重要的是,当在H 2O 2存在下用R837刺激pDC时,检测到pDC的表型活化降低,趋化因子和细胞因子释放降低,以及同种异体和自刺激功能受损,表明在体内暴露于氧化应激的pDC可能在调节适应性免疫反应中具有抗炎或抗致癌作用。

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