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Human Peripheral Blood Mononuclear Cell Function and Dendritic Cell Differentiation Are Affected by Bisphenol-A Exposure

机译:双酚A暴露影响人外周血单核细胞功能和树突状细胞分化。

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摘要

Environmental pollutants, including endocrine disruptor chemicals (EDCs), interfere on human health, leading to hormonal, immune and metabolic perturbations. Bisphenol-A (BPA), a main component of polycarbonate plastics, has been receiving increased attention due to its worldwide distribution with a large exposure. In humans, BPA, for its estrogenic activity, may have a role in autoimmunity, inflammatory and allergic diseases. To this aim, we assessed the effect of low BPA doses on functionality of human peripheral blood mononuclear cells (PBMCs), and on in vitro differentiation of dendritic cells from monocytes (mDCs). Fresh peripheral blood samples were obtained from 12 healthy adult volunteers. PBMCs were left unstimulated or were activated with the mitogen phytohemagglutinin (PHA) or the anti-CD3 and anti-CD28 antibodies and incubated in presence or absence of BPA at 0.1 and 1nM concentrations. The immune-modulatory effect of BPA was assessed by evaluating the cell proliferation and the levels of interferon-γ (IFN-γ), interleukin-4 (IL-4), interleukin-10 (IL-10) and interleukin-13 (IL-13) secreted by PBMCs. mDCs were differentiated with IL-4 and GC-CSF with or without BPA and the expression of differentiation/maturation markers (CD11c, CD1a, CD86, HLA-DR) was evaluated by flow cytometry; furthermore, a panel of 27 different cytokines, growth factors and chemokines were assayed in the mDC culture supernatants. PBMCs proliferation significantly increased upon BPA exposure compared to BPA untreated cells. In addition, a significant decrease in IL-10 secretion was observed in PBMCs incubated with BPA, either in unstimulated or mitogen-stimulated cells, and at both 0.1 and 1nM BPA concentrations. Similarly, IL-13 was reduced, mainly in cells activated by antiCD3/CD28. By contrast, no significant changes in IFN-γ and IL-4 production were found in any condition assayed. Finally, BPA at 1nM increased the density of dendritic cells expressing CD1a and concomitantly decreased the expression of HLA-DR and CD86 activation markers. In conclusion, in humans the exposure to BPA causes on PBMCs a significant modulation of proliferative capacity and cytokine production, and on mDCs alteration in differentiation and phenotype. These immune cell alterations suggest that low dose chronic exposure to BPA could be involved in immune deregulation and possibly in the increased susceptibility to develop inflammatory and autoimmune diseases.
机译:包括内分泌干扰物(EDC)在内的环境污染物会干扰人体健康,导致荷尔蒙,免疫和代谢紊乱。聚碳酸酯塑料的主要成分双酚A(BPA)由于其在世界范围内的广泛分布和大量曝光而受到越来越多的关注。在人类中,BPA具有雌激素活性,可能在自身免疫,炎症和过敏性疾病中起作用。为此,我们评估了低BPA剂量对人外周血单个核细胞(PBMC)的功能以及树突状细胞与单核细胞(mDC)体外分化的影响。从12位健康的成年人志愿者那里获得新鲜的外周血样本。 PBMC不受刺激或被丝裂素植物血凝素(PHA)或抗CD3和抗CD28抗体激活,并在存在或不存在浓度为0.1和1nM的BPA下孵育。通过评估细胞增殖和干扰素-γ(IFN-γ),白介素-4(IL-4),白介素10(IL-10)和白介素13(IL)的水平来评估BPA的免疫调节作用。 -13)由PBMC分泌。用IL-4和GC-CSF在有或没有BPA的情况下对mDC进行分化,并通过流式细胞术评估分化/成熟标志物(CD11c,CD1a,CD86,HLA-DR)的表达;此外,在mDC培养上清液中分析了27种不同的细胞因子,生长因子和趋化因子。与未处理BPA的细胞相比,接触BPA时PBMC的增殖明显增加。此外,在未刺激或有丝分裂原刺激的细胞中,在0.1nM和1nM BPA浓度下,与BPA孵育的PBMC中观察到IL-10分泌显着减少。同样,IL-13减少,主要在被抗CD3 / CD28激活的细胞中。相比之下,在任何测定的条件下均未发现IFN-γ和IL-4产生显着变化。最后,BPA在1nM时增加了表达CD1a的树突状细胞的密度,并同时降低了HLA-DR和CD86激活标记的表达。总之,在人类中,接触BPA会导致PBMC的增殖能力和细胞因子产生显着调节,以及mDC的分化和表型改变。这些免疫细胞改变表明,低剂量长期接触BPA可能与免疫失调有关,并可能导致发炎和自身免疫疾病的易感性增加。

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