二氧化硅和PM1648在体外修饰人肺泡巨噬细胞抗原提呈细胞活性。

R. Hamilton, J. Pfau, G. Marshall, A. Holian
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引用次数: 18

摘要

已知一些吸入颗粒会导致炎症和肺部病变,而其他颗粒似乎没有长期影响。解释这些差异的潜在机制才刚刚开始被理解。在本文中,我们研究了二氧化硅和PM1648(一种模型城市颗粒物)是否会导致人类肺泡巨噬细胞(HAM)表型(RFD1+/7+)的选择性缺失,以及这是否会影响自体T淋巴细胞抗原呈递细胞(APC)试验中细胞因子的产生。将HAM暴露于生物活性颗粒、二氧化硅和PM1648中24小时,然后分离细胞外颗粒和无活细胞;然后用自体淋巴细胞培养HAM,进行11天的APC实验。二氧化硅暴露上调TH1淋巴细胞来源的细胞因子干扰素γ (ifn - γ)和TH2淋巴细胞来源的细胞因子白细胞介素-4 (IL-4)。PM1648暴露主要上调IL-4。两种颗粒暴露对白细胞介素-10 (IL-10)的产生均无显著影响。与二氧化钛(TiO2)和硅灰石(Woll)的控制颗粒暴露不会改变APC活性。二氧化硅和PM1648对抑制巨噬细胞表现出选择性毒性(RFD1+/7+)。我们认为,由于抑制型巨噬细胞表型失能,激活型巨噬细胞(RFD1+/7-)不受抑制型巨噬细胞的影响,通过增加淋巴细胞源性促炎细胞因子的产生来增强APC活性。
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Silica and PM1648 modify human alveolar macrophage antigen-presenting cell activity in vitro.
Some inhaled particles are known to lead to inflammation and lung pathology, whereas others do not appear to have long-term effects. Potential mechanisms to account for these differences are only beginning to be understood. In this article we examine whether silica and PM1648 (a model urban particulate) caused selective deletion of the suppressor human alveolar macrophage (HAM) phenotype (RFD1+/7+), and whether this affected cytokine production in an antigen-presenting cell (APC) assay with autologous T lymphocytes. HAM were exposed to the bioactive particulates, silica and PM1648, for 24 hours, then isolated free of extracellular particulates and nonviable cells; HAM were then cultured with autologous lymphocytes in an 11-day APC assay. Silica exposure up-regulated a TH1 lymphocyte-derived cytokine, interferon gamma (IFN-gamma), and a TH2 lymphocyte-derived cytokine, interleukin-4 (IL-4). PM1648 exposure primarily upregulated IL-4. Neither particle exposure had a significant effect on interleukin-10 (IL-10) production. Control particulate exposures with titanium dioxide (TiO2) and wollastonite (Woll) caused no altered APC activity. Silica and PM1648 demonstrated selective toxicity to suppressor macrophages (RFD1+/7+). We propose that, because of the suppressor macrophage phenotype disabling, the activator macrophage (RFD1+/7-) operates free of the suppressor macrophage's influence, enhancing APC activity with increased lymphocyte-derived proinflammatory cytokine production.
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