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首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Suppression of cell-mediated immune responses to listeria infection by repeated exposure to diesel exhaust particles in brown Norway rats.
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Suppression of cell-mediated immune responses to listeria infection by repeated exposure to diesel exhaust particles in brown Norway rats.

机译:反复暴露于棕色挪威大鼠的柴油机排气颗粒中,可抑制细胞介导的针对李斯特菌感染的免疫反应。

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Diesel exhaust particles (DEP) have been shown to alter pulmonary immune responses to bacterial infection. Exposure of rats to 100 mg/m(3) DEP for 4 h was found to aggravate Listeria monocytogenes(Listeria) infection at 3 days postinfection, but the bacteria were largely cleared at 7 days postinfection due to the development of a strong T cell-mediated immunity. In the present study, we examined the effects of repeated DEP exposure at lower doses on pulmonary responses to bacterial infection. Brown Norway rats were exposed to DEP by inhalation at 20.62 +/- 1.31 mg/m 3 for 4 h/day for 5 days, followed by intratracheal inoculation with 100,000 Listeria at 2 h after the last DEP exposure. DEP-exposed rats showed a significant increase in lung bacterial load at both 3 and 7 days postinfection. The repeated DEP exposure was shown to suppress both the innate, orchestrated by alveolar macrophages (AM), and T cell-mediated responses to Listeria. DEP inhibited AM production of interleukin- (IL-) 1beta, tumor necrosis factor- (TNF-) alpha, and IL-12 but enhanced Listeria-induced AM production of IL-10, which has been shown to prolong the survival of intracellular pathogens such as Listeria. DEP exposure also suppressed the development of bacteria-specific lymphocytes from lung-draining lymph nodes, as indicated by the decreased numbers of T lymphocytes and their CD4(+) and CD8(+) subsets. Furthermore, the DEP exposure markedly inhibited the Listeria-induced lymphocyte secretion of IL-2 at day 7, IL-10 at days 3 and 7, and interferon- (IFN-) gamma at days 3 to 10 postinfection when compared to air-exposed controls. These results show a sustained pattern of downregulation of T cell-mediated immune responses by repeated low-dose DEP exposure, which is different from the results of a single high-dose exposure where the acute effect of DEP aggravated bacteria infection but triggered a strong T cell-mediated immunity.
机译:柴油机排气颗粒(DEP)已显示可改变对细菌感染的肺部免疫反应。发现大鼠在感染后3天暴露于100 mg / m(3)DEP 4小时会加剧单核细胞增生性李斯特菌感染,但由于强T细胞的形成,细菌在感染后7天已被大部分清除。介导的免疫力。在本研究中,我们检查了低剂量重复DEP暴露对肺部对细菌感染的反应的影响。褐挪威大鼠通过以20.62 +/- 1.31 mg / m 3的剂量吸入4h /天,暴露于DEP中,持续5天,然后在最后一次DEP暴露后2 h,用100,000李斯特菌进行气管内接种。暴露于DEP的大鼠在感染后3天和7天均显示肺细菌负荷显着增加。研究表明,重复的DEP暴露可抑制先天性肺泡巨噬细胞(AM)精心策划的活动,以及T细胞介导的对李斯特菌的应答。 DEP抑制白介素(IL-)1β,肿瘤坏死因子(TNF-)α和IL-12的AM产生,但增强了李斯特菌诱导的IL-10的AM产生,这已证明可以延长细胞内病原体的存活时间如李斯特菌。 T淋巴细胞及其CD4(+)和CD8(+)子集数量的减少表明,DEP暴露还抑制了肺引流淋巴结中细菌特异性淋巴细胞的发育。此外,与暴露于空气中相比,DEP暴露在感染后第7天,第3天和第7天显着抑制李斯特菌诱导的淋巴细胞分泌IL-2,在感染后3和7天抑制IL-10以及干扰素(IFN-)γ。控制。这些结果表明,通过反复的低剂量DEP暴露持续存在T细胞介导的免疫反应下调的持续模式,这与一次高剂量DEP的急性作用加剧细菌感染但触发了强烈的T细胞介导的免疫力。

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