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氟化物诱导人肺上皮细胞合成白细胞介素-6和白细胞介素-8

Fluoride-induced interleukin-6 and interleukin-8 synthesis in human epithelial lung cells.

作者信息

Refsnes M, Becher R, Lâg M, Skuland T, Schwarze P E

机构信息

Department of Environmental Medicine, National Institute of Public Health, P.O. Box 4404 Torshov, N-0403 Oslo, Norway.

出版信息

Hum Exp Toxicol. 1999 Nov;18(11):645-52. doi: 10.1191/096032799678839572.

Abstract

Exposure to fluorides has been associated with asthmatic symptoms among workers in the aluminium industry. In a recent experimental study hydrogen fluoride (HF) was found to induce a weak inflammatory response in humans. In the present study the potential of sodium fluoride (NaF) and HF to induce cytokine response was examined and how these responses are modulated by Al3+ in a human epithelial lung cell line (A549). Dose-response experiments showed a maximal release of IL-6 and IL-8 at a concentration of 5 mM NaF 24 h after addition. The responses to HF were of a similar magnitude as for NaF. Time-course experiments showed a NaF-induced IL-6 response at 5 h, whereas an IL-8 response was observed after 10 h. Cycloheximide treatment completely abolished the NaF-induced cytokine responses. A marked increase in the mRNA level for IL-6 was observed already 2 h after exposure to 5 mM NaF, and presumably is a prerequisite for the subsequent increase of IL-6. The fluoride-induced effects on IL-6 and IL-8 release were strongly reduced by pretreatment with deferoxamine (an Al3+-chelator), and enhanced by addition of Al3+. This indicates that an AlF4-- complex, a known activator of GTP-binding proteins, is involved in fluoride-induced IL-6 and IL-8 responses in A549 cells.

摘要

接触氟化物与铝行业工人的哮喘症状有关。在最近的一项实验研究中,发现氟化氢(HF)会在人体中诱发微弱的炎症反应。在本研究中,检测了氟化钠(NaF)和HF诱导细胞因子反应的潜力,以及在人肺上皮细胞系(A549)中这些反应如何被Al3+调节。剂量反应实验表明,添加后24小时,在5 mM NaF浓度下,IL-6和IL-8释放达到最大值。对HF的反应与对NaF的反应幅度相似。时间进程实验表明,NaF在5小时时诱导IL-6反应,而在10小时后观察到IL-8反应。环己酰亚胺处理完全消除了NaF诱导的细胞因子反应。暴露于5 mM NaF后2小时,IL-6的mRNA水平就已显著增加,这可能是随后IL-6增加的先决条件。用去铁胺(一种Al3+螯合剂)预处理可强烈降低氟化物对IL-6和IL-8释放的影响,而添加Al3+则会增强这种影响。这表明,已知的GTP结合蛋白激活剂AlF4-复合物参与了A549细胞中氟化物诱导的IL-6和IL-8反应。

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