Dagher Zeina, Garçon Guillaume, Billet Sylvain, Gosset Pierre, Ledoux Frédéric, Courcot Dominique, Aboukais Antoine, Shirali Pirouz
LCE EA2598, Toxicologie Industrielle et Environnementale, Maison de la Recherche en Environnement Industriel de Dunkerque 2, 189A, Avenue Maurice Schumann, 59140 Dunkerque, France.
Toxicology. 2006 Aug 1;225(1):12-24. doi: 10.1016/j.tox.2006.04.038. Epub 2006 Jun 19.
Epidemiological studies have associated the increase of respiratory and cardiovascular mortality and morbidity with high levels of air pollution particulate matter (PM). However, the underlying mechanisms of actions by which PM induce adverse health effects are still unclear. We have recently undertaken an extensive investigation of the adverse health effects of air pollution PM(2.5), and shown that in vitro short-term exposure to PM(2.5) induced oxidative stress and inflammation in human lung epithelial cells (L132). Hence, it was convenient to complete the physical and chemical characterization of PM and to investigate whether in vitro short-term exposure to PM could be imply in the activation of apoptosis. Accordingly, we found that 92.15% of PM were equal or smaller than 2.5 microm and their specific surface area was 1m(2)/g. Inorganic (i.e. Fe, Al, Ca, Na, K, Mg, Pb, etc.) and organic (i.e. polycyclic aromatic hydrocarbons) chemicals were found in PM, suggesting that much of them derived from wind-borne dust from the industrial complex and the heavy motor vehicle traffic. In other respects, we showed that PM exposure induced apoptosis by activating not only the tumor necrosis factor-alpha (TNF-alpha)-induced pathway (i.e. TNF-alpha secretion, caspase-8 and -3 activation), but also the mitochondrial pathway (i.e. 8-hydroxy-2'-desoxyguanosine formation, cytochrome c release from mitochondria, caspase-9 and -3 activation). Moreover, changes in the transcription rates of p53, bcl-2, and bax genes, on the one hand, and DNA fragmentation, on the other hand, were reported in PM-exposed proliferating L132 cells, revealing the occurrence of apoptotic events. Taken together, these findings suggested that in vitro short-term exposure to PM(2.5) induced apoptosis in L132 cells.
流行病学研究表明,呼吸系统和心血管疾病的死亡率及发病率增加与高浓度的空气污染颗粒物(PM)有关。然而,PM导致不良健康影响的潜在作用机制仍不清楚。我们最近对空气污染PM2.5的不良健康影响进行了广泛调查,结果显示,体外短期暴露于PM2.5可诱导人肺上皮细胞(L132)产生氧化应激和炎症。因此,对PM进行物理和化学特性分析,并研究体外短期暴露于PM是否会引发细胞凋亡,是很有必要的。相应地,我们发现92.15%的PM等于或小于2.5微米,其比表面积为1平方米/克。在PM中发现了无机(如铁、铝、钙、钠、钾、镁、铅等)和有机(如多环芳烃)化学物质,这表明其中许多物质来自工业园区的风尘和重型机动车交通。在其他方面,我们发现PM暴露不仅通过激活肿瘤坏死因子-α(TNF-α)诱导的途径(即TNF-α分泌、半胱天冬酶-8和-3激活),还通过线粒体途径(即8-羟基-2'-脱氧鸟苷形成、细胞色素c从线粒体释放、半胱天冬酶-9和-3激活)诱导细胞凋亡。此外,在暴露于PM的增殖L132细胞中,一方面报道了p53、bcl-2和bax基因转录率的变化,另一方面报道了DNA片段化,揭示了凋亡事件的发生。综上所述,这些发现表明体外短期暴露于PM2.5可诱导L132细胞凋亡。
