Shukla A, Timblin C R, Hubbard A K, Bravman J, Mossman B T
Department of Pathology, University of Vermont College of Medicine, Burlington 05405, USA.
Cancer Res. 2001 Mar 1;61(5):1791-5.
Crystalline silica has been classified as a group 1 human carcinogen in the lung. However, its mechanisms of action on pulmonary epithelial cells which give rise to lung cancers are unclear. Using a nontransformed alveolar type II epithelial cell line (C10), we show that alpha-quartz silica causes persistent dose-related increases in phosphorylation of c-Jun-NH2-terminal amino kinases (JNKs) that are inhibited by antioxidants (P < or = 0.05). Increases in activator protein-1 (AP-1) binding to DNA and transactivation of AP-1-dependent gene expression by silica were accompanied by increases in steady-state mRNA levels of the AP-1 family members, c-jun, junB, fra-1, and c-fos at 8 h and elevated mRNA levels of fra-1 at 24 h (P < or = 0.05). Addition of tetramethylthiourea inhibited silica-associated increases infra-1 and proportions of cells in S-phase (P < or = .05). Our findings indicate that silica induces JNK activity, AP-1-dependent gene expression, ie., fra-1, and DNA synthesis via oxidative stress. Moreover, they suggest that silica may act mechanistically as a mitogen or tumor promoter, rather than a genotoxic carcinogen, in the development of lung cancers.
结晶二氧化硅已被列为对人类有致癌性的第1类肺部致癌物。然而,其导致肺癌的对肺上皮细胞的作用机制尚不清楚。利用一种未转化的II型肺泡上皮细胞系(C10),我们发现α-石英二氧化硅会导致c-Jun氨基末端激酶(JNKs)磷酸化持续出现剂量相关的增加,而抗氧化剂可抑制这种增加(P≤0.05)。二氧化硅使激活蛋白-1(AP-1)与DNA的结合增加以及AP-1依赖的基因表达反式激活,同时在8小时时AP-1家族成员c-jun、junB、fra-1和c-fos的稳态mRNA水平增加,在24小时时fra-1的mRNA水平升高(P≤0.05)。添加四甲基硫脲可抑制二氧化硅相关的fra-1增加以及S期细胞比例的增加(P≤0.05)。我们的研究结果表明,二氧化硅通过氧化应激诱导JNK活性、AP-1依赖的基因表达(即fra-1)以及DNA合成。此外,这些结果提示,在肺癌发生过程中,二氧化硅在机制上可能作为一种有丝分裂原或肿瘤促进剂,而非基因毒性致癌物发挥作用。
