Zhang Dongyun, Li Jingxia, Wu Kangjian, Ouyang Weiming, Ding Jin, Liu Zheng-gang, Costa Max, Huang Chuanshu
Nelson Institute of Environmental Medicine, New York University School of Medicine, 57 Old Forge Road, Tuxedo, NY 10987, USA.
Carcinogenesis. 2007 Apr;28(4):883-91. doi: 10.1093/carcin/bgl186. Epub 2006 Oct 25.
Activation of the signaling pathways leading to gene expression regulation is critical in the carcinogenic effects of nickel exposure. In the present study, we found nickel exposure could induce cyclooxygenase-2 (COX-2) expression at transcriptional and protein levels in both human bronchoepithelial cells (Beas-2B) and murine embryonic fibroblasts (MEFs). We further provided direct evidence for the specific involvement of the JNK1 signaling pathway in the COX-2 induction using specific gene knockout approaches. Our results demonstrated that COX-2 induction by nickel was impaired in JNK1(-/-) MEFs, but not in JNK2(-/-) MEFs. Moreover, re-constitutional expression of JNK1 restored COX-2 induction, confirming the specific requirement of JNK1 in COX-2 induction. Further investigation revealed that JNK1 mediated the nickel-induced COX-2 expression in a c-Jun/AP-1-dependent manner. Ectopic expression of TAM67, a c-Jun dominant negative mutant, also suppressed the COX-2 induction. Our results demonstrate that the JNK1/c-Jun/AP-1 pathway, but not the JNK2 pathway, plays a critical role in nickel-induced COX-2 expression.
导致基因表达调控的信号通路激活在镍暴露的致癌作用中至关重要。在本研究中,我们发现镍暴露可在人支气管上皮细胞(Beas-2B)和小鼠胚胎成纤维细胞(MEF)中诱导转录和蛋白水平的环氧合酶-2(COX-2)表达。我们进一步使用特定基因敲除方法为JNK1信号通路在COX-2诱导中的特定参与提供了直接证据。我们的结果表明,镍诱导的COX-2在JNK1(-/-)MEF中受损,但在JNK2(-/-)MEF中未受损。此外,JNK1的重组表达恢复了COX-2诱导,证实了JNK1在COX-2诱导中的特定需求。进一步研究表明,JNK1以c-Jun/AP-1依赖性方式介导镍诱导的COX-2表达。c-Jun显性负突变体TAM67的异位表达也抑制了COX-2诱导。我们的结果表明,JNK1/c-Jun/AP-1通路而非JNK2通路在镍诱导的COX-2表达中起关键作用。
