| Literature DB >> 26601952 |
Andrea Comba1, Luciana L Almada2, Ezequiel J Tolosa2, Eriko Iguchi2, David L Marks2, Marianela Vara Messler3, Renata Silva3, Maite G Fernandez-Barrena2, Elisa Enriquez-Hesles2, Anne L Vrabel2, Bruno Botta4, Lucia Di Marcotulio5, Volker Ellenrieder6, Aldo R Eynard3, Maria E Pasqualini3, Martin E Fernandez-Zapico7.
Abstract
Numerous reports have demonstrated a tumor inhibitory effect of polyunsaturated fatty acids (PUFAs). However, the molecular mechanisms modulating this phenomenon are in part poorly understood. Here, we provide evidence of a novel antitumoral mechanism of the PUFA arachidonic acid (AA). In vivo and in vitro experiments showed that AA treatment decreased tumor growth and metastasis and increased apoptosis. Molecular analysis of this effect showed significantly reduced expression of a subset of antiapoptotic proteins, including BCL2, BFL1/A1, and 4-1BB, in AA-treated cells. We demonstrated that down-regulation of the transcription factor glioma-associated protein 1 (GLI1) in AA-treated cells is the underlying mechanism controlling BCL2, BFL1/A1, and 4-1BB expression. Using luciferase reporters, chromatin immunoprecipitation, and expression studies, we found that GLI1 binds to the promoter of these antiapoptotic molecules and regulates their expression and promoter activity. We provide evidence that AA-induced apoptosis and down-regulation of antiapoptotic genes can be inhibited by overexpressing GLI1 in AA-sensitive cells. Conversely, inhibition of GLI1 mimics AA treatments, leading to decreased tumor growth, cell viability, and expression of antiapoptotic molecules. Further characterization showed that AA represses GLI1 expression by stimulating nuclear translocation of NFATc1, which then binds the GLI1 promoter and represses its transcription. AA was shown to increase reactive oxygen species. Treatment with antioxidants impaired the AA-induced apoptosis and down-regulation of GLI1 and NFATc1 activation, indicating that NFATc1 activation and GLI1 repression require the generation of reactive oxygen species. Collectively, these results define a novel mechanism underlying AA antitumoral functions that may serve as a foundation for future PUFA-based therapeutic approaches.Entities:
Keywords: GLI1; arachidonic acid (AA) (ARA); cancer; cell death; polyunsaturated fatty acid (PUFA); transcription factor
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Year: 2015 PMID: 26601952 PMCID: PMC4722469 DOI: 10.1074/jbc.M115.691972
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157