期刊
CELL DEATH AND DIFFERENTIATION
卷 18, 期 1, 页码 109-121出版社
NATURE PUBLISHING GROUP
DOI: 10.1038/cdd.2010.75
关键词
melanoma; thiazolidinedione; chemokine; MITF; apoptosis
资金
- INSERM
- University of Nice Sophia-Antipolis
- Fondation pour la Recherche Medicale (FRM)
- ARC [5093]
- Ministere de l'Enseignement Superieur et de la Recherche
- ARC (France)
We have previously demonstrated that the thiazolidinedione ciglitazone inhibited, independently of PPAR gamma activation, melanoma cell growth. Further investigations now show that ciglitazone effects are mediated through the regulation of secreted factors. Q-PCR screening of several genes involved in melanoma biology reveals that ciglitazone inhibits expression of the CXCL1 chemokine gene. CXCL1 is overexpressed in melanoma and contributes to tumorigenicity. We show that ciglitazone induces a diminution of CXCL1 level in different human melanoma cell lines. This effect is mediated by the downregulation of microphthalmia-associated transcription factor, MITF, the master gene in melanocyte differentiation and involved in melanoma development. Further, recombinant CXCL1 protein is sufficient to abrogate thiazolidinedione effects such as apoptosis induction, whereas extinction of the CXCL1 pathway mimics phenotypic changes observed in response to ciglitazone. Finally, inhibition of human melanoma tumor development in nude mice treated with ciglitazone is associated with a strong decrease in MITF and CXCL1 levels. Our results show that anti-melanoma effects of thiazolidinediones involve an inhibition of the MITF/CXCL1 axis and highlight the key role of this specific pathway in melanoma malignancy. Cell Death and Differentiation (2011) 18, 109-121; doi: 10.1038/cdd.2010.75; published online 2 July 2010
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