Literature DB >> 21996743

Hypoxia and MITF control metastatic behaviour in mouse and human melanoma cells.

Y Cheli1, S Giuliano, N Fenouille, M Allegra, V Hofman, P Hofman, P Bahadoran, J-P Lacour, S Tartare-Deckert, C Bertolotto, R Ballotti.   

Abstract

Melanomas are very aggressive neoplasms with notorious resistance to therapeutics. It was recently proposed that the remarkable phenotypic plasticity of melanoma cells allows for the rapid development of both resistance to chemotherapeutic drugs and invasive properties. Indeed, the capacity of melanoma cells to form distant metastases is the main cause of mortality in melanoma patients. Therefore, the identification of the mechanism controlling melanoma phenotype is of paramount importance. In the present report, we show that deletion of microphthalmia-associated transcription factor (MITF), the master gene in melanocyte differentiation, is sufficient to increase the metastatic potential of mouse and human melanoma cells. MITF silencing also increases fibronectin and Snail, two mesenchymal markers that might explain the increased invasiveness in vitro and in vivo. Furthermore, ablation of this population by Forskolin-induced differentiation or MITF-forced expression significantly decreases tumour and metastasis formation, suggesting that eradication of low-MITF cells might improve melanoma treatment. Moreover, we demonstrate that a hypoxic microenvironment decreases MITF expression through an indirect, hypoxia-inducible factor 1 (HIF1)α-dependant transcriptional mechanism, and increases the tumourigenic and metastatic properties of melanoma cells. We identified Bhlhb2, a new factor in melanoma biology, as the mediator of hypoxia/HIF1α inhibitory effect on MITF expression. Our results reveal a hypoxia-HIF1α-BHLHB2-MITF cascade controlling the phenotypic plasticity in melanoma cells and favouring metastasis development. Targeting this pathway might be helpful in the design of new anti-melanoma therapies.

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Year:  2011        PMID: 21996743     DOI: 10.1038/onc.2011.425

Source DB:  PubMed          Journal:  Oncogene        ISSN: 0950-9232            Impact factor:   9.867


  90 in total

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Journal:  Epigenetics       Date:  2016-02-18       Impact factor: 4.528

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Journal:  Pigment Cell Melanoma Res       Date:  2018-01-29       Impact factor: 4.693

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4.  Distinct microRNA expression signatures are associated with melanoma subtypes and are regulated by HIF1A.

Authors:  Hun-Way Hwang; Laura L Baxter; Stacie K Loftus; Julia C Cronin; Niraj S Trivedi; Bhavesh Borate; William J Pavan
Journal:  Pigment Cell Melanoma Res       Date:  2014-05-27       Impact factor: 4.693

Review 5.  Pro-survival role of MITF in melanoma.

Authors:  Mariusz L Hartman; Malgorzata Czyz
Journal:  J Invest Dermatol       Date:  2014-08-21       Impact factor: 8.551

6.  Hypoxia and MITF regulate KIT oncogenic properties in melanocytes.

Authors:  F Laugier; J Delyon; J André; A Bensussan; N Dumaz
Journal:  Oncogene       Date:  2016-03-14       Impact factor: 9.867

Review 7.  Molecular pathways: BRAF induces bioenergetic adaptation by attenuating oxidative phosphorylation.

Authors:  Rizwan Haq; David E Fisher; Hans R Widlund
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Review 8.  Emerging role of DUBs in tumor metastasis and apoptosis: Therapeutic implication.

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Journal:  Pharmacol Ther       Date:  2017-03-06       Impact factor: 12.310

9.  Understanding melanoma stem cells.

Authors:  Nicholas Nguyen; Kasey L Couts; Yuchun Luo; Mayumi Fujita
Journal:  Melanoma Manag       Date:  2015

10.  PGC-1 coactivators regulate MITF and the tanning response.

Authors:  Jonathan Shoag; Rizwan Haq; Mingfeng Zhang; Laura Liu; Glenn C Rowe; Aihua Jiang; Nicole Koulisis; Caitlin Farrel; Christopher I Amos; Qingyi Wei; Jeffrey E Lee; Jiangwen Zhang; Thomas S Kupper; Abrar A Qureshi; Rutao Cui; Jiali Han; David E Fisher; Zoltan Arany
Journal:  Mol Cell       Date:  2012-11-29       Impact factor: 17.970

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