| Literature DB >> 31733993 |
Yurena Vivas-García1, Paola Falletta1, Jana Liebing2, Pakavarin Louphrasitthiphol1, Yongmei Feng3, Jagat Chauhan1, David A Scott3, Nicole Glodde2, Ana Chocarro-Calvo4, Sarah Bonham5, Andrei L Osterman3, Roman Fischer5, Ze'ev Ronai3, Custodia García-Jiménez6, Michael Hölzel2, Colin R Goding7.
Abstract
Phenotypic and metabolic heterogeneity within tumors is a major barrier to effective cancer therapy. How metabolism is implicated in specific phenotypes and whether lineage-restricted mechanisms control key metabolic vulnerabilities remain poorly understood. In melanoma, downregulation of the lineage addiction oncogene microphthalmia-associated transcription factor (MITF) is a hallmark of the proliferative-to-invasive phenotype switch, although how MITF promotes proliferation and suppresses invasion is poorly defined. Here, we show that MITF is a lineage-restricted activator of the key lipogenic enzyme stearoyl-CoA desaturase (SCD) and that SCD is required for MITFHigh melanoma cell proliferation. By contrast MITFLow cells are insensitive to SCD inhibition. Significantly, the MITF-SCD axis suppresses metastasis, inflammatory signaling, and an ATF4-mediated feedback loop that maintains de-differentiation. Our results reveal that MITF is a lineage-specific regulator of metabolic reprogramming, whereby fatty acid composition is a driver of melanoma phenotype switching, and highlight that cell phenotype dictates the response to drugs targeting lipid metabolism.Entities:
Keywords: ATF4; MITF; fatty acid saturation; melanoma; metastatic dissemination; phenotype switching; stearoyl CoA desaturase
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Year: 2019 PMID: 31733993 PMCID: PMC7137507 DOI: 10.1016/j.molcel.2019.10.014
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970