| Literature DB >> 24981740 |
Direna Alonso-Curbelo1, Erica Riveiro-Falkenbach1, Eva Pérez-Guijarro1, Metehan Cifdaloz1, Panagiotis Karras1, Lisa Osterloh1, Diego Megías2, Estela Cañón1, Tonantzin G Calvo1, David Olmeda1, Gonzalo Gómez-López3, Osvaldo Graña3, Víctor Javier Sánchez-Arévalo Lobo4, David G Pisano3, Hao-Wei Wang5, Pablo Ortiz-Romero6, Damià Tormo1, Keith Hoek7, José L Rodríguez-Peralto6, Johanna A Joyce5, María S Soengas8.
Abstract
Although common cancer hallmarks are well established, lineage-restricted oncogenes remain less understood. Here, we report an inherent dependency of melanoma cells on the small GTPase RAB7, identified within a lysosomal gene cluster that distinguishes this malignancy from over 35 tumor types. Analyses in human cells, clinical specimens, and mouse models demonstrated that RAB7 is an early-induced melanoma driver whose levels can be tuned to favor tumor invasion, ultimately defining metastatic risk. Importantly, RAB7 levels and function were independent of MITF, the best-characterized melanocyte lineage-specific transcription factor. Instead, we describe the neuroectodermal master modulator SOX10 and the oncogene MYC as RAB7 regulators. These results reveal a unique wiring of the lysosomal pathway that melanomas exploit to foster tumor progression.Entities:
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Year: 2014 PMID: 24981740 DOI: 10.1016/j.ccr.2014.04.030
Source DB: PubMed Journal: Cancer Cell ISSN: 1535-6108 Impact factor: 31.743