| Literature DB >> 29149598 |
Barbara Fontanals-Cirera1, Dan Hasson2, Chiara Vardabasso2, Raffaella Di Micco1, Praveen Agrawal1, Asif Chowdhury2, Madeleine Gantz2, Ana de Pablos-Aragoneses1, Ari Morgenstern1, Pamela Wu3, Dan Filipescu2, David Valle-Garcia2, Farbod Darvishian1, Jae-Seok Roe4, Michael A Davies5, Christopher R Vakoc4, Eva Hernando6, Emily Bernstein7.
Abstract
Bromodomain and extraterminal domain inhibitors (BETi) represent promising therapeutic agents for metastatic melanoma, yet their mechanism of action remains unclear. Here we interrogated the transcriptional effects of BETi and identified AMIGO2, a transmembrane molecule, as a BET target gene essential for melanoma cell survival. AMIGO2 is upregulated in melanoma cells and tissues compared to human melanocytes and nevi, and AMIGO2 silencing in melanoma cells induces G1/S arrest followed by apoptosis. We identified the pseudokinase PTK7 as an AMIGO2 interactor whose function is regulated by AMIGO2. Epigenomic profiling and genome editing revealed that AMIGO2 is regulated by a melanoma-specific BRD2/4-bound promoter and super-enhancer configuration. Upon BETi treatment, BETs are evicted from these regulatory elements, resulting in AMIGO2 silencing and changes in PTK7 proteolytic processing. Collectively, this study uncovers mechanisms underlying the therapeutic effects of BETi in melanoma and reveals the AMIGO2-PTK7 axis as a targetable pathway for metastatic melanoma.Entities:
Keywords: AMIGO2; BET; BET inhibition; BRD2; BRD4; PTK7; enhancers; melanoma
Mesh:
Substances:
Year: 2017 PMID: 29149598 PMCID: PMC5993436 DOI: 10.1016/j.molcel.2017.11.004
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970