| Literature DB >> 29212027 |
Katherine R Singleton1, Lorin Crawford2, Elizabeth Tsui1, Haley E Manchester3, Ophelia Maertens3, Xiaojing Liu1, Maria V Liberti4, Anniefer N Magpusao5, Elizabeth M Stein1, Jennifer P Tingley1, Dennie T Frederick6, Genevieve M Boland6, Keith T Flaherty6, Shannon J McCall7, Clemens Krepler8, Katrin Sproesser8, Meenhard Herlyn8, Drew J Adams5, Jason W Locasale1, Karen Cichowski9, Sayan Mukherjee10, Kris C Wood11.
Abstract
Diverse pathways drive resistance to BRAF/MEK inhibitors in BRAF-mutant melanoma, suggesting that durable control of resistance will be a challenge. By combining statistical modeling of genomic data from matched pre-treatment and post-relapse patient tumors with functional interrogation of >20 in vitro and in vivo resistance models, we discovered that major pathways of resistance converge to activate the transcription factor, c-MYC (MYC). MYC expression and pathway gene signatures were suppressed following drug treatment, and then rebounded during progression. Critically, MYC activation was necessary and sufficient for resistance, and suppression of MYC activity using genetic approaches or BET bromodomain inhibition was sufficient to resensitize cells and delay BRAFi resistance. Finally, MYC-driven, BRAFi-resistant cells are hypersensitive to the inhibition of MYC synthetic lethal partners, including SRC family and c-KIT tyrosine kinases, as well as glucose, glutamine, and serine metabolic pathways. These insights enable the design of combination therapies that select against resistance evolution.Entities:
Keywords: MYC; cancer therapeutics; melanoma; metabolism; signaling networks; synthetic lethality; therapeutic resistance
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Year: 2017 PMID: 29212027 PMCID: PMC5728698 DOI: 10.1016/j.celrep.2017.11.022
Source DB: PubMed Journal: Cell Rep Impact factor: 9.995