@article{baf155e65dfd456eb5c41f58dd71e9a0,
title = "A functional landscape of resistance to MEK1/2 and CDK4/6 inhibition in NRAS-mutant melanoma",
abstract = "Combinatorial inhibition of MEK1/2 and CDK4/6 is currently undergoing clinical investigation in NRAS-mutant melanoma. To prospectively map the landscape of resistance to this investigational regimen, we utilized a series of gain- and loss-of-function forward genetic screens to identify modulators of resistance to clinical inhibitors of MEK1/2 and CDK4/6 alone and in combination. First, we identified NRAS-mutant melanoma cell lines that were dependent on NRAS for proliferation and sensitive to MEK1/2 and CDK4/6 combination treatment. We then used a genome-scale ORF overexpression screen and a CRISPR knockout screen to identify modulators of resistance to each inhibitor alone or in combination. These orthogonal screening approaches revealed concordant means of achieving resistance to this therapeutic modality, including tyrosine kinases, RAF, RAS, AKT, and PI3K signaling. Activated KRAS was sufficient to cause resistance to combined MEK/CDK inhibition and to replace genetic depletion of oncogenic NRAS. In summary, our comprehensive functional genetic screening approach revealed modulation of resistance to the inhibition of MEK1/2, CDK4/6, or their combination in NRAS-mutant melanoma. Significance: These findings reveal that NRAS-mutant melanomas can acquire resistance to genetic ablation of NRAS or combination MEK1/2 and CDK4/6 inhibition by upregulating activity of the RTK-RAS-RAF and RTK-PI3K-AKT signaling cascade.",
author = "Hayes, {Tikvah K.} and Flora Luo and Ofir Cohen and Goodale, {Amy B.} and Yenarae Lee and Sasha Pantel and Mukta Bagul and Federica Piccioni and Root, {David E.} and Garraway, {Levi A.} and Matthew Meyerson and Johannessen, {Cory M.}",
note = "Funding Information: This workwas conducted as part of the Slim Initiative forGenomicMedicine, a project funded by the Carlos Slim Foundation in Mexico. This work was supported by a Career Development Award from the Melanoma Research Foundation (C.M. Johannessen). We acknowledge additional support from the NCI to L.A. Garraway (3R35CA197737) and M. Meyerson (1R35CA197568) andDamonRunyon Cancer Research Foundation award to T. K. Hayes (David Livingston Fellow).M.Meyerson is an American Cancer Society Research Professor. Funding Information: This work was conducted as part of the Slim Initiative for Genomic Medicine, a project funded by the Carlos Slim Foundation in Mexico. This work was supported by a Career Development Award from the Melanoma Research Foundation (C.M. Johannessen). We acknowledge additional support from the NCI to L.A. Garraway (3R35CA197737) and M. Meyerson Funding Information: F. Luo is a Technology Specialist at Wolf Greenfield & Sacks, P.C. L.A. Garraway is a Sr. VP Oncology R&D at Eli Lilly and Company; was at Howard Hughes Medical Institute; was equity consultant at Foundation Medicine; reports receiving commercial research grant from Novartis and Astellas; and has ownership interest (including stock, patents, etc.) in Tango Therapeutics. L.A. Garraway is a co-founder and equity holder of Tango Therapeutics and was a consultant for Foundation Medicine and held equity, some of which was sold to Roche. M. Meyerson is a scientific advisory board member for OrigiMed and receives consulting fees for this role; was a consultant for Foundation Medicine and held equity, some of which was sold to Roche; receives research support from Bayer and is an inventor of several joint patents and patent applications, none of which have been licensed at the time of this disclosure (12-17-18); is an inventor on several patents on EGFR mutations in lung cancer diagnosis, licensed to LabCorp, for which he receives royalties; is an inventor on several patent applications on Fusobacterium, none issued or licensed; the inventor on a patent for pathogen discovery, not licensed, for none of which he receives royalties. No potential conflicts of interest were disclosed by the other authors. Publisher Copyright: {\textcopyright} 2019 American Association for Cancer Research.",
year = "2019",
month = may,
doi = "10.1158/0008-5472.CAN-18-2711",
language = "English",
volume = "79",
pages = "2352--2366",
journal = "Cancer Research",
issn = "0008-5472",
publisher = "American Association for Cancer Research Inc.",
number = "9",
}