| Literature DB >> 24931611 |
Sandra Van Schaeybroeck1, Murugan Kalimutho1, Philip D Dunne1, Robbie Carson1, Wendy Allen1, Puthen V Jithesh1, Keara L Redmond1, Takehiko Sasazuki2, Senji Shirasawa3, Jaine Blayney1, Paolo Michieli4, Cathy Fenning1, Heinz-Josef Lenz5, Mark Lawler1, Daniel B Longley1, Patrick G Johnston6.
Abstract
There are currently no approved targeted therapies for advanced KRAS mutant (KRASMT) colorectal cancer (CRC). Using a unique systems biology approach, we identified JAK1/2-dependent activation of STAT3 as the key mediator of resistance to MEK inhibitors in KRASMT CRC in vitro and in vivo. Further analyses identified acute increases in c-MET activity following treatment with MEK inhibitors in KRASMT CRC models, which was demonstrated to promote JAK1/2-STAT3-mediated resistance. Furthermore, activation of c-MET following MEK inhibition was found to be due to inhibition of the ERK-dependent metalloprotease ADAM17, which normally inhibits c-MET signaling by promoting shedding of its endogenous antagonist, soluble "decoy" MET. Most importantly, pharmacological blockade of this resistance pathway with either c-MET or JAK1/2 inhibitors synergistically increased MEK-inhibitor-induced apoptosis and growth inhibition in vitro and in vivo in KRASMT models, providing clear rationales for the clinical assessment of these combinations in KRASMT CRC patients.Entities:
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Year: 2014 PMID: 24931611 DOI: 10.1016/j.celrep.2014.05.032
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423