| Literature DB >> 28289710 |
Melissa Gilbert-Ross1,2, Jessica Konen1,2, Junghui Koo1,2, John Shupe1,2, Brian S Robinson3, Walter Guy Wiles2,4, Chunzi Huang2,4, W David Martin1, Madhusmita Behera5, Geoffrey H Smith3, Charles E Hill3, Michael R Rossi3,6, Gabriel L Sica3, Manali Rupji2, Zhengjia Chen2,7, Jeanne Kowalski2,7, Andrea L Kasinski8, Suresh S Ramalingam1,2, Haian Fu2,9, Fadlo R Khuri1,2, Wei Zhou1,2,3,10, Adam I Marcus1,2.
Abstract
Loss of LKB1 activity is prevalent in KRAS mutant lung adenocarcinoma and promotes aggressive and treatment-resistant tumors. Previous studies have shown that LKB1 is a negative regulator of the focal adhesion kinase (FAK), but in vivo studies testing the efficacy of FAK inhibition in LKB1 mutant cancers are lacking. Here, we took a pharmacologic approach to show that FAK inhibition is an effective early-treatment strategy for this high-risk molecular subtype. We established a lenti-Cre-induced Kras and Lkb1 mutant genetically engineered mouse model (KLLenti) that develops 100% lung adenocarcinoma and showed that high spatiotemporal FAK activation occurs in collective invasive cells that are surrounded by high levels of collagen. Modeling invasion in 3D, loss of Lkb1, but not p53, was sufficient to drive collective invasion and collagen alignment that was highly sensitive to FAK inhibition. Treatment of early, stage-matched KLLenti tumors with FAK inhibitor monotherapy resulted in a striking effect on tumor progression, invasion, and tumor-associated collagen. Chronic treatment extended survival and impeded local lymph node spread. Lastly, we identified focally upregulated FAK and collagen-associated collective invasion in KRAS and LKB1 comutated human lung adenocarcinoma patients. Our results suggest that patients with LKB1 mutant tumors should be stratified for early treatment with FAK inhibitors.Entities:
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Year: 2017 PMID: 28289710 PMCID: PMC5333956 DOI: 10.1172/jci.insight.90487
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708