Journal
NATURE MEDICINE
Volume 25, Issue 4, Pages 620-+Publisher
NATURE PORTFOLIO
DOI: 10.1038/s41591-019-0367-9
Keywords
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Funding
- National Cancer Institute [R01-CA176839, R01-CA131261, P30-CA042014]
- Pancreatic Cancer Collective
- Melanoma Research Alliance
- Five for the Fight
- Huntsman Cancer Foundation
- Career Award for Medical Scientists from the Burroughs Wellcome Fund
- V Scholar Award
- NIH [R01CA212415]
- National Cancer Institute
- DoD [U54CA224076, W81XWH1410417]
- Fondation pour la Recherche Medicale [FDM20150633361]
- Societe Francaise de Dermatologie
- U.S. Department of Defense (DOD) [W81XWH1410417] Funding Source: U.S. Department of Defense (DOD)
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Pancreatic ductal adenocarcinoma (PDA) was responsible for similar to 44,000 deaths in the United States in 2018 and is the epitome of a recalcitrant cancer driven by a pharmacologically intractable oncoprotein, KRAS(1-4). Downstream of KRAS, the RAF. MEK. ERK signaling pathway plays a central role in pancreatic carcinogenesis(5). However, paradoxically, inhibition of this pathway has provided no clinical benefit to patients with PDA(6). Here we show that inhibition of KRAS -> RAF -> MEK -> ERK signaling elicits autophagy, a process of cellular recycling that protects PDA cells from the cytotoxic effects of KRAS pathway inhibition. Mechanistically, inhibition of MEK1/2 leads to activation of the LKB1 -> AMPK -> ULK1 signaling axis, a key regulator of autophagy. Furthermore, combined inhibition of MEK1/2 plus autophagy displays synergistic anti-proliferative effects against PDA cell lines in vitro and promotes regression of xenografted patient-derived PDA tumors in mice. The observed effect of combination trametinib plus chloroquine was not restricted to PDA as other tumors, including patient-derived xenografts (PDX) of NRAS-mutated melanoma and BRAF-mutated colorectal cancer displayed similar responses. Finally, treatment of a patient with PDA with the combination of trametinib plus hydroxychloroquine resulted in a partial, but nonetheless striking disease response. These data suggest that this combination therapy may represent a novel strategy to target RAS-driven cancers.
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