Research Papers:
Metformin and trametinib have synergistic effects on cell viability and tumor growth in NRAS mutant cancer
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Abstract
Igor Vujic1,2, Martina Sanlorenzo1,3, Christian Posch1,2 , Rosaura Esteve-Puig1, Adam J. Yen1, Andrew Kwong1, Aaron Tsumura1, Ryan Murphy1, Klemens Rappersberger2 and Susana Ortiz-Urda1
1 University of California, San Francisco, Department of Dermatology, Mt. Zion Cancer Research Center, San Francisco, CA, USA
2 Rudolfstiftung Hospital, Academic Teaching Hospital, Department of Dermatology, Juchgasse, Vienna, Austria
3 Department of Medical Sciences, Section of Dermatology, University of Turin, Italy
Correspondence:
Igor Vujic, email:
Keywords: NRAS, metformin, trametinib, combination therapy
Received: October 08, 2014 Accepted: November 24, 2014 Published: November 25, 2014
Abstract
Attempts to directly block the mutant neuroblastoma rat sarcoma oncogene (NRAS) protein, a driving mutation in many cancer types, have been unsuccessful. Current treatments focus on inhibition of different components of NRAS’ two main downstream cascades: PI3K/AKT/mTOR and MAPK. Here we test a novel dual therapy combination of metformin and trametinib on a panel of 16 NRAS mutant cell lines, including melanoma cells, melanoma cells with acquired trametinib resistance, lung cancer and neuroblastoma cells. We show that both of the main downstream cascades of NRAS can be blocked by this combination: metformin indirectly inhibits the PI3K/AKT/mTOR pathway and trametinib directly impedes the MAPK pathway. This dual therapy synergistically reduced cell viability in vitro and xenograft tumor growth in vivo. We conclude that metformin and trametinib combinations are effective in preclinical models and may be a possible option for treatment of NRAS mutant cancers.
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