Journal
ONCOTARGET
Volume 6, Issue 39, Pages 42183-42196Publisher
IMPACT JOURNALS LLC
DOI: 10.18632/oncotarget.5619
Keywords
HRAS mutations; MEK inhibitor; mTOR inhibitor; lung cancer; bladder cancer
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Funding
- Forschungskredit Zurich University
- Stiftung zur Krebsbekampfung
- Gottfried and Julia Bangerter-Rhyner Foundation
- FPU (Formacion del Profesorado Universitario) from the Spanish Government
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HRAS is a frequently mutated oncogene in cancer. However, mutant HRAS as drug target has not been investigated so far. Here, we show that mutant HRAS hyperactivates the RAS and the mTOR pathway in various cancer cell lines including lung, bladder and esophageal cancer. HRAS mutation sensitized toward growth inhibition by the MEK inhibitors AZD6244, MEK162 and PD0325901. Further, we found that MEK inhibitors induce apoptosis in mutant HRAS cell lines but not in cell lines lacking RAS mutations. In addition, knockdown of HRAS by siRNA blocked cell growth in mutant HRAS cell lines. Inhibition of the PI3K pathway alone or in combination with MEK inhibitors did not alter signaling nor had an impact on viability. However, inhibition of mTOR or combined inhibition of MEK and mTOR reduced cell growth in a synergistic manner. Finally, Ba/F3 cells transformed with mutant HRAS isoforms Q61L, Q61R and G12V demonstrated equal sensitivity towards MEK and mTOR inhibition. Our results show that HRAS mutations in cancer activate the RAS and mTOR pathways which might serve as a therapeutic option for patients with HRAS mutant tumors.
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