| Literature DB >> 26739882 |
Matthew P Patricelli1, Matthew R Janes1, Lian-Sheng Li1, Rasmus Hansen1, Ulf Peters1, Linda V Kessler1, Yuching Chen1, Jeff M Kucharski1, Jun Feng1, Tess Ely1, Jeffrey H Chen1, Sarah J Firdaus1, Anjali Babbar1, Pingda Ren1, Yi Liu2.
Abstract
UNLABELLED: KRAS gain-of-function mutations occur in approximately 30% of all human cancers. Despite more than 30 years of KRAS-focused research and development efforts, no targeted therapy has been discovered for cancers with KRAS mutations. Here, we describe ARS-853, a selective, covalent inhibitor of KRAS(G12C) that inhibits mutant KRAS-driven signaling by binding to the GDP-bound oncoprotein and preventing activation. Based on the rates of engagement and inhibition observed for ARS-853, along with a mutant-specific mass spectrometry-based assay for assessing KRAS activation status, we show that the nucleotide state of KRAS(G12C) is in a state of dynamic flux that can be modulated by upstream signaling factors. These studies provide convincing evidence that the KRAS(G12C) mutation generates a "hyperexcitable" rather than a "statically active" state and that targeting the inactive, GDP-bound form is a promising approach for generating novel anti-RAS therapeutics. SIGNIFICANCE: A cell-active, mutant-specific, covalent inhibitor of KRAS(G12C) is described that targets the GDP-bound, inactive state and prevents subsequent activation. Using this novel compound, we demonstrate that KRAS(G12C) oncoprotein rapidly cycles bound nucleotide and responds to upstream signaling inputs to maintain a highly active state. ©2016 American Association for Cancer Research.Entities:
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Year: 2016 PMID: 26739882 DOI: 10.1158/2159-8290.CD-15-1105
Source DB: PubMed Journal: Cancer Discov ISSN: 2159-8274 Impact factor: 39.397