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Discovery of Aminopyrazole Derivatives as Potent Inhibitors of Wild-Type and Gatekeeper Mutant FGFR2 and 3 |
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| Authors: | Ryan A. Brawn Andrew Cook Kiyoyuki Omoto Jiyuan Ke Craig Karr Federico Colombo Milena Virrankoski Sudeep Prajapati Dominic Reynolds David M. Bolduc Tuong-Vi Nguyen Patricia Gee Deanna Borrelli Benjamin Caleb Shihua Yao Sean Irwin Nicholas A. Larsen Anand Selvaraj Xuesong Zhao Stephanos Ioannidis |
| Affiliation: | H3 Biomedicine, 300 Technology Square, Cambridge, Massachusetts 02139, United States |
| Abstract: | Fibroblast growth factor receptors (FGFR) 2 and 3 have been established as drivers of numerous types of cancer with multiple drugs approved or entering late stage clinical trials. A limitation of current inhibitors is vulnerability to gatekeeper resistance mutations. Using a combination of targeted high-throughput screening and structure-based drug design, we have developed a series of aminopyrazole based FGFR inhibitors that covalently target a cysteine residue on the P-loop of the kinase. The inhibitors show excellent activity against the wild-type and gatekeeper mutant versions of the enzymes. Further optimization using SAR analysis and structure-based drug design led to analogues with improved potency and drug metabolism and pharmacokinetics properties. |
| Keywords: | FGFR FGFR2 FGFR3 kinase inhibitor gatekeeper mutant RTK |