| Literature DB >> 31820981 |
Brian A Lanman, Jennifer R Allen, John G Allen, Albert K Amegadzie, Kate S Ashton, Shon K Booker, Jian Jeffrey Chen, Ning Chen, Michael J Frohn, Guy Goodman, David J Kopecky, Longbin Liu, Patricia Lopez, Jonathan D Low, Vu Ma, Ana E Minatti, Thomas T Nguyen, Nobuko Nishimura, Alexander J Pickrell, Anthony B Reed, Youngsook Shin, Aaron C Siegmund, Nuria A Tamayo, Christopher M Tegley, Mary C Walton, Hui-Ling Wang, Ryan P Wurz, May Xue, Kevin C Yang, Pragathi Achanta, Michael D Bartberger, Jude Canon, L Steven Hollis, John D McCarter, Christopher Mohr, Karen Rex, Anne Y Saiki, Tisha San Miguel, Laurie P Volak, Kevin H Wang, Douglas A Whittington, Stephan G Zech, J Russell Lipford, Victor J Cee.
Abstract
KRASG12C has emerged as a promising target in the treatment of solid tumors. Covalent inhibitors targeting the mutant cysteine-12 residue have been shown to disrupt signaling by this long-"undruggable" target; however clinically viable inhibitors have yet to be identified. Here, we report efforts to exploit a cryptic pocket (H95/Y96/Q99) we identified in KRASG12C to identify inhibitors suitable for clinical development. Structure-based design efforts leading to the identification of a novel quinazolinone scaffold are described, along with optimization efforts that overcame a configurational stability issue arising from restricted rotation about an axially chiral biaryl bond. Biopharmaceutical optimization of the resulting leads culminated in the identification of AMG 510, a highly potent, selective, and well-tolerated KRASG12C inhibitor currently in phase I clinical trials (NCT03600883).Entities:
Year: 2019 PMID: 31820981 DOI: 10.1021/acs.jmedchem.9b01180
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446