Discovery and Optimization of a Potent, Efficacious, and Brain-Penetrant Inhibitor of KRAS G12C.

Publication Type:

Journal Article

Authors:

Landry, Matthew L; Malhotra, Sushant; Beresini, Maureen; Chan, Connie; Chan, Emily; de la Cruz, Cecile C; Endres, Nicholas F; Evangelista, Marie; Gustafson, Amy; Hu, Dennis; Hunsaker, Thomas; Hsu, Peter; Izrayelit, Yevgeniy; La, Hank; Saenz-Lopez Larrocha, Pablo; Lian, Qihui; Merchant, Mark; Mao, Jialin; Mroue, Rana; Oh, Angela; Plise, Emile; Shao, Cheng; Siu, Michael; Tran, John C; Wang, Yanguang; Wang, Weiru; Wei, Binqing; Wong, Susan; Yen, Chun-Wan; Zhou, Yuhui; Purkey, Hans E; Heffron, Timothy P; Salphati, Laurent

Source:

J Med Chem, Volume 69, Issue 5, p.5241-5258 (2026)

Keywords:

Animals, Antineoplastic Agents, Brain, Cell Line, Tumor, Drug Discovery, Humans, Mice, Mutation, Proto-Oncogene Proteins p21(ras), Rats, Structure-Activity Relationship

Abstract:

<p>Mutant KRAS is highly prevalent in human cancer and has been actively pursued as a target for drug discovery. Much progress has been made in drugging KRAS G12C, owing to the ability of inhibitors to covalently target its oncogenic cysteine mutation at codon 12. A number of KRAS G12C inhibitors have advanced to clinical development and are being investigated for the treatment of a variety of solid tumors. Notably, many patients with KRAS G12C-positive non-small cell lung cancer develop brain metastases. Herein, we report the discovery and development of a brain-penetrant inhibitor of KRAS G12C using as a starting point. Optimization efforts focused on reducing molecular weight and topological polar surface area as well as shielding of hydrogen bond donors. In this manner, active transport by both P-gp and breast cancer resistance protein (BCRP) was attenuated, and high exposure in rodent brain tissue was achieved.</p>

PDB: 
9PIZ
Beamline: 
24-ID-C