| Literature DB >> 34992247 |
Christopher W Davies1, Angela J Oh2, Rana Mroue3, Micah Steffek4, John M Bruning4, Yang Xiao3, Siyu Feng3, Sangeeta Jayakar5, Emily Chan6, Vidhyalakshmi Arumugam6, Sean Carlo Uribe4, Jake Drummond4, Alexandra Frommlet4, Cheng Lu7, Yvonne Franke8, Mark Merchant6, Hartmut Koeppen5, John G Quinn4, Sushant Malhotra9, Steve Do9, Lewis Gazzard9, Hans E Purkey9, Joachim Rudolph9, Melinda M Mulvihill10, James T Koerber11, Weiru Wang12, Marie Evangelista13.
Abstract
Small molecules that stabilize inactive protein conformations are an underutilized strategy for drugging dynamic or otherwise intractable proteins. To facilitate the discovery and characterization of such inhibitors, we created a screening platform to identify conformation-locking antibodies for molecular probes (CLAMPs) that distinguish and induce rare protein conformational states. Applying the approach to KRAS, we discovered CLAMPs that recognize the open conformation of KRASG12C stabilized by covalent inhibitors. One CLAMP enables the visualization of KRASG12C covalent modification in vivo and can be used to investigate response heterogeneity to KRASG12C inhibitors in patient tumors. A second CLAMP enhances the affinity of weak ligands binding to the KRASG12C switch II region (SWII) by stabilizing a specific conformation of KRASG12C, thereby enabling the discovery of such ligands that could serve as leads for the development of drugs in a high-throughput screen. We show that combining the complementary properties of antibodies and small molecules facilitates the study and drugging of dynamic proteins.Entities:
Mesh:
Substances:
Year: 2022 PMID: 34992247 DOI: 10.1038/s41587-021-01126-9
Source DB: PubMed Journal: Nat Biotechnol ISSN: 1087-0156 Impact factor: 68.164