Identification of GDC-1971 (RLY-1971), a SHP2 Inhibitor Designed for the Treatment of Solid Tumors.
Alexander M TaylorBret R WilliamsFabrizio GiordanettoElizabeth H KelleyAndré LescarbeauKelley ShortsleevesYong TangW Patrick WaltersAlfonso ArrazateChristine BowmanErin BrophyEmily W ChanGauri DeshmukhJack B GreismanThomas L HunsakerD Randal KippPablo Saenz Lopez-LarrochaDanilo MaddaloIain J MartinPaul MaragakisMark MerchantMark MurckoHunter M NisonoffVi NguyenVy NguyenOlivia OrozcoChristopher OwenLevi PierceMolly SchmidtDavid E ShawSherri SmithEric TherrienJohn C TranJim WattersNigel J WatersJeremy WilburLindsay WillmorePublished in: Journal of medicinal chemistry (2023)
Protein tyrosine phosphatase SHP2 mediates RAS-driven MAPK signaling and has emerged in recent years as a target of interest in oncology, both for treating with a single agent and in combination with a KRAS inhibitor. We were drawn to the pharmacological potential of SHP2 inhibition, especially following the initial observation that drug-like compounds could bind an allosteric site and enforce a closed, inactive state of the enzyme. Here, we describe the identification and characterization of GDC-1971 (formerly RLY-1971), a SHP2 inhibitor currently in clinical trials in combination with KRAS G12C inhibitor divarasib (GDC-6036) for the treatment of solid tumors driven by a KRAS G12C mutation.