Targeting KRAS Mutant Cancers via Combination Treatment: Discovery of a 5-Fluoro-4-(3H)-quinazolinone Aryl Urea pan-RAF Kinase Inhibitor.
Malcolm P HuestisDarlene Dela CruzAntonio G DiPasqualeMatthew R DurkCharles EigenbrotPaul GibbonsAlberto GobbiThomas L HunsakerHank LaDennis H LeungWendy LiuShiva MalekMark MerchantJohn G MoffatChristine S MuliChristine J OrrBrendan T ParrFrances ShanahanChristopher J SneeringerWeiru WangIvana YenJianping YinMichael SiuJoachim RudolphPublished in: Journal of medicinal chemistry (2021)
Optimization of a series of aryl urea RAF inhibitors led to the identification of type II pan-RAF inhibitor GNE-0749 (7), which features a fluoroquinazolinone hinge-binding motif. By minimizing reliance on common polar hinge contacts, this hinge binder allows for a greater contribution of RAF-specific residue interactions, resulting in exquisite kinase selectivity. Strategic substitution of fluorine at the C5 position efficiently masked the adjacent polar NH functionality and increased solubility by impeding a solid-state conformation associated with stronger crystal packing of the molecule. The resulting improvements in permeability and solubility enabled oral dosing of 7. In vivo evaluation of 7 in combination with the MEK inhibitor cobimetinib demonstrated synergistic pathway inhibition and significant tumor growth inhibition in a KRAS mutant xenograft mouse model.