AZD4625 is a Potent and Selective Inhibitor of KRASG12C.
Atanu ChakrabortyLyndsey HansonDavid RobinsonHilary J LewisSue BickertonMichael DaviesRadoslaw PolanskiRebecca WhiteleyAlex KoersJames AtkinsonTamara BakerIvan Del Barco BarrantesGiovanni CiottaJason G KettleLukasz MagieraCarla P MartinsAlison PeterEleanor M WigmoreZoe UnderwoodSabina CosulichMichael NiedbalaSarah J RossPublished in: Molecular cancer therapeutics (2022)
AZD4625 is a potent, selective, and orally bioavailable inhibitor of oncogenic KRASG12C as demonstrated in cellular assays and in vivo in preclinical cell line-derived and patient-derived xenograft models. In vitro and cellular assays have shown selective binding and inhibition of the KRASG12C mutant isoform, which carries a glycine to cysteine mutation at residue 12, with no binding and inhibition of wild-type RAS or isoforms carrying non-KRASG12C mutations. The pharmacology of AZD4625 shows that it has the potential to provide therapeutic benefit to patients with KRASG12C mutant cancer as either a monotherapy treatment or in combination with other targeted drug agents.