Concurrent inhibition of oncogenic and wild-type RAS-GTP for cancer therapy.
Matthew HolderfieldBianca J LeeJingjing JiangAidan TomlinsonKyle J SeamonAlessia MiraEnrico PatruccoGrace GoodhartJulien DillyYevgeniy GindinNuntana DinglasanYingyun WangLick Pui LaiShurui CaiLingyan JiangNicole NasholmNataliya ShifrinCristina BlajHarshit ShahJames W EvansNilufar MontazerOliver LaiJade ShiEthan AhlerElsa QuintanaStephanie ChangAnthony SalvadorAbby MarquezJim CreggYang LiuAnthony MilinAnqi ChenTamar Bar ZivDylan ParsonsJohn E KnoxJennifer E KlompJennifer A RothMatthew G ReesMelissa A RonanAntonio Cuevas-NavarroFeng HuPiro LitoDavid SantamariaAndrew J AguirreAndrew M WatersChanning J DerChiara AmbrogioZhengping WangAdrian L GillElena S KoltunJacqueline A M SmithDavid WildesMallika SinghPublished in: Nature (2024)
RAS oncogenes (collectively NRAS, HRAS and especially KRAS) are among the most frequently mutated genes in cancer, with common driver mutations occurring at codons 12, 13 and 61 1 . Small molecule inhibitors of the KRAS(G12C) oncoprotein have demonstrated clinical efficacy in patients with multiple cancer types and have led to regulatory approvals for the treatment of non-small cell lung cancer 2,3 . Nevertheless, KRAS G12C mutations account for only around 15% of KRAS-mutated cancers 4,5 , and there are no approved KRAS inhibitors for the majority of patients with tumours containing other common KRAS mutations. Here we describe RMC-7977, a reversible, tri-complex RAS inhibitor with broad-spectrum activity for the active state of both mutant and wild-type KRAS, NRAS and HRAS variants (a RAS(ON) multi-selective inhibitor). Preclinically, RMC-7977 demonstrated potent activity against RAS-addicted tumours carrying various RAS genotypes, particularly against cancer models with KRAS codon 12 mutations (KRAS G12X ). Treatment with RMC-7977 led to tumour regression and was well tolerated in diverse RAS-addicted preclinical cancer models. Additionally, RMC-7977 inhibited the growth of KRAS G12C cancer models that are resistant to KRAS(G12C) inhibitors owing to restoration of RAS pathway signalling. Thus, RAS(ON) multi-selective inhibitors can target multiple oncogenic and wild-type RAS isoforms and have the potential to treat a wide range of RAS-addicted cancers with high unmet clinical need. A related RAS(ON) multi-selective inhibitor, RMC-6236, is currently under clinical evaluation in patients with KRAS-mutant solid tumours (ClinicalTrials.gov identifier: NCT05379985).