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. 2025 Jul 3;15(7):1392-1409.
doi: 10.1158/2159-8290.CD-24-0614.

Direct Inhibition of RAS Reveals the Features of Oncogenic Signaling Driven by RAS G12 and Q61 Mutations

Michelangelo Marasco  1 Dinesh Kumar  1 Santiago Garcia Borrego  2 Tessa Seale  2 Giulia Maddalena  3   4   5 Riccardo Mezzadra  6 Kylie Belanger  2   7   8 Soren Cole  2 Brayan Perez  2   7   8 Wei Luan  6 Radha Mukherjee  1 Ilinca Aricescu  1 Vladimir Markov  9 Yuxin Zhu  9 Sabrina Arena  10   11 Alberto Bardelli  12   13 Elisa de Stanchina  9 Scott W Lowe  6 Richard A Burkhart  2   14 Jacquelyn W Zimmerman  2   8 Rona Yaeger  15 Scott E Kopetz  3 Neal Rosen  1   15 Sandra Misale  2
Affiliations

Direct Inhibition of RAS Reveals the Features of Oncogenic Signaling Driven by RAS G12 and Q61 Mutations

Michelangelo Marasco et al. Cancer Discov. .

Abstract

RAS genes are frequently mutated in cancer, often at codons 12 and 61. With the recent introduction of RAS inhibitors, we can now directly investigate the effects of specific RAS mutations in cancer cells. In this study, we demonstrate that in tumors with RASG12X mutations, mutant RAS can be activated by receptor tyrosine kinases (RTK), and PI3K activation is dependent on mutant RAS. Conversely, RASQ61X mutations activate the MAPK cascade independently of RTKs, and inhibition of RASQ61X impairs MAPK pathway activation but leaves the PI3K pathway unaffected. Our characterization of these distinct features of G12X and Q61X mutations suggests that co-inhibition of RAS and RTKs selectively inhibits the growth of RASG12X-mutant tumors, both in vitro and in vivo, regardless of the RAS isoform and tumor type. Additionally, our findings offer a mechanistic explanation for the increased frequency of RASQ61X mutations as a secondary resistance mechanism against EGFR inhibition in colorectal cancer.

Significance: RAS inhibition in multiple tumor types reveals the difference between G12 mutants and Q61 mutants in their cooperation with upstream regulators and downstream effectors to promote oncogenic signaling. Our findings provide the rationale for combinatorial approaches and contribute to explaining the nonuniform distribution of RAS mutations, de novo and at resistance.

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Conflict of interest statement

S.A. reports personal fees from MSD Italia and a patent (international PCT patent application No. WO 2023/199255 and Italian patent application No. 102022000007535) outside the submitted work. A.B. reports receipt of grants/research support from Neophore, AstraZeneca and Boehringer Ingelheim and honoraria/consultation fees from Guardant Health and Inivata. A.B. is a stock shareholder of Neophore and Kither Biotech. A.B. is an advisory board member for Inivata, Neophore, Roche/Genentech. S.W.L. declares competing interest outside consultancy and equity for Oric Pharmaceuticals, Blueprint Medicines, Mirimus, Senecea Therapeutics, Faeth Therapeutics and PMV Pharmaceuticals; and outside consultancy (no equity) for Fate Therapeutics. J.W.Z. has received a Genentech imCORE grant from Genentech. R.Y. has served as an advisor for Array BioPharma/Pfizer, Mirati Therapeutics, Amgen, and Revolution Medicines, received a speaker’s honorarium from Zai Lab, and has received research support to her institution from Array BioPharma/Pfizer, Boehringer Ingelheim, Boundless Bio, Mirati Therapeutics, and Daiichi Sankyo. S.E.K. has ownership interest in Lutris, Iylon, Frontier Medicines, Xilis, Navire and is a consultant for Genentech, EMD Serono, Merck, Holy Stone Healthcare, Novartis, Lilly, Boehringer Ingelheim, AstraZeneca/MedImmune, Bayer Health, Redx Pharma, Ipsen, HalioDx, Lutris, Jacobio, Pfizer, Repare Therapeutics, Inivata, GlaxoSmithKline, Jazz Pharmaceuticals, Iylon, Xilis, Abbvie, Amal Therapeutics, Gilead Sciences, Mirati Therapeutics, Flame Biosciences, Servier, Carina Biotech, Bicara Therapeutics, Endeavor BioMedicines, Numab, Johnson & Johnson/Janssen, Genomic Health, Frontier Medicines, Replimune, Taiho Pharmaceutical, Cardiff Oncology, Ono Pharmaceutical, Bristol-Myers Squibb-Medarex, Amgen, Tempus, Foundation Medicine, Harbinger Oncology, Inc, Takeda, CureTeq, Zentalis, Black Stone Therapeutics, NeoGenomics Laboratories, Accademia Nazionale Di Medicina, Tachyon Therapeutics and receives research funding from Sanofi, Biocartis, Guardant Health, Array BioPharma, Genentech/Roche, EMD Serono, MedImmune, Novartis, Amgen, Lilly, Daiichi Sankyo. N.R. is on the scientific advisory board (SAB) and owns equity in Beigene, Zai Labs, MapKure, Ribon and Effector. N.R. is also on the SAB of Astra Zeneca and Chugai and a past SAB member of Novartis, Millennium-Takeda, Kura, and Araxes. N.R. is a consultant to Revolution Medicines, Tarveda, Array-Pfizer, Boehringer-Ingelheim and Eli Lilly. He receives research funding from Revolution Medicines, AstraZeneca, Array Pfizer and Boehringer-Ingelheim and owns equity in Kura Oncology and Fortress. S.M. has received research support to her institution from AstraZeneca and she is a co-founder and scientific advisor of Bionseek srl. No conflicts of interest were reported by the other Authors.

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