Revolution Medicines (RVMD) Study result summary
Event summary combining transcript, slides, and related documents.
Study result summary
19 Jun, 2026Landmark clinical results and regulatory progress
RASolute 302 phase III trial showed daraxonrasib reduced risk of death by 60% vs. chemotherapy in metastatic pancreatic cancer, with median overall survival of 13.2 months vs. 6.6–6.7 months for chemotherapy, marking unprecedented outcomes in this setting.
Progression-free survival was doubled with daraxonrasib (7.3 vs 3.5 months in RAS G12; 7.2 vs 3.6 months in ITT), and objective response rate was nearly tripled compared to chemotherapy, with a manageable safety profile and improved patient-reported outcomes.
Regulatory submissions are underway, including a rolling NDA to the FDA under Breakthrough Therapy Designation, and an expanded access program is operational in the U.S. with high demand.
Plans for sequential international filings and a robust commercialization infrastructure are in place to support global launch upon approval.
Daraxonrasib significantly delayed time to deterioration in pain (median 9.2 vs 3.8 months; HR 0.51) and global health status/quality of life (median 5.7 vs 2.6 months; HR 0.60) compared to chemotherapy.
Study design and patient population
RASolute 302 enrolled 500 adults with metastatic pancreatic adenocarcinoma who had one prior chemotherapy regimen, randomized 1:1 to daraxonrasib or investigator's choice of chemotherapy.
Patients included those with a broad range of RAS variants, including RAS G12 mutations and wild-type RAS.
Dual primary endpoints were overall survival (OS) and progression-free survival (PFS) in the RAS G12 population; secondary endpoints included OS and PFS in the overall population, objective response rate, and patient-reported outcomes.
Subgroup analyses showed consistent benefit across age, sex, performance status, and mutational status.
Safety and tolerability
Daraxonrasib had a manageable safety profile with no unexpected findings and fewer grade ≥3 treatment-related adverse events (43.6%) compared to chemotherapy (57.5%).
Most common treatment-related adverse events were rash (14%) and stomatitis (12%) for daraxonrasib, and neutropenia, thrombocytopenia, fatigue, diarrhea, and neuropathy for chemotherapy.
Treatment discontinuation due to adverse events was lower with daraxonrasib (1.2%) than chemotherapy (11.2%).
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