A Phase Ia/b study of MEK1/2 inhibitor binimetinib with MET inhibitor crizotinib in patients with <i>RAS</i> mutant advanced colorectal cancer (MErCuRIC)

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Authors	AROLDI Francesca ELEZ Elena ANDRE Thierry PERKINS Geraldine PRENEN Hans POPOVICI Vlad GALLAGHER Peter HOULDEN Jennifer COLLINS Linda ROBERTS Corran ROLFO Christian DI NICOLANTONIO Federica GRAYSON Margaret BOYD Ruth BETTENS Karolien DELFAVERO Jurgen COYLE Victoria LAWLER Mark KHAWAJA Hajrah LAURENT-PUIG Pierre SALTO-TELLEZ Manuel MAUGHAN Tim S. TABERNERO Josep ADAMS Richard JONES Robert HENNESSY Bryan T. BARDELLI Alberto PEETERS Marc MIDDLETON Mark R. WILSON Richard H. VAN SCHAEYBROECK Sandra
Year of publication	2025
Type	Article in Periodical
Magazine / Source	BMC Cancer
MU Faculty or unit	Faculty of Science
Citation
web	https://bmccancer.biomedcentral.com/articles/10.1186/s12885-025-14068-1
Doi	http://dx.doi.org/10.1186/s12885-025-14068-1
Keywords	RAS mutant; Colorectal cancer; Phase I; Binimetinib; Crizotinib; Pharmacokinetics; Pharmacodynamics; MET biomarker; CtDNA
Attached files	2507624.pdf
Description	Background Targeting RAS mutant (MT) colorectal cancer (CRC) remains a difficult challenge, mainly due to the pervasiveness of RAS/MEK-mediated feedback loops. Preclinical studies identified MET/STAT3 as an important mediator of resistance to KRAS-MEK1/2 blockade in RASMT CRC. This dose escalation/expansion study assessed safety and initial efficacy of the MEK1/2 inhibitor binimetinib with MET inhibitor crizotinib in RASMT advanced CRC patients. Methods In the dose escalation phase, patients with advanced solid tumours received binimetinib with crizotinib, using a rolling- 6 design to determine the maximum tolerable dose (MTD) and safety/tolerability. A subsequent dose expansion in RASMT CRC patients assessed treatment response. Blood samples for pharmacokinetics, MET biomarker and ctDNA analyses, and skin/tumour biopsies for pharmacodynamics, c-MET immunohistochemistry (IHC), MET in situ hybridisation (ISH) and MET DNA-ISH analyses were collected. Results Twenty patients were recruited in 3 cohorts in the dose escalation. The MTD was binimetinib 30 mg B.D, days 1-21 every 28 days, with crizotinib 250 mg O.D continuously. Dose-limiting toxicities included grade >= 3 transaminitis, creatinine phosphokinase increases and fatigue. Thirty-six RASMT metastatic CRC patients were enrolled in the dose expansion. Pharmacokinetic and pharmacodynamic parameters showed evidence of target engagement. Across the entire study, the most frequent treatment-related adverse events (TR-AE) were rash (80.4%), fatigue (53.4%) and diarrhoea (51.8%) with grade >= 3 TR-AE occurring in 44.6%. Best clinical response within the RASMT CRC cohort was stable disease in seven patients (24%). Tumour MET super-expression (IHC H-score > 180 and MET ISH + 3) was observed in 7 patients (24.1%), with MET-amplification only present in 1 of these patients. This patient discontinued treatment early during cycle 1 due to toxicity. Patients with high baseline RASMT allele frequency had a significant shorter median overall survival compared with that seen for patients with low baseline KRASMT allele frequency. Conclusions Combination binimetinib/crizotinib showed a poor tolerability with no objective responses observed in RASMT advanced CRC patients.EudraCT-Number: 2014-000463 - 40 (20/06/2014: A Sequential Phase I study of MEK1/2 inhibitors PD- 0325901 or Binimetinib combined with cMET inhibitor Crizotinib in RAS Mutant and RAS Wild Type with aberrant c-MET).
Related projects:	MErCuRIC - A Phase Ib/II study of MEK1/2 inhibitor PD--0325901 with cMET inhibitor PF--02341066 in KRASMT and KRASWT (with aberrant c--MET) Colorectal Cancer Patients