Sorafenib Plus Irinotecan Combination in Patients With RAS-mutated Metastatic Colorectal Cancer Refractory To Standard Combined Chemotherapies: A Multicenter, Randomized Phase 2 Trial (NEXIRI-2/PRODIGE 27)

No treatment option was available for patients with RAS-mutated (RASmt) metastatic colorectal cancer (mCRC) who progress after standard combined chemotherapies at the time of the study. After promising results in phase II, the aim of the present NEXIRI-2/PRODIGE 27 trial was to assess the 2-month no...

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Veröffentlicht in:Clinical colorectal cancer 2020-12, Vol.19 (4), p.301-310.e1
Hauptverfasser: Samalin, Emmanuelle, Fouchardière, Christelle de la, Thézenas, Simon, Boige, Valérie, Senellart, Hélène, Guimbaud, Rosine, Taïeb, Julien, François, Eric, Galais, Marie-Pierre, Lièvre, Astrid, Seitz, Jean-François, Metges, Jean-Philippe, Bouché, Olivier, Boissière-Michot, Florence, Lopez-Crapez, Evelyne, Bibeau, Frédéric, Ho-Pun-Cheung, Alexandre, Ychou, Marc, Adenis, Antoine, Di Fiore, Frédéric, Mazard, Thibault
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Sprache:eng
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Zusammenfassung:No treatment option was available for patients with RAS-mutated (RASmt) metastatic colorectal cancer (mCRC) who progress after standard combined chemotherapies at the time of the study. After promising results in phase II, the aim of the present NEXIRI-2/PRODIGE 27 trial was to assess the 2-month non-progression rate for sorafenib (NEX) plus irinotecan (IRI), that is, NEXIRI, treatment. Patients with RASmt mCRC after failure of oxaliplatin, IRI, fluoropyrimidines, and bevacizumab were randomized between NEXIRI (IRI 120-180 mg/m2 intravenous, D1 = D15 plus oral NEX 400 mg twice a day) versus IRI (180 mg/m2) versus NEX. Primary endpoint was the 2-month non-progression rate. Secondary endpoints included progression-free and overall survival (PFS and OS), safety, and germline cyclin D1 (CCND1) rs9344 polymorphisms analyses. A total of 173 patients were included, 59 in NEXIRI, 57 in IRI, and 57 in NEX arms. The 2-month non-progression rate was 52.6% (95% confidence interval [CI]: 39%–66%), 21.4% (10%–33%), and 19.3% (9%–30%) for NEXIRI, IRI, and NEX. Median PFS was 3.6 (95% CI: 2–4.2), 1.7 (1.7–1.8), and 2 (1.8–2.3) months and the median OS was 7.2 (5.8–9.4), 6.3 (4.8–8), and 5.6 (3.9–7.7) months for NEXIRI, IRI, and NEX, respectively. For NEXIRI rs9344CCND1 A/A genotype patients, OS was 19.6 months (95% CI: 4.8–not reached). Main grade 3 toxicities included neutropenia, febrile neutropenia, diarrhea, hand-foot syndrome, and hypertension. In patients with RASmt mCRC who progressed after standard combined chemotherapies, the results of 2-month non-progression rate and median PFS in the NEXIRI arm were in favor of an increase of the time before progression. No treatment was available for patients with RAS-mutated (RASmt) metastatic colorectal cancer (mCRC) refractory to standard chemotherapies at the time of the study. A total of 173 patients with RASmt mCRC were randomized between NEXIRI (IRI + NEX), irinotecan (IRI), and sorafenib (NEX). The 2-month nonprogression disease rate was 52.6% [95% CI: 39%–66%], 21.4% [10%–33%], and 19.3% [9%–30%], respectively. NEXIRI combination can delay progression of RASmt mCRC.
ISSN:1533-0028
1938-0674
DOI:10.1016/j.clcc.2020.04.008