Hyperthermic intraperitoneal chemotherapy in colorectal cancer.

Oliver M Fisher,Chris Brown,Jesus Esquivel,Stein G Larsen,Winston Liauw,Nayef A Alzahrani,David L Morris,Vahan Kepenekian,Isabelle Sourrouille,Frédéric Dumont,Jean-Jacques Tuech,Cécilia Ceribelli,Béranger Doussot,Olivia Sgarbura,Mohammed Alhosni,Francois Quenet,Olivier Glehen,Peter H Cashin,Kjersti Flatmark,Wilhelm Graf,Heikki Takala,Andrew M Lowy,Terence Chua,Joerg Pelz,Dario Baratti,Joel M Baumgartner,Richard Berri,Pedro Bretcha-Boix,Marcello Deraco,Guillermo Flores-Ayala,Alberto Gomez-Portilla,Santiago González-Moreno,Martin Goodman,Evgenia Halkia,Shigeki Kusamura,Mecker Moller,Guillaume Passot,Marc Pocard,George Salti,Armando Sardi,Maheswari Senthil,John Spilioitis,Juan Torres-Melero,Kiran Turaga,Jean-Marc Bereder,Jean-Louis Bernard,Naoual Bakrin,Sébastien Carrère,Julien Coget,Eddy Cotte,Olivier Facy,Maximiliano Gelli,François-Noël Gilly,Pablo Ortega-Deballon,Patrick Rat,Pascal Rousset,Emilie Thibaudeau,Delphine Vaudoyer

doi:10.1093/bjsopen/zrae017

Abstract

This study evaluated the efficacy of hyperthermic intraperitoneal chemotherapy (HIPEC) in colorectal cancer with peritoneal metastases (pmCRC) in a large international data set of patients. Patients with pmCRC from 39 centres who underwent cytoreductive surgery with HIPEC between 1991 and 2018 were selected and compared for the HIPEC protocols received-oxaliplatin-HIPEC versus mitomycin-HIPEC. Following analysis of crude data, propensity-score matching (PSM) and Cox-proportional hazard modelling were performed. Outcomes of interest were overall survival (OS), recurrence-free survival (RFS) and the HIPEC dose-response effects (high versus low dose, dose intensification and double drug protocols) on OS, RFS and 90-day morbidity. Furthermore, the impact of the treatment time period was assessed. Of 2760 patients, 2093 patients were included. Median OS was 43 months (95% c.i. 41 to 46 months) with a median RFS of 12 months (95% c.i. 12 to 13 months). The oxaliplatin-HIPEC group had an OS of 47 months (95% c.i. 42 to 53 months) versus 39 months (95% c.i. 36 to 43 months) in the mitomycin-HIPEC group (P = 0.002), aHR 0.77, 95% c.i. 0.67 to 0.90, P < 0.001. The OS benefit persisted after PSM of the oxaliplatin-HIPEC group and mitomycin-HIPEC group (48 months (95% c.i. 42 to 59 months) versus 40 months (95% c.i. 37 to 44 months)), P < 0.001, aHR 0.78 (95% c.i. 0.65 to 0.94), P = 0.009. Similarly, matched RFS was significantly higher for oxaliplatin-HIPEC versus others (13 months (95% c.i. 12 to 15 months) versus 11 months (95% c.i. 10 to 12 months, P = 0.02)). High-dose mitomycin-HIPEC protocols had similar OS compared to oxaliplatin-HIPEC. HIPEC dose intensification within each protocol resulted in improved survival. Oxaliplatin + irinotecan-HIPEC resulted in the most improved OS (61 months (95% c.i. 51 to 101 months)). Ninety-day mortality in both crude and PSM analysis was worse for mitomycin-HIPEC. There was no change in treatment effect depending on the analysed time period. Oxaliplatin-based HIPEC provided better outcomes compared to mitomycin-based HIPEC. High-dose mitomycin-HIPEC was similar to oxaliplatin-HIPEC. The 90-day mortality difference favours the oxaliplatin-HIPEC group. A trend for dose-response between low- and high-dose HIPEC was reported.

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