The PENDOR study: establishment of a panel of patient-derived tumor organoids from endometrial cancer to assess efficacy of PARP inhibitors
Gwenn Le Gall,
François Cherifi,
Jordane Divoux,
Romane Florent,
François Christy,
Alexandra Leconte,
Chankannira San,
Amélie Devillers,
Guillaume Desmartin,
Lucie Lecouflet,
Bénédicte Clarisse,
Samantha Ballesta,
Lucie Thorel,
Brice Dubois,
Valentin Harter,
Nathalie Rousseau,
Léopold Gaichies,
Sandrine Martin-Françoise,
Jean-François Le Brun,
Enora Dolivet,
Roman Rouzier,
Corinne Jeanne,
Cécile Blanc-Fournier,
Martin Figeac,
Raphaël Leman,
Laurent Castera,
Laurent Poulain,
Louis-Bastien Weiswald,
Florence Joly
Affiliations
Gwenn Le Gall
INSERM U1086 ANTICIPE (Interdisciplinary Research Unit for Cancers Prevention and Treatment), BioTICLA Laboratory (Precision Medicine for Ovarian Cancers), Université de Caen Normandie
François Cherifi
Clinical Research Department, Comprehensive Cancer Center François Baclesse, UNICANCER
Jordane Divoux
INSERM U1086 ANTICIPE (Interdisciplinary Research Unit for Cancers Prevention and Treatment), BioTICLA Laboratory (Precision Medicine for Ovarian Cancers), Université de Caen Normandie
Romane Florent
ORGAPRED core facility, US PLATON, Université de Caen Normandie
François Christy
Clinical Research Department, Comprehensive Cancer Center François Baclesse, UNICANCER
Alexandra Leconte
Clinical Research Department, Comprehensive Cancer Center François Baclesse, UNICANCER
Chankannira San
Clinical Research Department, Comprehensive Cancer Center François Baclesse, UNICANCER
Amélie Devillers
Clinical Research Department, Comprehensive Cancer Center François Baclesse, UNICANCER
Guillaume Desmartin
Comprehensive Cancer Center François Baclesse, UNICANCER
Lucie Lecouflet
Comprehensive Cancer Center François Baclesse, UNICANCER
Bénédicte Clarisse
Clinical Research Department, Comprehensive Cancer Center François Baclesse, UNICANCER
Samantha Ballesta
Plateforme 3D-ONCO, Inserm U1052, CNRS UMR5286, Centre de Recherche en Cancérologie de Lyon (CRCL) , Université Claude Bernard Lyon 1
Lucie Thorel
INSERM U1086 ANTICIPE (Interdisciplinary Research Unit for Cancers Prevention and Treatment), BioTICLA Laboratory (Precision Medicine for Ovarian Cancers), Université de Caen Normandie
Brice Dubois
North-West Canceropole Data Center, Comprehensive Cancer Center François Baclesse, UNICANCER
Valentin Harter
North-West Canceropole Data Center, Comprehensive Cancer Center François Baclesse, UNICANCER
Nathalie Rousseau
Biological Resource Center ‘Tumorotheque de Caen Basse-Normandie’, IRCBN Institut Régional du Cancer Basse Normandie
Léopold Gaichies
Department of Surgery, Comprehensive Cancer Center François Baclesse, UNICANCER
Sandrine Martin-Françoise
Department of Surgery, Comprehensive Cancer Center François Baclesse, UNICANCER
Jean-François Le Brun
Department of Surgery, Comprehensive Cancer Center François Baclesse, UNICANCER
Enora Dolivet
INSERM U1086 ANTICIPE (Interdisciplinary Research Unit for Cancers Prevention and Treatment), BioTICLA Laboratory (Precision Medicine for Ovarian Cancers), Université de Caen Normandie
Roman Rouzier
Department of Surgery, Comprehensive Cancer Center François Baclesse, UNICANCER
Corinne Jeanne
Department of Biopathology, Comprehensive Cancer Center François Baclesse, UNICANCER
Cécile Blanc-Fournier
INSERM U1086 ANTICIPE (Interdisciplinary Research Unit for Cancers Prevention and Treatment), BioTICLA Laboratory (Precision Medicine for Ovarian Cancers), Université de Caen Normandie
Martin Figeac
US 41 - UAR 2014 - PLBS,CNRS, Inserm, CHU Lille, Institut Pasteur de Lille, University of Lille
Raphaël Leman
Department of Cancer Biology and Genetics, U1245 “Cancer and brain genomics”, Comprehensive Cancer Center François Baclesse, UNICANCER
Laurent Castera
Department of Cancer Biology and Genetics, U1245 “Cancer and brain genomics”, Comprehensive Cancer Center François Baclesse, UNICANCER
Laurent Poulain
INSERM U1086 ANTICIPE (Interdisciplinary Research Unit for Cancers Prevention and Treatment), BioTICLA Laboratory (Precision Medicine for Ovarian Cancers), Université de Caen Normandie
Louis-Bastien Weiswald
INSERM U1086 ANTICIPE (Interdisciplinary Research Unit for Cancers Prevention and Treatment), BioTICLA Laboratory (Precision Medicine for Ovarian Cancers), Université de Caen Normandie
Florence Joly
Clinical Research Department, Comprehensive Cancer Center François Baclesse, UNICANCER
Abstract Background Combination of chemotherapy and immunotherapy is the current standard of care for advanced endometrial cancer. However, survival outcome remains poor, highlighting the urgent need for new treatments and reliable tools to identify patients who will benefit from them. Patient-Derived Tumor Organoids (PDTO) are three-dimensional structures established from patient tumors, and are closely mimicking the features of the tumor of origin. Moreover, more and more evidences show that PTDOs hold promises as predictive tools for the response to treatment of patients. Method The PENDOR study is a monocentric observational study designed to assess the feasibility of generating and testing PDTOs derived from endometrial cancer for evaluating treatment sensitivity. PDTOS will be established from surgical specimens not required for anatomopathological diagnosis. Tumor cells will be dissociated, embedded in extracellular matrix, and cultured in a medium supplemented with growth factors and signaling pathways inhibitors. Molecular and histological analyses will be conducted to validate the resemblance of PDTO to the original tumor. Response of PDTO to conventional chemotherapy and PARP inhibitors will be evaluated and compared to clinical response and to the results of an academic HRD test Genomic Instability Scar (GIScar), respectively, to assess their predictive value. Discussion This pilot study aims to validate the feasibility to develop PDTOs from endometrial cancer from patients who will undergo surgical resection. We aim to provide a proof of concept regarding the predictive value of these models for their potential application into routine clinical practice as part of precision medicine. This approach could therefore facilitate the identification of patients who could benefit from PARP inhibitors. Trial registration This clinical trial (N°ID-RCB: 2024-A01206-41) has been validated by local research ethic committee on July 16th 2024 and registered at ClinicalTrials.gov with the identifier NCT06603506 on September 6th 2024, version 1.
