Description du projet
Un meilleur outil pour la prise en charge du cancer du pancréas
L’adénocarcinome canalaire pancréatique (ACP ou PDA pour «pancreatic ductal adenocarcinoma»), qui représente 90 % des cas de cancer du pancréas, est associé à un taux de mortalité élevé. Cependant, les recherches menées au cours des 30 dernières années étaient principalement axées sur la caractérisation et la compréhension des propriétés des cellules cancéreuses de PDA, tout en négligeant leur contexte cellulaire spécifique. Il est important de noter que le PDA est composé à 80 % de cellules non tumorales. Le projet S-Target-in-PANR du CER a démontré que le titrage sérique d’un candidat spécifique, PAP/REG3A, peut être un biomarqueur pour stratifier le PDA et optimiser la prise en charge des patients en prédisant la résécabilité. Le projet pBioStrat-for-PDA, financé par le CER, validera cette découverte à l’aide de cohortes robustes et de méthodes de test adaptées.
Objectif
With an overall 3-year survival rate of only ~6% together with an increased incidence pancreatic ductal adenocarcinoma (PDA), which represents 90% of pancreatic cancer, figures as the solid cancer with the worst prognosis. In trying to understand “the” reason for such negative outlook, one has to consider that the fundamental and clinical research conducted during the last 30 years has focused on characterizing and understanding the properties of the PDA cancer cells, neglecting the specific cellular context of those tumors. Indeed PDA consists of 80% of non-tumor cells. In the ERC Starting grant, S-Target-in-PANR, I conducted from 2011 to 2016 we took into account this specificity and analyzed the impact of this stromal compartment on PDA physiology. The discoveries and conceptual progresses obtained throughout the S-Target-in-PANR programme opened new potent improvements of PDA patients’ management. Among them, we revealed that one of the candidates, PAP/REG3A, was secreted by acinar cells from the peri-tumoral microenvironment to enhance peri-neural invasion ability of tumor cells. Interestingly, we demonstrated that PAP/REG3A titration in serum was a potent biomarker in order to stratify PDA and could lead to patients’ management optimization and more specifically to predict resectability.
This validation, using robust cohorts and adapted testing, constitutes the main goal of our ERC-PoC pBioStrat-for-PDA. Indeed, it will provide a powerful tool for clinicians in order to better determine the resectability of a tumor by taking into account its biological nature on top of the only clinical criteria used so far. As a consequence the use of a non-invasive PAP/REG3A serum level determination will improve patients’ managements by (1) shortening the delay to start palliative chemotherapy, (2) limiting unnecessary surgery with important mortality/morbidity and (3) improving their redirection to adapted clinical trials, as the one targeting JAK2/STAT3 signalling.
Champ scientifique
Programme(s)
Thème(s)
Régime de financement
ERC-POC - Proof of Concept GrantInstitution d’accueil
75654 Paris
France