Pancreatic ductal adenocarcinoma in BRCA2 mutation carriers
- Louis de Mestier1,
- Jean-Baptiste Danset2,
- Cindy Neuzillet3,
- Vinciane Rebours1,
- Jérôme Cros4,
- Nadem Soufir5 and
- Pascal Hammel3⇑
- 1Department of Gastroenterology and Pancreatology, Beaujon Hospital, Paris 7 University, APHP, Clichy, France
- 2Department of Hepato-Gastroenterology, European Georges-Pompidou Hospital, APHP, Paris, France
- 3Department of Digestive Oncology, Beaujon Hospital, Paris 7 University, APHP, Clichy, France
- 4Department of Pathology, Beaujon Hospital, Paris 7 University, APHP, Clichy, France
- 5Department of Genetics, Bichat Hospital, Paris 7 University, APHP, Clichy, France
- Correspondence should be addressed to P Hammel; Email: pascal.hammel{at}aphp.fr
Abstract
Germline BRCA2 mutations are the first known cause of inherited (familial) pancreatic ductal adenocarcinoma (PDAC). This tumor is the third most frequent cancer in carriers of germline BRCA2 mutations, as it occurs in around 10% of BRCA2 families. PDAC is known as one of the most highly lethal cancers, mainly because of its chemoresistance and frequently late diagnosis. Based on recent developments in molecular biology, a subgroup of BRCA2-associated PDAC has been created, allowing screening, early surgical treatment and personalized systemic treatment. BRCA2 germline mutation carriers who have ≥1 first-degree relative, or ≥2 blood relatives with PDAC, should undergo screening and regular follow-up based on magnetic resonance imaging and endoscopic ultrasound. The goal of screening is to detect early invasive PDAC and advanced precancerous lesions suitable for a stepwise surgical complete (R0) resection. Increasing evidence on the molecular role of the BRCA2 protein in the homologous recombination of DNA damages suggest that BRCA2-related PDAC are sensitive to agents causing DNA cross-linking damage, such as platinum salts, and treatments targeting rescue DNA repair pathways, such as poly(ADP-ribose) polymerase inhibitors that are currently under investigation.
- Received 6 August 2016
- Accepted 10 August 2016
- Made available online as an Accepted Preprint 10 August 2016
- © 2016 Society for Endocrinology