Comprehensive Study of the Clinical Phenotype of Germline BAP1 Variant-Carrying Families Worldwide
- Creators
- Walpole, Sebastian
- Pritchard, Antonia L
- Cebulla, Colleen M
- Pilarski, Robert
- Stautberg, Meredith
- Davidorf, Frederick H
- de la Fouchardière, Arnaud
- Cabaret, Odile
- Golmard, Lisa
- Stoppa-Lyonnet, Dominique
- Garfield, Erin
- Njauw, Ching-Ni
- Cheung, Mitchell
- Turunen, Joni A
- Repo, Pauliina
- Järvinen, Reetta-Stiina
- van Doorn, Remco
- Jager, Martine J
- Luyten, Gregorius P M
- Marinkovic, Marina
- Chau, Cindy
- Potrony, Miriam
- Höiom, Veronica
- Helgadottir, Hildur
- Pastorino, Lorenza
- Bruno, William
- Andreotti, Virginia
- Dalmasso, Bruna
- Ciccarese, Giulia
- Queirolo, Paola
- Mastracci, Luca
- Wadt, Karin
- Kiilgaard, Jens Folke
- Speicher, Michael R
- van Poppelen, Natasha
- Kilic, Emine
- Al-Jamal, Rana'a T
- Dianzani, Irma
- BETTI, MARTA
- Bergmann, Carsten
- Santagata, Sandro
- Dahiya, Sonika
- Taibjee, Saleem
- Burke, Jo
- Poplawski, Nicola
- O'Shea, Sally J
- Newton-Bishop, Julia
- Adlard, Julian
- Adams, David J
- Lane, Anne-Marie
- Kim, Ivana
- Klebe, Sonja
- Racher, Hilary
- Harbour, J William
- Nickerson, Michael L
- Murali, Rajmohan
- Palmer, Jane M
- Howlie, Madeleine
- Symmons, Judith
- Hamilton, Hayley
- Warrier, Sunil
- Glasson, William
- Johansson, Peter
- Robles-Espinoza, Carla Daniela
- Ossio, Raul
- de Klein, Annelies
- Puig, Susana
- Ghiorzo, Paola
- Nielsen, Maartje
- Kivelä, Tero T
- Tsao, Hensin
- Testa, Joseph R
- Gerami, Pedram
- Stern, Marc-Henri
- Paillerets, Brigitte Bressac-de
- Abdel-Rahman, Mohamed H
- Hayward, Nicholas K
- Others:
- Walpole, Sebastian
- Pritchard, Antonia L
- Cebulla, Colleen M
- Pilarski, Robert
- Stautberg, Meredith
- Davidorf, Frederick H
- de la Fouchardière, Arnaud
- Cabaret, Odile
- Golmard, Lisa
- Stoppa-Lyonnet, Dominique
- Garfield, Erin
- Njauw, Ching-Ni
- Cheung, Mitchell
- Turunen, Joni A
- Repo, Pauliina
- Järvinen, Reetta-Stiina
- van Doorn, Remco
- Jager, Martine J
- Luyten, Gregorius P M
- Marinkovic, Marina
- Chau, Cindy
- Potrony, Miriam
- Höiom, Veronica
- Helgadottir, Hildur
- Pastorino, Lorenza
- Bruno, William
- Andreotti, Virginia
- Dalmasso, Bruna
- Ciccarese, Giulia
- Queirolo, Paola
- Mastracci, Luca
- Wadt, Karin
- Kiilgaard, Jens Folke
- Speicher, Michael R
- van Poppelen, Natasha
- Kilic, Emine
- Al-Jamal, Rana'a T
- Dianzani, Irma
- Betti, Marta
- Bergmann, Carsten
- Santagata, Sandro
- Dahiya, Sonika
- Taibjee, Saleem
- Burke, Jo
- Poplawski, Nicola
- O'Shea, Sally J
- Newton-Bishop, Julia
- Adlard, Julian
- Adams, David J
- Lane, Anne-Marie
- Kim, Ivana
- Klebe, Sonja
- Racher, Hilary
- Harbour, J William
- Nickerson, Michael L
- Murali, Rajmohan
- Palmer, Jane M
- Howlie, Madeleine
- Symmons, Judith
- Hamilton, Hayley
- Warrier, Sunil
- Glasson, William
- Johansson, Peter
- Robles-Espinoza, Carla Daniela
- Ossio, Raul
- de Klein, Annelie
- Puig, Susana
- Ghiorzo, Paola
- Nielsen, Maartje
- Kivelä, Tero T
- Tsao, Hensin
- Testa, Joseph R
- Gerami, Pedram
- Stern, Marc-Henri
- Paillerets, Brigitte Bressac-de
- Abdel-Rahman, Mohamed H
- Hayward, Nicholas K
Description
Background: The BRCA1-associated protein-1 (BAP1) tumor predisposition syndrome (BAP1-TPDS) is a hereditary tumor syndrome caused by germline pathogenic variants in BAP1 encoding a tumor suppressor associated with uveal melanoma, mesothelioma, cutaneous melanoma, renal cell carcinoma, and cutaneous BAP1-inactivated melanocytic tumors. However, the full spectrum of tumors associated with the syndrome is yet to be determined. Improved understanding of the BAP1-TPDS is crucial for appropriate clinical management of BAP1 germline variant carriers and their families, including genetic counseling and surveillance for new tumors. Methods: We collated germline variant status, tumor diagnoses, and information on BAP1 immunohistochemistry or loss of somatic heterozygosity on 106 published and 75 unpublished BAP1 germline variant-positive families worldwide to better characterize the genotypes and phenotypes associated with the BAP1-TPDS. Tumor spectrum and ages of onset were compared between missense and null variants. All statistical tests were two-sided. Results: The 181 families carried 140 unique BAP1 germline variants. The collated data confirmed the core tumor spectrum associated with the BAP1-TPDS and showed that some families carrying missense variants can exhibit this phenotype. A variety of noncore BAP1-TPDS -associated tumors were found in families of variant carriers. Median ages of onset of core tumor types were lower in null than missense variant carriers for all tumors combined (P < .001), mesothelioma (P < .001), cutaneous melanoma (P < .001), and nonmelanoma skin cancer (P < .001). Conclusions: This analysis substantially increases the number of pathogenic BAP1 germline variants and refines the phenotype. It highlights the need for a curated registry of germline variant carriers for proper assessment of the clinical phenotype of the BAP1-TPDS and pathogenicity of new variants, thus guiding management of patients and informing areas requiring further research.
Abstract
Background: The BRCA1-associated protein-1 (BAP1) tumor predisposition syndrome (BAP1-TPDS) is a hereditary tumor syndrome caused by germline pathogenic variants in BAP1 encoding a tumor suppressor associated with uveal melanoma, mesothelioma, cutaneous melanoma, renal cell carcinoma, and cutaneous BAP1-inactivated melanocytic tumors. However, the full spectrum of tumors associated with the syndrome is yet to be determined. Improved understanding of the BAP1-TPDS is crucial for appropriate clinical management of BAP1 germline variant carriers and their families, including genetic counseling and surveillance for new tumors. Methods: We collated germline variant status, tumor diagnoses, and information on BAP1 immunohistochemistry or loss of somatic heterozygosity on 106 published and 75 unpublished BAP1 germline variant-positive families worldwide to better characterize the genotypes and phenotypes associated with the BAP1-TPDS. Tumor spectrum and ages of onset were compared between missense and null variants. All statistical tests were two-sided. Results: The 181 families carried 140 unique BAP1 germline variants. The collated data confirmed the core tumor spectrum associated with the BAP1-TPDS and showed that some families carrying missense variants can exhibit this phenotype. A variety of noncore BAP1-TPDS -associated tumors were found in families of variant carriers. Median ages of onset of core tumor types were lower in null than missense variant carriers for all tumors combined (P < .001), mesothelioma (P < .001), cutaneous melanoma (P < .001), and nonmelanoma skin cancer (P < .001). Conclusions: This analysis substantially increases the number of pathogenic BAP1 germline variants and refines the phenotype. It highlights the need for a curated registry of germline variant carriers for proper assessment of the clinical phenotype of the BAP1-TPDS and pathogenicity of new variants, thus guiding management of patients and informing areas requiring further research.
Additional details
- URL
- http://hdl.handle.net/11567/935475
- URN
- urn:oai:iris.unige.it:11567/935475
- Origin repository
- UNIGE