Comprehensive Study of the Clinical Phenotype of Germline BAP1 Variant-Carrying Families Worldwide

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

doi:10.1093/jnci/djy171

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tumor diagnoses, and information on BAP1 immunohistochemistry or loss of somatic heterozygosity on 106 published and 75 unpublished BAP1 germline variant-positive families worldwide to better characterize the genotypes and phenotypes associated with the BAP1-TPDS.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.