Exome sequencing identifies breast cancer susceptibility genes and defines the contribution of coding variants to breast cancer risk
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Published:2023-08-17
Issue:9
Volume:55
Page:1435-1439
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ISSN:1061-4036
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Container-title:Nature Genetics
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language:en
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Short-container-title:Nat Genet
Author:
Wilcox Naomi, Dumont Martine, González-Neira Anna, Carvalho Sara, Joly Beauparlant Charles, Crotti Marco, Luccarini Craig, Soucy Penny, Dubois Stéphane, Nuñez-Torres Rocio, Pita Guillermo, Gardner Eugene J.ORCID, Dennis Joe, Alonso M. Rosario, Álvarez Nuria, Baynes Caroline, Collin-Deschesnes Annie Claude, Desjardins Sylvie, Becher HeikoORCID, Behrens SabineORCID, Bolla Manjeet K., Castelao Jose E., Chang-Claude Jenny, Cornelissen Sten, Dörk ThiloORCID, Engel Christoph, Gago-Dominguez Manuela, Guénel PascalORCID, Hadjisavvas Andreas, Hahnen Eric, Hartman Mikael, Herráez Belén, Tan Benita Kiat-Tee, Tan Veronique Kiak Mien, Tan Su-Ming, Lim Geok Hoon, Tan Ern Yu, Ho Peh Joo, Khng Alexis Jiaying, Jung Audrey, Keeman Renske, Kiechle Marion, Li JingmeiORCID, Loizidou Maria A., Lush MichaelORCID, Michailidou KyriakiORCID, Panayiotidis Mihalis I.ORCID, Sim XuelingORCID, Teo Soo HwangORCID, Tyrer Jonathan P.ORCID, van der Kolk Lizet E., Wahlström Cecilia, Wang QinORCID, Perry John R. B.ORCID, Benitez Javier, Schmidt Marjanka K.ORCID, Schmutzler Rita K., Pharoah Paul D. P.ORCID, Droit Arnaud, Dunning Alison M.ORCID, Kvist AndersORCID, Devilee PeterORCID, Easton Douglas F.ORCID, Simard JacquesORCID,
Abstract
AbstractLinkage and candidate gene studies have identified several breast cancer susceptibility genes, but the overall contribution of coding variation to breast cancer is unclear. To evaluate the role of rare coding variants more comprehensively, we performed a meta-analysis across three large whole-exome sequencing datasets, containing 26,368 female cases and 217,673 female controls. Burden tests were performed for protein-truncating and rare missense variants in 15,616 and 18,601 genes, respectively. Associations between protein-truncating variants and breast cancer were identified for the following six genes at exome-wide significance (P < 2.5 × 10−6): the five known susceptibility genes ATM, BRCA1, BRCA2, CHEK2 and PALB2, together with MAP3K1. Associations were also observed for LZTR1, ATRIP and BARD1 with P < 1 × 10−4. Associations between predicted deleterious rare missense or protein-truncating variants and breast cancer were additionally identified for CDKN2A at exome-wide significance. The overall contribution of coding variants in genes beyond the previously known genes is estimated to be small.
Funder
Genome Canada EC | Horizon 2020 Framework Programme Wellcome Trust Cancer Research UK RCUK | Medical Research Council
Publisher
Springer Science and Business Media LLC
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