Co-observation of germline pathogenic variants in breast cancer predisposition genes: Results from analysis of the BRIDGES sequencing dataset.

Davidson, AL; Michailidou, K; Parsons, MT; Fortuno, C; Bolla, MK; Wang, Q; Dennis, J; Naven, M; Abubakar, M; Ahearn, TU; Alonso, MR; Andrulis, IL; Antoniou, AC; Auvinen, P; Behrens, S; Bermisheva, MA; Bogdanova, NV; Bojesen, SE; Brüning, T; Byers, HJ; Camp, NJ; Campbell, A; Castelao, JE; Cessna, MH; Chang-Claude, J; Chanock, SJ; Chenevix-Trench, G; NBCS Collaborators,; Collée, JM; Czene, K; Dörk, T; Eriksson, M; Evans, DG; Fasching, PA; Figueroa, JD; Flyger, H; Gago-Dominguez, M; García-Closas, M; Glendon, G; González-Neira, A; Grassmann, F; Gronwald, J; Guénel, P; Hadjisavvas, A; Haeberle, L; Hall, P; Hamann, U; Hartman, M; Ho, PJ; Hooning, MJ; Hoppe, R; Howell, A; kConFab Investigators,; Jakubowska, A; Khusnutdinova, EK; Kristensen, VN; Li, J; Lim, J; Lindblom, A; Liu, J; Lophatananon, A; Mannermaa, A; Mavroudis, DA; Mensenkamp, AR; Milne, RL; Muir, KR; Newman, WG; Obi, N; Panayiotidis, MI; Park, SK; Park-Simon, T-W; Peterlongo, P; Radice, P; Rashid, MU; Rhenius, V; Saloustros, E; Sawyer, EJ; Schmidt, MK; Seibold, P; Shah, M; Southey, MC; Teo, SH; Tomlinson, I; Torres, D; Truong, T; van de Beek, I; van der Hout, AH; Wendt, CC; Dunning, AM; Pharoah, PDP; Devilee, P; Easton, DF; James, PA; Spurdle, AB

Co-observation of germline pathogenic variants in breast cancer predisposition genes: Results from analysis of the BRIDGES sequencing dataset.

Davidson, AL Michailidou, K Parsons, MT Fortuno, C Bolla, MK Wang, Q Dennis, J Naven, M Abubakar, M Ahearn, TU Alonso, MR Andrulis, IL Antoniou, AC Auvinen, P Behrens, S Bermisheva, MA Bogdanova, NV Bojesen, SE Brüning, T Byers, HJ Camp, NJ Campbell, A Castelao, JE Cessna, MH Chang-Claude, J Chanock, SJ Chenevix-Trench, G NBCS Collaborators, Collée, JM Czene, K Dörk, T Eriksson, M Evans, DG Fasching, PA Figueroa, JD Flyger, H Gago-Dominguez, M García-Closas, M Glendon, G González-Neira, A Grassmann, F Gronwald, J Guénel, P Hadjisavvas, A Haeberle, L Hall, P Hamann, U Hartman, M Ho, PJ Hooning, MJ Hoppe, R Howell, A kConFab Investigators, Jakubowska, A Khusnutdinova, EK Kristensen, VN Li, J Lim, J Lindblom, A Liu, J Lophatananon, A Mannermaa, A Mavroudis, DA Mensenkamp, AR Milne, RL Muir, KR Newman, WG Obi, N Panayiotidis, MI Park, SK Park-Simon, T-W Peterlongo, P Radice, P Rashid, MU Rhenius, V Saloustros, E Sawyer, EJ Schmidt, MK Seibold, P Shah, M Southey, MC Teo, SH Tomlinson, I Torres, D Truong, T van de Beek, I van der Hout, AH Wendt, CC Dunning, AM Pharoah, PDP Devilee, P Easton, DF James, PA Spurdle, AB

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Publisher:: Elsevier
Publication Type:: Journal Article
Citation:: Am J Hum Genet, 2024, 111, (9), pp. 2059-2069
Issue Date:: 2024-09-05

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Field	Value	Language
dc.contributor.author	Davidson, AL
dc.contributor.author	Michailidou, K
dc.contributor.author	Parsons, MT
dc.contributor.author	Fortuno, C
dc.contributor.author	Bolla, MK
dc.contributor.author	Wang, Q
dc.contributor.author	Dennis, J
dc.contributor.author	Naven, M
dc.contributor.author	Abubakar, M
dc.contributor.author	Ahearn, TU
dc.contributor.author	Alonso, MR
dc.contributor.author	Andrulis, IL
dc.contributor.author	Antoniou, AC
dc.contributor.author	Auvinen, P
dc.contributor.author	Behrens, S
dc.contributor.author	Bermisheva, MA
dc.contributor.author	Bogdanova, NV
dc.contributor.author	Bojesen, SE
dc.contributor.author	Brüning, T
dc.contributor.author	Byers, HJ
dc.contributor.author	Camp, NJ
dc.contributor.author	Campbell, A
dc.contributor.author	Castelao, JE
dc.contributor.author	Cessna, MH
dc.contributor.author	Chang-Claude, J
dc.contributor.author	Chanock, SJ
dc.contributor.author	Chenevix-Trench, G
dc.contributor.author	NBCS Collaborators,
dc.contributor.author	Collée, JM
dc.contributor.author	Czene, K
dc.contributor.author	Dörk, T
dc.contributor.author	Eriksson, M
dc.contributor.author	Evans, DG
dc.contributor.author	Fasching, PA
dc.contributor.author	Figueroa, JD
dc.contributor.author	Flyger, H
dc.contributor.author	Gago-Dominguez, M
dc.contributor.author	García-Closas, M
dc.contributor.author	Glendon, G
dc.contributor.author	González-Neira, A
dc.contributor.author	Grassmann, F
dc.contributor.author	Gronwald, J
dc.contributor.author	Guénel, P
dc.contributor.author	Hadjisavvas, A
dc.contributor.author	Haeberle, L
dc.contributor.author	Hall, P
dc.contributor.author	Hamann, U
dc.contributor.author	Hartman, M
dc.contributor.author	Ho, PJ
dc.contributor.author	Hooning, MJ
dc.contributor.author	Hoppe, R
dc.contributor.author	Howell, A
dc.contributor.author	kConFab Investigators,
dc.contributor.author	Jakubowska, A
dc.contributor.author	Khusnutdinova, EK
dc.contributor.author	Kristensen, VN
dc.contributor.author	Li, J
dc.contributor.author	Lim, J
dc.contributor.author	Lindblom, A
dc.contributor.author	Liu, J
dc.contributor.author	Lophatananon, A
dc.contributor.author	Mannermaa, A
dc.contributor.author	Mavroudis, DA
dc.contributor.author	Mensenkamp, AR
dc.contributor.author	Milne, RL
dc.contributor.author	Muir, KR
dc.contributor.author	Newman, WG
dc.contributor.author	Obi, N
dc.contributor.author	Panayiotidis, MI
dc.contributor.author	Park, SK
dc.contributor.author	Park-Simon, T-W
dc.contributor.author	Peterlongo, P
dc.contributor.author	Radice, P
dc.contributor.author	Rashid, MU
dc.contributor.author	Rhenius, V
dc.contributor.author	Saloustros, E
dc.contributor.author	Sawyer, EJ
dc.contributor.author	Schmidt, MK
dc.contributor.author	Seibold, P
dc.contributor.author	Shah, M
dc.contributor.author	Southey, MC
dc.contributor.author	Teo, SH
dc.contributor.author	Tomlinson, I
dc.contributor.author	Torres, D
dc.contributor.author	Truong, T
dc.contributor.author	van de Beek, I
dc.contributor.author	van der Hout, AH
dc.contributor.author	Wendt, CC
dc.contributor.author	Dunning, AM
dc.contributor.author	Pharoah, PDP
dc.contributor.author	Devilee, P
dc.contributor.author	Easton, DF
dc.contributor.author	James, PA
dc.contributor.author	Spurdle, AB
dc.date.accessioned	2025-04-02T06:06:15Z
dc.date.available	2024-07-03
dc.date.available	2025-04-02T06:06:15Z
dc.date.issued	2024-09-05
dc.identifier.citation	Am J Hum Genet, 2024, 111, (9), pp. 2059-2069
dc.identifier.issn	0002-9297
dc.identifier.issn	1537-6605
dc.identifier.uri	http://hdl.handle.net/10453/186501
dc.description.abstract	Co-observation of a gene variant with a pathogenic variant in another gene that explains the disease presentation has been designated as evidence against pathogenicity for commonly used variant classification guidelines. Multiple variant curation expert panels have specified, from consensus opinion, that this evidence type is not applicable for the classification of breast cancer predisposition gene variants. Statistical analysis of sequence data for 55,815 individuals diagnosed with breast cancer from the BRIDGES sequencing project was undertaken to formally assess the utility of co-observation data for germline variant classification. Our analysis included expected loss-of-function variants in 11 breast cancer predisposition genes and pathogenic missense variants in BRCA1, BRCA2, and TP53. We assessed whether co-observation of pathogenic variants in two different genes occurred more or less often than expected under the assumption of independence. Co-observation of pathogenic variants in each of BRCA1, BRCA2, and PALB2 with the remaining genes was less frequent than expected. This evidence for depletion remained after adjustment for age at diagnosis, study design (familial versus population-based), and country. Co-observation of a variant of uncertain significance in BRCA1, BRCA2, or PALB2 with a pathogenic variant in another breast cancer gene equated to supporting evidence against pathogenicity following criterion strength assignment based on the likelihood ratio and showed utility in reclassification of missense BRCA1 and BRCA2 variants identified in BRIDGES. Our approach has applicability for assessing the value of co-observation as a predictor of variant pathogenicity in other clinical contexts, including for gene-specific guidelines developed by ClinGen Variant Curation Expert Panels.
dc.format	Print-Electronic
dc.language	eng
dc.publisher	Elsevier
dc.relation.ispartof	Am J Hum Genet
dc.relation.isbasedon	10.1016/j.ajhg.2024.07.004
dc.rights	info:eu-repo/semantics/restrictedAccess
dc.subject	06 Biological Sciences, 11 Medical and Health Sciences
dc.subject.classification	Genetics & Heredity
dc.subject.classification	31 Biological sciences
dc.subject.classification	32 Biomedical and clinical sciences
dc.subject.classification	42 Health sciences
dc.subject.mesh	Humans
dc.subject.mesh	Breast Neoplasms
dc.subject.mesh	Genetic Predisposition to Disease
dc.subject.mesh	Germ-Line Mutation
dc.subject.mesh	Female
dc.subject.mesh	BRCA2 Protein
dc.subject.mesh	BRCA1 Protein
dc.subject.mesh	Fanconi Anemia Complementation Group N Protein
dc.subject.mesh	Middle Aged
dc.subject.mesh	Mutation, Missense
dc.subject.mesh	Adult
dc.subject.mesh	Tumor Suppressor Protein p53
dc.subject.mesh	Humans
dc.subject.mesh	Breast Neoplasms
dc.subject.mesh	Genetic Predisposition to Disease
dc.subject.mesh	BRCA1 Protein
dc.subject.mesh	BRCA2 Protein
dc.subject.mesh	Germ-Line Mutation
dc.subject.mesh	Mutation, Missense
dc.subject.mesh	Adult
dc.subject.mesh	Middle Aged
dc.subject.mesh	Female
dc.subject.mesh	Tumor Suppressor Protein p53
dc.subject.mesh	Fanconi Anemia Complementation Group N Protein
dc.subject.mesh	Humans
dc.subject.mesh	Breast Neoplasms
dc.subject.mesh	Genetic Predisposition to Disease
dc.subject.mesh	Germ-Line Mutation
dc.subject.mesh	Female
dc.subject.mesh	BRCA2 Protein
dc.subject.mesh	BRCA1 Protein
dc.subject.mesh	Fanconi Anemia Complementation Group N Protein
dc.subject.mesh	Middle Aged
dc.subject.mesh	Mutation, Missense
dc.subject.mesh	Adult
dc.subject.mesh	Tumor Suppressor Protein p53
dc.title	Co-observation of germline pathogenic variants in breast cancer predisposition genes: Results from analysis of the BRIDGES sequencing dataset.
dc.type	Journal Article
utslib.citation.volume	111
utslib.location.activity	United States
utslib.for	06 Biological Sciences
utslib.for	11 Medical and Health Sciences
pubs.organisational-group	University of Technology Sydney
pubs.organisational-group	University of Technology Sydney/Faculty of Engineering and Information Technology
pubs.organisational-group	University of Technology Sydney/Faculty of Engineering and Information Technology/School of Biomedical Engineering
utslib.copyright.status	recently_added	*
dc.date.updated	2025-04-02T06:06:12Z
pubs.issue	9
pubs.publication-status	Published
pubs.volume	111
utslib.citation.issue	9

Abstract:

Co-observation of a gene variant with a pathogenic variant in another gene that explains the disease presentation has been designated as evidence against pathogenicity for commonly used variant classification guidelines. Multiple variant curation expert panels have specified, from consensus opinion, that this evidence type is not applicable for the classification of breast cancer predisposition gene variants. Statistical analysis of sequence data for 55,815 individuals diagnosed with breast cancer from the BRIDGES sequencing project was undertaken to formally assess the utility of co-observation data for germline variant classification. Our analysis included expected loss-of-function variants in 11 breast cancer predisposition genes and pathogenic missense variants in BRCA1, BRCA2, and TP53. We assessed whether co-observation of pathogenic variants in two different genes occurred more or less often than expected under the assumption of independence. Co-observation of pathogenic variants in each of BRCA1, BRCA2, and PALB2 with the remaining genes was less frequent than expected. This evidence for depletion remained after adjustment for age at diagnosis, study design (familial versus population-based), and country. Co-observation of a variant of uncertain significance in BRCA1, BRCA2, or PALB2 with a pathogenic variant in another breast cancer gene equated to supporting evidence against pathogenicity following criterion strength assignment based on the likelihood ratio and showed utility in reclassification of missense BRCA1 and BRCA2 variants identified in BRIDGES. Our approach has applicability for assessing the value of co-observation as a predictor of variant pathogenicity in other clinical contexts, including for gene-specific guidelines developed by ClinGen Variant Curation Expert Panels.

Please use this identifier to cite or link to this item:

http://hdl.handle.net/10453/186501