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Aggregation tests identify new gene associations with breast cancer in populations with diverse ancestry

Aggregation tests identify new gene associations with breast cancer in populations with diverse ancestry
Aggregation tests identify new gene associations with breast cancer in populations with diverse ancestry

Background: Low-frequency variants play an important role in breast cancer (BC) susceptibility. Gene-based methods can increase power by combining multiple variants in the same gene and help identify target genes. Methods: We evaluated the potential of gene-based aggregation in the Breast Cancer Association Consortium cohorts including 83,471 cases and 59,199 controls. Low-frequency variants were aggregated for individual genes’ coding and regulatory regions. Association results in European ancestry samples were compared to single-marker association results in the same cohort. Gene-based associations were also combined in meta-analysis across individuals with European, Asian, African, and Latin American and Hispanic ancestry. Results: In European ancestry samples, 14 genes were significantly associated (q < 0.05) with BC. Of those, two genes, FMNL3 (P = 6.11 × 10 −6) and AC058822.1 (P = 1.47 × 10 −4), represent new associations. High FMNL3 expression has previously been linked to poor prognosis in several other cancers. Meta-analysis of samples with diverse ancestry discovered further associations including established candidate genes ESR1 and CBLB. Furthermore, literature review and database query found further support for a biologically plausible link with cancer for genes CBLB, FMNL3, FGFR2, LSP1, MAP3K1, and SRGAP2C. Conclusions: Using extended gene-based aggregation tests including coding and regulatory variation, we report identification of plausible target genes for previously identified single-marker associations with BC as well as the discovery of novel genes implicated in BC development. Including multi ancestral cohorts in this study enabled the identification of otherwise missed disease associations as ESR1 (P = 1.31 × 10 −5), demonstrating the importance of diversifying study cohorts.

Black People, Breast Neoplasms/genetics, Female, Formins/genetics, Genetic Predisposition to Disease, Genetic Testing, Genome-Wide Association Study/methods, Humans, Polymorphism, Single Nucleotide, Gene regulation, Rare variants, Breast cancer susceptibility, Genome-wide association study, Diverse ancestry
1756-994X
Mueller, Stefanie H
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Lai, Alvina G
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Valkovskaya, Maria
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Michailidou, Kyriaki
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Bolla, Manjeet K
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Wang, Qin
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Dennis, Joe
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Lush, Michael
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Abu-Ful, Zomoruda
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Ahearn, Thomas U
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Andrulis, Irene L
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Anton-Culver, Hoda
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Antonenkova, Natalia N
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Arndt, Volker
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Aronson, Kristan J
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Augustinsson, Annelie
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Baert, Thais
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Freeman, Laura E Beane
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Beckmann, Matthias W
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Behrens, Sabine
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Benitez, Javier
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Bermisheva, Marina
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Blomqvist, Carl
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Bogdanova, Natalia V
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Bojesen, Stig E
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Bonanni, Bernardo
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Brenner, Hermann
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Brucker, Sara Y
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Buys, Saundra S
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Castelao, Jose E
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Chan, Tsun L
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Chang-Claude, Jenny
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Chanock, Stephen J
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Choi, Ji-Yeob
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Chung, Wendy K
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Colonna, Sarah V
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Cornelissen, Sten
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Couch, Fergus J
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Czene, Kamila
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Daly, Mary B
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Devilee, Peter
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Dörk, Thilo
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Dossus, Laure
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Dwek, Miriam
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Eccles, Diana M
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Ekici, Arif B.
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Eliassen, A. Heather
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Engel, Christoph
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Evans, D Gareth
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Howell, Anthony
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Jones, Michael E
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Scott, Christopher
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Tapper, William J
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Taylor, Jack A
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NBCS Collaborators
Mueller, Stefanie H
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Lai, Alvina G
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Valkovskaya, Maria
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Michailidou, Kyriaki
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Bolla, Manjeet K
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Wang, Qin
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Dennis, Joe
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Lush, Michael
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Abu-Ful, Zomoruda
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Ahearn, Thomas U
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Andrulis, Irene L
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Anton-Culver, Hoda
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Antonenkova, Natalia N
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Arndt, Volker
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Aronson, Kristan J
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Augustinsson, Annelie
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Baert, Thais
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Freeman, Laura E Beane
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Beckmann, Matthias W
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Behrens, Sabine
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Benitez, Javier
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Bermisheva, Marina
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Blomqvist, Carl
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Bogdanova, Natalia V
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Bojesen, Stig E
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Bonanni, Bernardo
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Brenner, Hermann
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Brucker, Sara Y
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Buys, Saundra S
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Castelao, Jose E
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Chan, Tsun L
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Chang-Claude, Jenny
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Chanock, Stephen J
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Choi, Ji-Yeob
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Chung, Wendy K
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Colonna, Sarah V
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Cornelissen, Sten
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Couch, Fergus J
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Czene, Kamila
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Daly, Mary B
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Devilee, Peter
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Dörk, Thilo
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Dossus, Laure
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Dwek, Miriam
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Eccles, Diana M
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Ekici, Arif B.
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Eliassen, A. Heather
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Engel, Christoph
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Evans, D Gareth
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Howell, Anthony
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Jones, Michael E
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Scott, Christopher
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Tapper, William J
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Taylor, Jack A
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Mueller, Stefanie H, Lai, Alvina G, Valkovskaya, Maria, Michailidou, Kyriaki, Bolla, Manjeet K, Wang, Qin, Dwek, Miriam, Ekici, Arif B., Eliassen, A. Heather and Engel, Christoph , NBCS Collaborators (2023) Aggregation tests identify new gene associations with breast cancer in populations with diverse ancestry. Genome Medicine, 15 (7), [7]. (doi:10.1186/s13073-022-01152-5).

Record type: Article

Abstract

Background: Low-frequency variants play an important role in breast cancer (BC) susceptibility. Gene-based methods can increase power by combining multiple variants in the same gene and help identify target genes. Methods: We evaluated the potential of gene-based aggregation in the Breast Cancer Association Consortium cohorts including 83,471 cases and 59,199 controls. Low-frequency variants were aggregated for individual genes’ coding and regulatory regions. Association results in European ancestry samples were compared to single-marker association results in the same cohort. Gene-based associations were also combined in meta-analysis across individuals with European, Asian, African, and Latin American and Hispanic ancestry. Results: In European ancestry samples, 14 genes were significantly associated (q < 0.05) with BC. Of those, two genes, FMNL3 (P = 6.11 × 10 −6) and AC058822.1 (P = 1.47 × 10 −4), represent new associations. High FMNL3 expression has previously been linked to poor prognosis in several other cancers. Meta-analysis of samples with diverse ancestry discovered further associations including established candidate genes ESR1 and CBLB. Furthermore, literature review and database query found further support for a biologically plausible link with cancer for genes CBLB, FMNL3, FGFR2, LSP1, MAP3K1, and SRGAP2C. Conclusions: Using extended gene-based aggregation tests including coding and regulatory variation, we report identification of plausible target genes for previously identified single-marker associations with BC as well as the discovery of novel genes implicated in BC development. Including multi ancestral cohorts in this study enabled the identification of otherwise missed disease associations as ESR1 (P = 1.31 × 10 −5), demonstrating the importance of diversifying study cohorts.

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Accepted/In Press date: 16 December 2022
Published date: 26 January 2023
Additional Information: Funding Information: This result is part of a project that has received funding from the European Research Council (ERC) under the European Union’s Horizon 2020 research and innovation programme (Grant agreement No. 948561). Funding Information: BCAC is funded by the European Union’s Horizon 2020 Research and Innovation Programme (grant numbers 634935 and 633,784 for BRIDGES and B-CAST respectively), and the PERSPECTIVE I&I project, funded by the Government of Canada through Genome Canada and the Canadian Institutes of Health Research, the Ministère de l’Économie et de l'Innovation du Québec through Genome Québec, the Quebec Breast Cancer Foundation. The EU Horizon 2020 Research and Innovation Programme funding source had no role in study design, data collection, data analysis, data interpretation, or writing of the report. Additional funding for BCAC is provided via the Confluence project which is funded with intramural funds from the National Cancer Institute Intramural Research Program, National Institutes of Health. Publisher Copyright: © 2023, The Author(s).
Keywords: Black People, Breast Neoplasms/genetics, Female, Formins/genetics, Genetic Predisposition to Disease, Genetic Testing, Genome-Wide Association Study/methods, Humans, Polymorphism, Single Nucleotide, Gene regulation, Rare variants, Breast cancer susceptibility, Genome-wide association study, Diverse ancestry

Identifiers

Local EPrints ID: 476582
URI: http://eprints.soton.ac.uk/id/eprint/476582
DOI: doi:10.1186/s13073-022-01152-5
ISSN: 1756-994X
PURE UUID: cb40087e-0f98-4b4f-9996-d675a460c38e
ORCID for Diana M Eccles: ORCID iD orcid.org/0000-0002-9935-3169
ORCID for William J Tapper: ORCID iD orcid.org/0000-0002-5896-1889

Catalogue record

Date deposited: 09 May 2023 16:46
Last modified: 17 Mar 2024 02:49

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Contributors

Author: Stefanie H Mueller
Author: Alvina G Lai
Author: Maria Valkovskaya
Author: Kyriaki Michailidou
Author: Manjeet K Bolla
Author: Qin Wang
Author: Joe Dennis
Author: Michael Lush
Author: Zomoruda Abu-Ful
Author: Thomas U Ahearn
Author: Irene L Andrulis
Author: Hoda Anton-Culver
Author: Natalia N Antonenkova
Author: Volker Arndt
Author: Kristan J Aronson
Author: Annelie Augustinsson
Author: Thais Baert
Author: Laura E Beane Freeman
Author: Matthias W Beckmann
Author: Sabine Behrens
Author: Javier Benitez
Author: Marina Bermisheva
Author: Carl Blomqvist
Author: Natalia V Bogdanova
Author: Stig E Bojesen
Author: Bernardo Bonanni
Author: Hermann Brenner
Author: Sara Y Brucker
Author: Saundra S Buys
Author: Jose E Castelao
Author: Tsun L Chan
Author: Jenny Chang-Claude
Author: Stephen J Chanock
Author: Ji-Yeob Choi
Author: Wendy K Chung
Author: Sarah V Colonna
Author: Sten Cornelissen
Author: Fergus J Couch
Author: Kamila Czene
Author: Mary B Daly
Author: Peter Devilee
Author: Thilo Dörk
Author: Laure Dossus
Author: Miriam Dwek
Author: Diana M Eccles ORCID iD
Author: Arif B. Ekici
Author: A. Heather Eliassen
Author: Christoph Engel
Author: D Gareth Evans
Author: Anthony Howell
Author: Michael E Jones
Author: Christopher Scott
Author: William J Tapper ORCID iD
Author: Jack A Taylor
Corporate Author: NBCS Collaborators

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