Copy Number Variants Are Ovarian Cancer Risk Alleles at Known and Novel Risk Loci

Authors

Amber A DeVries
Joe Dennis
Jonathan P Tyrer
Pei-Chen Peng
Simon G Coetzee
Alberto L Reyes
Jasmine T Plummer
Brian D Davis
Stephanie S Chen
Felipe Segato Dezem
Katja K H Aben
Hoda Anton-Culver
Natalia N Antonenkova
Matthias W Beckmann
Alicia Beeghly-Fadiel
Andrew Berchuck
Natalia V Bogdanova
Nadja Bogdanova-Markov
James D Brenton
Ralf Butzow
Ian Campbell
Jenny Chang-Claude
Georgia Chenevix-Trench
Linda S Cook
Anna DeFazio
Jennifer A Doherty
Thilo Dörk
Diana M Eccles
A Heather Eliassen
Peter A Fasching
Renée T Fortner
Graham G Giles
Ellen L Goode
Marc T Goodman
Jacek Gronwald
OPAL Study Group
AOCS Group
Niclas Håkansson
Michelle A T Hildebrandt
Chad Huff
David G Huntsman
Allan Jensen
Siddhartha Kar
Beth Y Karlan
Elza K Khusnutdinova
Lambertus A Kiemeney
Susanne K Kjaer
Jolanta Kupryjanczyk
Marilyne Labrie
Diether Lambrechts
Nhu D Le
Jan Lubiński
Taymaa May
Usha Menon
Roger L Milne
Francesmary Modugno
Alvaro N Monteiro
Kirsten B Moysich
Kunle Odunsi
Håkan Olsson
Celeste L Pearce
Tanja Pejovic
Susan J Ramus
Elio Riboli
Marjorie J Riggan
Isabelle Romieu
Dale P Sandler
Joellen M Schildkraut
V Wendy Setiawan
Weiva Sieh
Honglin Song
Rebecca Sutphen
Kathryn L Terry
Pamela J Thompson
Linda Titus
Shelley S Tworoger
Els Van Nieuwenhuysen
Digna Velez Edwards
Penelope M Webb
Nicolas Wentzensen
Alice S Whittemore
Alicja Wolk
Anna H Wu
Argyrios Ziogas
Matthew L Freedman
Kate Lawrenson
Paul D P Pharoah
Douglas F Easton
Simon A Gayther
Michelle R Jones

Publication Date

11-14-2022

Journal

Journal of the National Cancer Institute

Abstract

BACKGROUND: Known risk alleles for epithelial ovarian cancer (EOC) account for approximately 40% of the heritability for EOC. Copy number variants (CNVs) have not been investigated as EOC risk alleles in a large population cohort.

METHODS: Single nucleotide polymorphism array data from 13 071 EOC cases and 17 306 controls of White European ancestry were used to identify CNVs associated with EOC risk using a rare admixture maximum likelihood test for gene burden and a by-probe ratio test. We performed enrichment analysis of CNVs at known EOC risk loci and functional biofeatures in ovarian cancer-related cell types.

RESULTS: We identified statistically significant risk associations with CNVs at known EOC risk genes; BRCA1 (PEOC = 1.60E-21; OREOC = 8.24), RAD51C (Phigh-grade serous ovarian cancer [HGSOC] = 5.5E-4; odds ratio [OR]HGSOC = 5.74 del), and BRCA2 (PHGSOC = 7.0E-4; ORHGSOC = 3.31 deletion). Four suggestive associations (P < .001) were identified for rare CNVs. Risk-associated CNVs were enriched (P < .05) at known EOC risk loci identified by genome-wide association study. Noncoding CNVs were enriched in active promoters and insulators in EOC-related cell types.

CONCLUSIONS: CNVs in BRCA1 have been previously reported in smaller studies, but their observed frequency in this large population-based cohort, along with the CNVs observed at BRCA2 and RAD51C gene loci in EOC cases, suggests that these CNVs are potentially pathogenic and may contribute to the spectrum of disease-causing mutations in these genes. CNVs are likely to occur in a wider set of susceptibility regions, with potential implications for clinical genetic testing and disease prevention.

Keywords

Female, Humans, Carcinoma, Ovarian Epithelial, Genome-Wide Association Study, Alleles, DNA Copy Number Variations, Genetic Predisposition to Disease, Polymorphism, Single Nucleotide, Ovarian Neoplasms

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Supplementary Materials

PMID: 36210504