Evaluation of copy-number variants as modifiers of breast and ovarian cancer risk for BRCA1 pathogenic variant carriers

Logan C. Walker; Louise Marquart; John F. Pearson; George A.R. Wiggins; Tracy A. O'Mara; Michael T. Parsons; Daniel Barrowdale; Lesley McGuffog; Joe Dennis; Javier Benitez; Thomas P. Slavin; Paolo Radice; Debra Frost; Andrew K. Godwin; Alfons Meindl; Rita Katharina Schmutzler; Claudine Isaacs; Beth N. Peshkin; Trinidad Caldes; Frans B.L. Hogervorst; Conxi Lazaro; Anna Jakubowska; Marco Montagna; Xiaoqing Chen; Kenneth Offit; Peter J. Hulick; Irene L. Andrulis; Annika Lindblom; Robert L. Nussbaum; Katherine L. Nathanson; Georgia Chenevix-Trench; Antonis C. Antoniou; Fergus J. Couch; Amanda B. Spurdle

doi:10.1038/ejhg.2016.203

Evaluation of copy-number variants as modifiers of breast and ovarian cancer risk for BRCA1 pathogenic variant carriers

Logan C. Walker, Louise Marquart, John F. Pearson, George A.R. Wiggins, Tracy A. O'Mara, Michael T. Parsons, Daniel Barrowdale, Lesley McGuffog, Joe Dennis, Javier Benitez, Thomas P. Slavin, Paolo Radice, Debra Frost, Andrew K. Godwin, Alfons Meindl, Rita Katharina Schmutzler, Claudine Isaacs, Beth N. Peshkin, Trinidad Caldes, Frans B.L. HogervorstConxi Lazaro, Anna Jakubowska, Marco Montagna, Xiaoqing Chen, Kenneth Offit, Peter J. Hulick, Irene L. Andrulis, Annika Lindblom, Robert L. Nussbaum, Katherine L. Nathanson, Georgia Chenevix-Trench, Antonis C. Antoniou, Fergus J. Couch, Amanda B. Spurdle

Research output: Contribution to journal › Article › peer-review

11 Scopus citations

Abstract

Genome-wide studies of patients carrying pathogenic variants (mutations) in BRCA1 or BRCA2 have reported strong associations between single-nucleotide polymorphisms (SNPs) and cancer risk. To conduct the first genome-wide association analysis of copy-number variants (CNVs) with breast or ovarian cancer risk in a cohort of 2500 BRCA1 pathogenic variant carriers, CNV discovery was performed using multiple calling algorithms and Illumina 610k SNP array data from a previously published genome-wide association study. Our analysis, which focused on functionally disruptive genomic deletions overlapping gene regions, identified a number of loci associated with risk of breast or ovarian cancer for BRCA1 pathogenic variant carriers. Despite only including putative deletions called by at least two or more algorithms, detection of selected CNVs by ancillary molecular technologies only confirmed 40% of predicted common (>1% allele frequency) variants. These include four loci that were associated (unadjusted P<0.05) with breast cancer (GTF2H2, ZNF385B, NAALADL2 and PSG5), and two loci associated with ovarian cancer (CYP2A7 and OR2A1). An interesting finding from this study was an association of a validated CNV deletion at the CYP2A7 locus (19q13.2) with decreased ovarian cancer risk (relative risk=0.50, P=0.007). Genomic analysis found this deletion coincides with a region displaying strong regulatory potential in ovarian tissue, but not in breast epithelial cells. This study highlighted the need to verify CNVs in vitro, but also provides evidence that experimentally validated CNVs (with plausible biological consequences) can modify risk of breast or ovarian cancer in BRCA1 pathogenic variant carriers.

Original language	English (US)
Pages (from-to)	432-438
Number of pages	7
Journal	European Journal of Human Genetics
Volume	25
Issue number	4
DOIs	https://doi.org/10.1038/ejhg.2016.203
State	Published - Apr 1 2017

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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10.1038/ejhg.2016.203

Cite this

Walker, L. C., Marquart, L., Pearson, J. F., Wiggins, G. A. R., O'Mara, T. A., Parsons, M. T., Barrowdale, D., McGuffog, L., Dennis, J., Benitez, J., Slavin, T. P., Radice, P., Frost, D., Godwin, A. K., Meindl, A., Schmutzler, R. K., Isaacs, C., Peshkin, B. N., Caldes, T., ... Spurdle, A. B. (2017). Evaluation of copy-number variants as modifiers of breast and ovarian cancer risk for BRCA1 pathogenic variant carriers. European Journal of Human Genetics, 25(4), 432-438. https://doi.org/10.1038/ejhg.2016.203

Walker, LC, Marquart, L, Pearson, JF, Wiggins, GAR, O'Mara, TA, Parsons, MT, Barrowdale, D, McGuffog, L, Dennis, J, Benitez, J, Slavin, TP, Radice, P, Frost, D, Godwin, AK, Meindl, A, Schmutzler, RK, Isaacs, C, Peshkin, BN, Caldes, T, Hogervorst, FBL, Lazaro, C, Jakubowska, A, Montagna, M, Chen, X, Offit, K, Hulick, PJ, Andrulis, IL, Lindblom, A, Nussbaum, RL, Nathanson, KL, Chenevix-Trench, G, Antoniou, AC, Couch, FJ & Spurdle, AB 2017, 'Evaluation of copy-number variants as modifiers of breast and ovarian cancer risk for BRCA1 pathogenic variant carriers', European Journal of Human Genetics, vol. 25, no. 4, pp. 432-438. https://doi.org/10.1038/ejhg.2016.203

@article{39e9ea4d57334199a38752af07eb2e97,

title = "Evaluation of copy-number variants as modifiers of breast and ovarian cancer risk for BRCA1 pathogenic variant carriers",

abstract = "Genome-wide studies of patients carrying pathogenic variants (mutations) in BRCA1 or BRCA2 have reported strong associations between single-nucleotide polymorphisms (SNPs) and cancer risk. To conduct the first genome-wide association analysis of copy-number variants (CNVs) with breast or ovarian cancer risk in a cohort of 2500 BRCA1 pathogenic variant carriers, CNV discovery was performed using multiple calling algorithms and Illumina 610k SNP array data from a previously published genome-wide association study. Our analysis, which focused on functionally disruptive genomic deletions overlapping gene regions, identified a number of loci associated with risk of breast or ovarian cancer for BRCA1 pathogenic variant carriers. Despite only including putative deletions called by at least two or more algorithms, detection of selected CNVs by ancillary molecular technologies only confirmed 40% of predicted common (>1% allele frequency) variants. These include four loci that were associated (unadjusted P<0.05) with breast cancer (GTF2H2, ZNF385B, NAALADL2 and PSG5), and two loci associated with ovarian cancer (CYP2A7 and OR2A1). An interesting finding from this study was an association of a validated CNV deletion at the CYP2A7 locus (19q13.2) with decreased ovarian cancer risk (relative risk=0.50, P=0.007). Genomic analysis found this deletion coincides with a region displaying strong regulatory potential in ovarian tissue, but not in breast epithelial cells. This study highlighted the need to verify CNVs in vitro, but also provides evidence that experimentally validated CNVs (with plausible biological consequences) can modify risk of breast or ovarian cancer in BRCA1 pathogenic variant carriers.",

author = "Walker, {Logan C.} and Louise Marquart and Pearson, {John F.} and Wiggins, {George A.R.} and O'Mara, {Tracy A.} and Parsons, {Michael T.} and Daniel Barrowdale and Lesley McGuffog and Joe Dennis and Javier Benitez and Slavin, {Thomas P.} and Paolo Radice and Debra Frost and Godwin, {Andrew K.} and Alfons Meindl and Schmutzler, {Rita Katharina} and Claudine Isaacs and Peshkin, {Beth N.} and Trinidad Caldes and Hogervorst, {Frans B.L.} and Conxi Lazaro and Anna Jakubowska and Marco Montagna and Xiaoqing Chen and Kenneth Offit and Hulick, {Peter J.} and Andrulis, {Irene L.} and Annika Lindblom and Nussbaum, {Robert L.} and Nathanson, {Katherine L.} and Georgia Chenevix-Trench and Antoniou, {Antonis C.} and Couch, {Fergus J.} and Spurdle, {Amanda B.}",

note = "Funding Information: HCSC: We acknowledge Alicia Tosar and Paula Diaque for their technical assistance. HCSC was supported by a grant RD12/0036/0006 and 15/00059 from ISCIII (Spain), partially supported by European Regional Development FEDER funds. HEBON: The Hereditary Breast and Ovarian Cancer Research Group Netherlands (HEBON) consists of the following Collaborating Centers: Coordinating center: Netherlands Cancer Institute, Amsterdam, Netherlands: MA Rookus, FBL Hogervorst, FE van Leeuwen, S Verhoef, MK Schmidt, NS Russell, JL de Lange and R Wijnands; Erasmus Medical Center, Rotterdam, Netherlands: JM Coll{\'e}e, AMW van den Ouweland, MJ Hooning, C Seynaeve, CHM van Deurzen and IM Obdeijn; Leiden University Medical Center, Netherlands: CJ van Asperen, JT Wijnen, RAEM Tollenaar, P Devilee and TCTEF van Cronenburg; Radboud University Nijmegen Medical Center, Netherlands: CM Kets and AR Mensenkamp; University Medical Center Utrecht, Netherlands: MGEM Ausems, RB van der Luijt and CC van der Pol; Amsterdam Medical Center, Netherlands: CM Aalfs and TAM van Os; VU University Medical Center, Amsterdam, Netherlands: JJP Gille, Q Waisfisz and HEJ Meijers-Heijboer; University Hospital Maastricht, Netherlands: EB G{\'o}mez-Garcia and MJ Blok; University Medical Center Groningen, Netherlands: JC Oosterwijk, AH van der Hout, MJ Mourits and GH de Bock; The Netherlands Foundation for the detection of hereditary tumors, Leiden, Netherlands: HF Vasen; The Netherlands Comprehensive Cancer Organization (IKNL): S Siesling and J Verloop; The Dutch Pathology Registry (PALGA): LIH Overbeek. The HEBON study is supported by the Dutch Cancer Society grants NKI1998-1854, NKI2004-3088 and NKI2007-3756, the Netherlands Organization of Scientific Research grant NWO 91109024, the Pink Ribbon grants 110005 and 2014-187.WO76, the BBMRI grant NWO 184.021.007/ CP46, and the Transcan grant JTC 2012 Cancer 12-054. HEBON thanks the registration teams of IKNL and PALGA for part of the data collection. Funding Information: FOR provided by the UCSF Cancer Risk Program and Helen Diller Family Comprehensive Cancer Center. UPENN: National Institutes of Health (NIH; R01-CA102776 and R01-CA083855; Breast Cancer Research Foundation; Susan G. Komen Foundation for the cure, Basser Research Center for BRCA. Funding Information: BCFR: This work was supported by grant UM1 CA164920 from the USA National Cancer Institute. The content of this manuscript does not necessarily reflect the views or policies of the National Cancer Institute or any of the collaborating centers in the Breast Cancer Family Registry (BCFR), nor does mention of trade names, commercial products or organizations imply endorsement by the USA Government or the BCFR. CIMBA: We wish to thank the patients and families, physicians, genetic counselors and research nurses involved in the CIMBA studies. The CIMBA data management and data analysis were supported by CRUK grants C12292/ A11174 and C1287/A10118. Funding Information: COH-CCGCRN: Patients were recruited for study from the City of Hope Clinical Cancer Genomics Community Research Network, supported in part by Award Number RC4CA153828 (PI: J Weitzel) from the National Cancer Institute and the Office of the Director, National Institutes of Health. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. CONSIT TEAM–INT: Monica Barile and Irene Feroce of the Istituto Europeo di Oncologia, Milan, Italy; Gabriele Capone of the University of Florence, Florence, Italy; Alessandra Viel and Riccardo Dolcetti of the CRO Aviano National Cancer Institute, Aviano (PN), Italy. Associazione Italiana Ricerca sul Cancro (AIRC) to P Radice (IG 2014 Id.15547). Funds from Italian citizens who allocated the 5 × 1000 share of their tax payment in support of the Fondazione IRCCS Istituto Nazionale Tumori, according to Italian laws (INT-Institutional strategic projects {\textquoteleft}5×1000{\textquoteright}). Funding Information: GEMO: Genetic Modifiers of Cancer Risk in BRCA1/2 Mutation Carriers (GEMO) study: National Cancer Genetics Network «UNICANCER Genetic Group», France. We wish to pay a tribute to Olga M Sinilnikova, who with Dominique Stoppa-Lyonnet initiated and coordinated GEMO until she sadly passed away on 30 June 2014, and to thank all the GEMO collaborating groups for their contribution to this study. GEMO Collaborating Centers are: Coordinating Centers, Unit{\'e} Mixte de G{\'e}n{\'e}tique Constitutionnelle des Cancers Fr{\'e}quents, Hospices Civils de Lyon - Centre L{\'e}on B{\'e}rard and Equipe «G{\'e}n{\'e}tique du cancer du sein»; Centre de Recherche en Canc{\'e}rologie de Lyon: Olga Sinilnikova, Sylvie Mazoyer, Francesca Damiola, Laure Barjhoux, Carole Verny-Pierre, M{\'e}lanie L{\'e}one, Nadia Boutry-Kryza, Alain Calender and Sophie Giraud; and Service de G{\'e}n{\'e}tique Oncologique, Institut Curie, Paris: Dominique Stoppa-Lyonnet, Marion Gauthier-Villars, Bruno Buecher, Claude Houdayer, Etienne Rouleau, Lisa Golmard, Agn{\`e}s Collet, Virginie Moncoutier, Muriel Belotti, Antoine de Pauw, Camille Elan, Catherine Nogues, Emmanuelle Fourme and Anne-Marie Birot. Institut Gustave Roussy, Villejuif: Brigitte Bressac-de-Paillerets, Olivier Caron and Marine Guillaud-Bataille. Centre Jean Perrin, Clermont–Ferrand: Yves-Jean Bignon and Nancy Uhrhammer. Centre L{\'e}on B{\'e}rard, Lyon: Christine Lasset, Val{\'e}rie Bonadona and Sandrine Handallou. Centre Fran{\c c}ois Baclesse, Caen: Agn{\`e}s Hardouin, Pascaline Berthet, Dominique Vaur and Laurent Castera. Institut Paoli Calmettes, Marseille: Hagay Sobol, Violaine Bourdon, Tetsuro Noguchi, Audrey Remenieras and Fran{\c c}ois Eisinger. CHU Arnaud-de-Villeneuve, Montpellier: Isabelle Coupier and Pascal Pujol. Centre Oscar Lambret, Lille: Jean-Philippe Peyrat, Jo{\"e}lle Fournier, Fran{\c c}oise R{\'e}villion, Philippe Vennin and Claude Adenis. Centre Paul Strauss, Strasbourg: Dani{\`e}le Muller and Jean-Pierre Fricker. Institut Bergoni{\'e}, Bordeaux: Emmanuelle Barouk-Simonet, Fran{\c c}oise Bonnet, Virginie Bubien, Nicolas Sevenet and Michel Longy. Institut Claudius Regaud, Toulouse: Christine Toulas, Rosine Guimbaud, Laurence Gladieff and Viviane Feillel. CHU Grenoble: Dominique Leroux, H{\'e}l{\`e}ne Dreyfus, Christine Rebischung and Magalie Peysselon. CHU Dijon: Fanny Coron, Laurence Faivre. CHU St-Etienne: Fabienne Prieur, Marine Lebrun and Caroline Kientz. H{\^o}tel Dieu Centre Hospitalier, Chamb{\'e}ry: Sandra Fert Ferrer. Centre Antoine Lacassagne, Nice: Marc Fr{\'e}nay. CHU Limoges: Laurence V{\'e}nat-Bouvet. CHU Nantes: Capucine Delnatte. CHU Bretonneau, Tours: Isabelle Mortemousque. Groupe Hospitalier Piti{\'e}-Salp{\'e}tri{\`e}re, Paris: Florence Coulet, Chrystelle Colas, Florent Soubrier and Mathilde Warcoin. CHU Vandoeuvre-les-Nancy: Johanna Sokolowska and Myriam Bronner. CHU Besan{\c c}on: Marie-Agn{\`e}s Collonge-Rame and Alexandre Damette. Creighton University, Omaha, USA: Henry T Lynch and Carrie L Snyder. The study was supported by the Ligue Nationale Contre le Cancer; the Association {\textquoteleft}Le cancer du sein, parlons-en!{\textquoteright} Award; the Canadian Institutes of Health Research for the {\textquoteleft}CIHR Team in Familial Risks of Breast Cancer{\textquoteright} program and the French National Institute of Cancer (INCa). GEORGETOWN: Support was provided by the Nontherapeutic Subject Registry Shared Resource at Georgetown University (NIH/NCI grant P30-CA051008), the Fisher Center for Hereditary Cancer and Clinical Genomics Research and Swing Fore the Cure. Funding Information: SWE-BRCA: Swedish scientists participating as SWE-BRCA collaborators are from: Lund University and University Hospital: {\AA}ke Borg, H{\aa}kan Olsson, Helena Jernstr{\"o}m, Karin Henriksson, Katja Harbst, Maria Soller and Ulf Kristoffersson; Gothenburg Sahlgrenska University Hospital: Anna {\"O}fverholm, Margareta Nordling, Per Karlsson and Zakaria Einbeigi; Stockholm and Karolinska University Hospital: Anna von Wachenfeldt, Annelie Liljegren, Annika Lindblom, Brita Arver, Gisela Barbany Bustinza and Johanna Rantala; Ume{\aa} University Hospital: Beatrice Melin, Christina Edwinsdotter Ardnor and Monica Emanuelsson; Uppsala University: Hans Ehrencrona, Maritta Hellstr{\"o}m Pigg and Richard Rosenquist; and Link{\"o}ping University Hospital: Marie Stenmark-Askmalm and Sigrun Liedgren. SWE-BRCA collaborators are supported by the Swedish Cancer Society. UCSF: We would like to thank Dr Robert Nussbaum and the following genetic counselors for participant recruitment: Beth Crawford, Kate Loranger, Julie Mak, Nicola Stewart, Robin Lee, Amie Blanco and Peggy Conrad. And thanks to Ms Salina Chan for her data management. Funding was provided by the UCSF Cancer Risk Program and Helen Diller Family Comprehensive Cancer Center. UPENN: National Institutes of Health (NIH; R01-CA102776 and R01-CA083855; Breast Cancer Research Foundation; Susan G. Komen Foundation for the cure, Basser Research Center for BRCA. Funding Information: ICO: We wish to thank the ICO Hereditary Cancer Program team led by Dr Gabriel Capella. Contract grant sponsor: Asociaci{\'o}n Espa{\~n}ola Contra el C{\'a}ncer and Spanish Health Research Fund; Carlos III Health Institute; Catalan Health Institute; and Autonomous Government of Catalonia. Contract grant numbers: ISCIIIRETIC RD06/0020/1051, RD12/0036/008, PI10/01422, PI10/00748, PI13/00285, PIE13/00022, 2009SGR290 and 2014SGR364. IHCC: The IHCC was supported by Grant PBZ_KBN_122/P05/2004. IOVHBOCS: IOVHBOCS is supported by Ministero della Salute and {\textquoteleft}5× 1000{\textquoteright} Istituto Oncologico Veneto grant. Funding Information: MSKCC: We wish to thank Anne Lincoln and Lauren Jacobs. MSKCC is supported by grants from the Breast Cancer Research Foundation, the Robert and Kate Niehaus Clinical Cancer Genetics Initiative and the Andrew Sabin Research Fund. Funding Information: KCONFAB: We wish to thank Heather Thorne, Eveline Niedermayr, all the kConFab research nurses and staff, the heads and staff of the Family Cancer Clinics, and the Clinical Follow Up Study (which has received funding from the NHMRC, the National Breast Cancer Foundation, Cancer Australia and the National Institute of Health (USA)) for their contributions to this resource, and the many families who contribute to kConFab. kConFab is supported by a grant from the National Breast Cancer Foundation, and previously by the National Health and Medical Research Council (NHMRC), the Queensland Cancer Fund, the Cancer Councils of New South Wales, Victoria, Tasmania and South Australia, and the Cancer Foundation of Western Australia. MAYO: MAYO is supported by NIH grants CA116167, CA192393 and CA176785, an NCI Specialized Program of Research Excellence (SPORE) in Breast Cancer (CA116201), a grant from the Breast Cancer Research Foundation and a generous gift from the David F and Margaret T Grohne Family Foundation. Funding Information: CNIO: We thank Alicia Barroso, Rosario Alonso and Guillermo Pita for their assistance. This work was partially supported by Spanish Association against Cancer (AECC08), RTICC 06/0020/1060, FISPI08/1120, Mutua Madrile{\~n}a Foundation (FMMA) and SAF2010-20493. Funding Information: FCCC: We thank Ms JoEllen Weaver and Dr Betsy Bove for their technical support. The authors acknowledge support from The University of Kansas Cancer Center (P30 CA168524) and the Kansas Bioscience Authority Eminent Scholar Program. AKG was funded by 5U01CA113916, R01CA140323 and by the Chancellors Distinguished Chair in Biomedical Sciences Professorship. GC-HBOC: The German Consortium of Hereditary Breast and Ovarian Cancer (GC-HBOC) is supported by the German Cancer Aid (grant no 110837, Rita K Schmutzler). Funding Information: EMBRACE: EMBRACE is supported by Cancer Research UK Grants C1287/ A10118 and C1287/A11990. The Investigators at The Institute of Cancer Research and The Royal Marsden NHS Foundation Trust are supported by an NIHR grant to the Biomedical Research Centre at The Institute of Cancer Research and The Royal Marsden NHS Foundation Trust. Publisher Copyright: {\textcopyright} 2017 Macmillan Publishers Limited, part of Springer Nature. All rights reserved.",

year = "2017",

month = apr,

day = "1",

doi = "10.1038/ejhg.2016.203",

language = "English (US)",

volume = "25",

pages = "432--438",

journal = "European Journal of Human Genetics",

issn = "1018-4813",

publisher = "Nature Publishing Group",

number = "4",

}

TY - JOUR

T1 - Evaluation of copy-number variants as modifiers of breast and ovarian cancer risk for BRCA1 pathogenic variant carriers

AU - Walker, Logan C.

AU - Marquart, Louise

AU - Pearson, John F.

AU - Wiggins, George A.R.

AU - O'Mara, Tracy A.

AU - Parsons, Michael T.

AU - Barrowdale, Daniel

AU - McGuffog, Lesley

AU - Dennis, Joe

AU - Benitez, Javier

AU - Slavin, Thomas P.

AU - Radice, Paolo

AU - Frost, Debra

AU - Godwin, Andrew K.

AU - Meindl, Alfons

AU - Schmutzler, Rita Katharina

AU - Isaacs, Claudine

AU - Peshkin, Beth N.

AU - Caldes, Trinidad

AU - Hogervorst, Frans B.L.

AU - Lazaro, Conxi

AU - Jakubowska, Anna

AU - Montagna, Marco

AU - Chen, Xiaoqing

AU - Offit, Kenneth

AU - Hulick, Peter J.

AU - Andrulis, Irene L.

AU - Lindblom, Annika

AU - Nussbaum, Robert L.

AU - Nathanson, Katherine L.

AU - Chenevix-Trench, Georgia

AU - Antoniou, Antonis C.

AU - Couch, Fergus J.

AU - Spurdle, Amanda B.

N1 - Funding Information: HCSC: We acknowledge Alicia Tosar and Paula Diaque for their technical assistance. HCSC was supported by a grant RD12/0036/0006 and 15/00059 from ISCIII (Spain), partially supported by European Regional Development FEDER funds. HEBON: The Hereditary Breast and Ovarian Cancer Research Group Netherlands (HEBON) consists of the following Collaborating Centers: Coordinating center: Netherlands Cancer Institute, Amsterdam, Netherlands: MA Rookus, FBL Hogervorst, FE van Leeuwen, S Verhoef, MK Schmidt, NS Russell, JL de Lange and R Wijnands; Erasmus Medical Center, Rotterdam, Netherlands: JM Collée, AMW van den Ouweland, MJ Hooning, C Seynaeve, CHM van Deurzen and IM Obdeijn; Leiden University Medical Center, Netherlands: CJ van Asperen, JT Wijnen, RAEM Tollenaar, P Devilee and TCTEF van Cronenburg; Radboud University Nijmegen Medical Center, Netherlands: CM Kets and AR Mensenkamp; University Medical Center Utrecht, Netherlands: MGEM Ausems, RB van der Luijt and CC van der Pol; Amsterdam Medical Center, Netherlands: CM Aalfs and TAM van Os; VU University Medical Center, Amsterdam, Netherlands: JJP Gille, Q Waisfisz and HEJ Meijers-Heijboer; University Hospital Maastricht, Netherlands: EB Gómez-Garcia and MJ Blok; University Medical Center Groningen, Netherlands: JC Oosterwijk, AH van der Hout, MJ Mourits and GH de Bock; The Netherlands Foundation for the detection of hereditary tumors, Leiden, Netherlands: HF Vasen; The Netherlands Comprehensive Cancer Organization (IKNL): S Siesling and J Verloop; The Dutch Pathology Registry (PALGA): LIH Overbeek. The HEBON study is supported by the Dutch Cancer Society grants NKI1998-1854, NKI2004-3088 and NKI2007-3756, the Netherlands Organization of Scientific Research grant NWO 91109024, the Pink Ribbon grants 110005 and 2014-187.WO76, the BBMRI grant NWO 184.021.007/ CP46, and the Transcan grant JTC 2012 Cancer 12-054. HEBON thanks the registration teams of IKNL and PALGA for part of the data collection. Funding Information: FOR provided by the UCSF Cancer Risk Program and Helen Diller Family Comprehensive Cancer Center. UPENN: National Institutes of Health (NIH; R01-CA102776 and R01-CA083855; Breast Cancer Research Foundation; Susan G. Komen Foundation for the cure, Basser Research Center for BRCA. Funding Information: BCFR: This work was supported by grant UM1 CA164920 from the USA National Cancer Institute. The content of this manuscript does not necessarily reflect the views or policies of the National Cancer Institute or any of the collaborating centers in the Breast Cancer Family Registry (BCFR), nor does mention of trade names, commercial products or organizations imply endorsement by the USA Government or the BCFR. CIMBA: We wish to thank the patients and families, physicians, genetic counselors and research nurses involved in the CIMBA studies. The CIMBA data management and data analysis were supported by CRUK grants C12292/ A11174 and C1287/A10118. Funding Information: COH-CCGCRN: Patients were recruited for study from the City of Hope Clinical Cancer Genomics Community Research Network, supported in part by Award Number RC4CA153828 (PI: J Weitzel) from the National Cancer Institute and the Office of the Director, National Institutes of Health. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. CONSIT TEAM–INT: Monica Barile and Irene Feroce of the Istituto Europeo di Oncologia, Milan, Italy; Gabriele Capone of the University of Florence, Florence, Italy; Alessandra Viel and Riccardo Dolcetti of the CRO Aviano National Cancer Institute, Aviano (PN), Italy. Associazione Italiana Ricerca sul Cancro (AIRC) to P Radice (IG 2014 Id.15547). Funds from Italian citizens who allocated the 5 × 1000 share of their tax payment in support of the Fondazione IRCCS Istituto Nazionale Tumori, according to Italian laws (INT-Institutional strategic projects ‘5×1000’). Funding Information: GEMO: Genetic Modifiers of Cancer Risk in BRCA1/2 Mutation Carriers (GEMO) study: National Cancer Genetics Network «UNICANCER Genetic Group», France. We wish to pay a tribute to Olga M Sinilnikova, who with Dominique Stoppa-Lyonnet initiated and coordinated GEMO until she sadly passed away on 30 June 2014, and to thank all the GEMO collaborating groups for their contribution to this study. GEMO Collaborating Centers are: Coordinating Centers, Unité Mixte de Génétique Constitutionnelle des Cancers Fréquents, Hospices Civils de Lyon - Centre Léon Bérard and Equipe «Génétique du cancer du sein»; Centre de Recherche en Cancérologie de Lyon: Olga Sinilnikova, Sylvie Mazoyer, Francesca Damiola, Laure Barjhoux, Carole Verny-Pierre, Mélanie Léone, Nadia Boutry-Kryza, Alain Calender and Sophie Giraud; and Service de Génétique Oncologique, Institut Curie, Paris: Dominique Stoppa-Lyonnet, Marion Gauthier-Villars, Bruno Buecher, Claude Houdayer, Etienne Rouleau, Lisa Golmard, Agnès Collet, Virginie Moncoutier, Muriel Belotti, Antoine de Pauw, Camille Elan, Catherine Nogues, Emmanuelle Fourme and Anne-Marie Birot. Institut Gustave Roussy, Villejuif: Brigitte Bressac-de-Paillerets, Olivier Caron and Marine Guillaud-Bataille. Centre Jean Perrin, Clermont–Ferrand: Yves-Jean Bignon and Nancy Uhrhammer. Centre Léon Bérard, Lyon: Christine Lasset, Valérie Bonadona and Sandrine Handallou. Centre François Baclesse, Caen: Agnès Hardouin, Pascaline Berthet, Dominique Vaur and Laurent Castera. Institut Paoli Calmettes, Marseille: Hagay Sobol, Violaine Bourdon, Tetsuro Noguchi, Audrey Remenieras and François Eisinger. CHU Arnaud-de-Villeneuve, Montpellier: Isabelle Coupier and Pascal Pujol. Centre Oscar Lambret, Lille: Jean-Philippe Peyrat, Joëlle Fournier, Françoise Révillion, Philippe Vennin and Claude Adenis. Centre Paul Strauss, Strasbourg: Danièle Muller and Jean-Pierre Fricker. Institut Bergonié, Bordeaux: Emmanuelle Barouk-Simonet, Françoise Bonnet, Virginie Bubien, Nicolas Sevenet and Michel Longy. Institut Claudius Regaud, Toulouse: Christine Toulas, Rosine Guimbaud, Laurence Gladieff and Viviane Feillel. CHU Grenoble: Dominique Leroux, Hélène Dreyfus, Christine Rebischung and Magalie Peysselon. CHU Dijon: Fanny Coron, Laurence Faivre. CHU St-Etienne: Fabienne Prieur, Marine Lebrun and Caroline Kientz. Hôtel Dieu Centre Hospitalier, Chambéry: Sandra Fert Ferrer. Centre Antoine Lacassagne, Nice: Marc Frénay. CHU Limoges: Laurence Vénat-Bouvet. CHU Nantes: Capucine Delnatte. CHU Bretonneau, Tours: Isabelle Mortemousque. Groupe Hospitalier Pitié-Salpétrière, Paris: Florence Coulet, Chrystelle Colas, Florent Soubrier and Mathilde Warcoin. CHU Vandoeuvre-les-Nancy: Johanna Sokolowska and Myriam Bronner. CHU Besançon: Marie-Agnès Collonge-Rame and Alexandre Damette. Creighton University, Omaha, USA: Henry T Lynch and Carrie L Snyder. The study was supported by the Ligue Nationale Contre le Cancer; the Association ‘Le cancer du sein, parlons-en!’ Award; the Canadian Institutes of Health Research for the ‘CIHR Team in Familial Risks of Breast Cancer’ program and the French National Institute of Cancer (INCa). GEORGETOWN: Support was provided by the Nontherapeutic Subject Registry Shared Resource at Georgetown University (NIH/NCI grant P30-CA051008), the Fisher Center for Hereditary Cancer and Clinical Genomics Research and Swing Fore the Cure. Funding Information: SWE-BRCA: Swedish scientists participating as SWE-BRCA collaborators are from: Lund University and University Hospital: Åke Borg, Håkan Olsson, Helena Jernström, Karin Henriksson, Katja Harbst, Maria Soller and Ulf Kristoffersson; Gothenburg Sahlgrenska University Hospital: Anna Öfverholm, Margareta Nordling, Per Karlsson and Zakaria Einbeigi; Stockholm and Karolinska University Hospital: Anna von Wachenfeldt, Annelie Liljegren, Annika Lindblom, Brita Arver, Gisela Barbany Bustinza and Johanna Rantala; Umeå University Hospital: Beatrice Melin, Christina Edwinsdotter Ardnor and Monica Emanuelsson; Uppsala University: Hans Ehrencrona, Maritta Hellström Pigg and Richard Rosenquist; and Linköping University Hospital: Marie Stenmark-Askmalm and Sigrun Liedgren. SWE-BRCA collaborators are supported by the Swedish Cancer Society. UCSF: We would like to thank Dr Robert Nussbaum and the following genetic counselors for participant recruitment: Beth Crawford, Kate Loranger, Julie Mak, Nicola Stewart, Robin Lee, Amie Blanco and Peggy Conrad. And thanks to Ms Salina Chan for her data management. Funding was provided by the UCSF Cancer Risk Program and Helen Diller Family Comprehensive Cancer Center. UPENN: National Institutes of Health (NIH; R01-CA102776 and R01-CA083855; Breast Cancer Research Foundation; Susan G. Komen Foundation for the cure, Basser Research Center for BRCA. Funding Information: ICO: We wish to thank the ICO Hereditary Cancer Program team led by Dr Gabriel Capella. Contract grant sponsor: Asociación Española Contra el Cáncer and Spanish Health Research Fund; Carlos III Health Institute; Catalan Health Institute; and Autonomous Government of Catalonia. Contract grant numbers: ISCIIIRETIC RD06/0020/1051, RD12/0036/008, PI10/01422, PI10/00748, PI13/00285, PIE13/00022, 2009SGR290 and 2014SGR364. IHCC: The IHCC was supported by Grant PBZ_KBN_122/P05/2004. IOVHBOCS: IOVHBOCS is supported by Ministero della Salute and ‘5× 1000’ Istituto Oncologico Veneto grant. Funding Information: MSKCC: We wish to thank Anne Lincoln and Lauren Jacobs. MSKCC is supported by grants from the Breast Cancer Research Foundation, the Robert and Kate Niehaus Clinical Cancer Genetics Initiative and the Andrew Sabin Research Fund. Funding Information: KCONFAB: We wish to thank Heather Thorne, Eveline Niedermayr, all the kConFab research nurses and staff, the heads and staff of the Family Cancer Clinics, and the Clinical Follow Up Study (which has received funding from the NHMRC, the National Breast Cancer Foundation, Cancer Australia and the National Institute of Health (USA)) for their contributions to this resource, and the many families who contribute to kConFab. kConFab is supported by a grant from the National Breast Cancer Foundation, and previously by the National Health and Medical Research Council (NHMRC), the Queensland Cancer Fund, the Cancer Councils of New South Wales, Victoria, Tasmania and South Australia, and the Cancer Foundation of Western Australia. MAYO: MAYO is supported by NIH grants CA116167, CA192393 and CA176785, an NCI Specialized Program of Research Excellence (SPORE) in Breast Cancer (CA116201), a grant from the Breast Cancer Research Foundation and a generous gift from the David F and Margaret T Grohne Family Foundation. Funding Information: CNIO: We thank Alicia Barroso, Rosario Alonso and Guillermo Pita for their assistance. This work was partially supported by Spanish Association against Cancer (AECC08), RTICC 06/0020/1060, FISPI08/1120, Mutua Madrileña Foundation (FMMA) and SAF2010-20493. Funding Information: FCCC: We thank Ms JoEllen Weaver and Dr Betsy Bove for their technical support. The authors acknowledge support from The University of Kansas Cancer Center (P30 CA168524) and the Kansas Bioscience Authority Eminent Scholar Program. AKG was funded by 5U01CA113916, R01CA140323 and by the Chancellors Distinguished Chair in Biomedical Sciences Professorship. GC-HBOC: The German Consortium of Hereditary Breast and Ovarian Cancer (GC-HBOC) is supported by the German Cancer Aid (grant no 110837, Rita K Schmutzler). Funding Information: EMBRACE: EMBRACE is supported by Cancer Research UK Grants C1287/ A10118 and C1287/A11990. The Investigators at The Institute of Cancer Research and The Royal Marsden NHS Foundation Trust are supported by an NIHR grant to the Biomedical Research Centre at The Institute of Cancer Research and The Royal Marsden NHS Foundation Trust. Publisher Copyright: © 2017 Macmillan Publishers Limited, part of Springer Nature. All rights reserved.

PY - 2017/4/1

Y1 - 2017/4/1

N2 - Genome-wide studies of patients carrying pathogenic variants (mutations) in BRCA1 or BRCA2 have reported strong associations between single-nucleotide polymorphisms (SNPs) and cancer risk. To conduct the first genome-wide association analysis of copy-number variants (CNVs) with breast or ovarian cancer risk in a cohort of 2500 BRCA1 pathogenic variant carriers, CNV discovery was performed using multiple calling algorithms and Illumina 610k SNP array data from a previously published genome-wide association study. Our analysis, which focused on functionally disruptive genomic deletions overlapping gene regions, identified a number of loci associated with risk of breast or ovarian cancer for BRCA1 pathogenic variant carriers. Despite only including putative deletions called by at least two or more algorithms, detection of selected CNVs by ancillary molecular technologies only confirmed 40% of predicted common (>1% allele frequency) variants. These include four loci that were associated (unadjusted P<0.05) with breast cancer (GTF2H2, ZNF385B, NAALADL2 and PSG5), and two loci associated with ovarian cancer (CYP2A7 and OR2A1). An interesting finding from this study was an association of a validated CNV deletion at the CYP2A7 locus (19q13.2) with decreased ovarian cancer risk (relative risk=0.50, P=0.007). Genomic analysis found this deletion coincides with a region displaying strong regulatory potential in ovarian tissue, but not in breast epithelial cells. This study highlighted the need to verify CNVs in vitro, but also provides evidence that experimentally validated CNVs (with plausible biological consequences) can modify risk of breast or ovarian cancer in BRCA1 pathogenic variant carriers.

AB - Genome-wide studies of patients carrying pathogenic variants (mutations) in BRCA1 or BRCA2 have reported strong associations between single-nucleotide polymorphisms (SNPs) and cancer risk. To conduct the first genome-wide association analysis of copy-number variants (CNVs) with breast or ovarian cancer risk in a cohort of 2500 BRCA1 pathogenic variant carriers, CNV discovery was performed using multiple calling algorithms and Illumina 610k SNP array data from a previously published genome-wide association study. Our analysis, which focused on functionally disruptive genomic deletions overlapping gene regions, identified a number of loci associated with risk of breast or ovarian cancer for BRCA1 pathogenic variant carriers. Despite only including putative deletions called by at least two or more algorithms, detection of selected CNVs by ancillary molecular technologies only confirmed 40% of predicted common (>1% allele frequency) variants. These include four loci that were associated (unadjusted P<0.05) with breast cancer (GTF2H2, ZNF385B, NAALADL2 and PSG5), and two loci associated with ovarian cancer (CYP2A7 and OR2A1). An interesting finding from this study was an association of a validated CNV deletion at the CYP2A7 locus (19q13.2) with decreased ovarian cancer risk (relative risk=0.50, P=0.007). Genomic analysis found this deletion coincides with a region displaying strong regulatory potential in ovarian tissue, but not in breast epithelial cells. This study highlighted the need to verify CNVs in vitro, but also provides evidence that experimentally validated CNVs (with plausible biological consequences) can modify risk of breast or ovarian cancer in BRCA1 pathogenic variant carriers.

UR - http://www.scopus.com/inward/record.url?scp=85011277736&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85011277736&partnerID=8YFLogxK

U2 - 10.1038/ejhg.2016.203

DO - 10.1038/ejhg.2016.203

M3 - Article

C2 - 28145423

AN - SCOPUS:85011277736

SN - 1018-4813

VL - 25

SP - 432

EP - 438

JO - European Journal of Human Genetics

JF - European Journal of Human Genetics

IS - 4

ER -

Evaluation of copy-number variants as modifiers of breast and ovarian cancer risk for BRCA1 pathogenic variant carriers

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