Investigation of exomic variants associated with overall survival in ovarian cancer

The Australian Ovarian Cancer Study Group; ACS Investigators

doi:10.1158/1055-9965.EPI-15-0240

Investigation of exomic variants associated with overall survival in ovarian cancer

The Australian Ovarian Cancer Study Group, ACS Investigators

Obstetrics and Gynecology

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

9 Scopus citations

Abstract

Background: While numerous susceptibility loci for epithelial ovarian cancer (EOC) have been identified, few associations have been reported with overall survival. In the absence of common prognostic genetic markers, we hypothesize that rare coding variants may be associated with overall EOC survival and assessed their contribution in two exome-based genotyping projects of the Ovarian Cancer Association Consortium (OCAC). Methods: The primary patient set (Set 1) included 14 independentEOCstudies (4,293 patients) and 227,892 variants, and a secondary patient set (Set 2) included six additional EOC studies (1,744 patients) and 114,620 variants. Because power to detect rare variants individually is reduced, gene-level tests were conducted. Sets were analyzed separately at individual variants and by gene, and then combined with meta-analyses (73,203 variants and 13,163 genes overlapped). Results: No individual variant reached genome-wide statistical significance. A SNP previously implicated to be associated with EOC risk and, to a lesser extent, survival, rs8170, showed the strongest evidence of association with survival and similar effect size estimates across sets (P_meta=1.1E-6,HR_Set1=1.17,HR_Set2= 1.14). Rare variants in ATG2B, an autophagy gene important for apoptosis, were significantly associated with survival after multiple testing correction (P_meta = 1.1E-6; P_corrected = 0.01). Conclusions: Common variant rs8170 and rare variants in ATG2B may be associated with EOC overall survival, although further study is needed. Impact: This study represents the first exome-wide association study of EOCsurvival to include rare variant analyses, and suggests that complementary single variant and gene-level analyses in large studies are needed to identify rare variants that warrant follow-up study. Cancer Epidemiol Biomarkers Prev; 25(3); 446-54.

Original language	English (US)
Pages (from-to)	446-454
Number of pages	9
Journal	Cancer Epidemiology Biomarkers and Prevention
Volume	25
Issue number	3
DOIs	https://doi.org/10.1158/1055-9965.EPI-15-0240
State	Published - Mar 2016

ASJC Scopus subject areas

Medicine(all)

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10.1158/1055-9965.EPI-15-0240

Cite this

@article{37fdbb15751c42ff800db786920700a9,

title = "Investigation of exomic variants associated with overall survival in ovarian cancer",

abstract = "Background: While numerous susceptibility loci for epithelial ovarian cancer (EOC) have been identified, few associations have been reported with overall survival. In the absence of common prognostic genetic markers, we hypothesize that rare coding variants may be associated with overall EOC survival and assessed their contribution in two exome-based genotyping projects of the Ovarian Cancer Association Consortium (OCAC). Methods: The primary patient set (Set 1) included 14 independentEOCstudies (4,293 patients) and 227,892 variants, and a secondary patient set (Set 2) included six additional EOC studies (1,744 patients) and 114,620 variants. Because power to detect rare variants individually is reduced, gene-level tests were conducted. Sets were analyzed separately at individual variants and by gene, and then combined with meta-analyses (73,203 variants and 13,163 genes overlapped). Results: No individual variant reached genome-wide statistical significance. A SNP previously implicated to be associated with EOC risk and, to a lesser extent, survival, rs8170, showed the strongest evidence of association with survival and similar effect size estimates across sets (Pmeta=1.1E-6,HRSet1=1.17,HRSet2= 1.14). Rare variants in ATG2B, an autophagy gene important for apoptosis, were significantly associated with survival after multiple testing correction (Pmeta = 1.1E-6; Pcorrected = 0.01). Conclusions: Common variant rs8170 and rare variants in ATG2B may be associated with EOC overall survival, although further study is needed. Impact: This study represents the first exome-wide association study of EOCsurvival to include rare variant analyses, and suggests that complementary single variant and gene-level analyses in large studies are needed to identify rare variants that warrant follow-up study. Cancer Epidemiol Biomarkers Prev; 25(3); 446-54.",

author = "{The Australian Ovarian Cancer Study Group} and {ACS Investigators} and Winham, {Stacey J.} and Ailith Pirie and Chen, {Yian Ann} and Larson, {Melissa C.} and Fogarty, {Zachary C.} and Earp, {Madalene A.} and Hoda Anton-Culver and Bandera, {Elisa V.} and Daniel Cramer and Doherty, {Jennifer A.} and Goodman, {Marc T.} and Jacek Gronwald and Karlan, {Beth Y.} and Kjaer, {Susanne K.} and Levine, {Douglas A.} and Usha Menon and Ness, {Roberta B.} and Pearce, {Celeste L.} and Tanja Pejovic and Rossing, {Mary Anne} and Nicolas Wentzensen and Bean, {Yukie T.} and Maria Bisogna and Brinton, {Louise A.} and Carney, {Michael E.} and Cunningham, {Julie M.} and Cezary Cybulski and Anna DeFazio and Dicks, {Ed M.} and Edwards, {Robert P.} and Gayther, {Simon A.} and Aleksandra Gentry-Maharaj and Martin Gore and Iversen, {Edwin S.} and Allan Jensen and Johnatty, {Sharon E.} and Jenny Lester and Lin, {Hui Yi} and Jolanta Lissowska and Jan Lubinski and Janusz Menkiszak and Francesmary Modugno and Moysich, {Kirsten B.} and Irene Orlow and Pike, {Malcolm C.} and Ramus, {Susan J.} and Honglin Song and Terry, {Kathryn L.} and Thompson, {Pamela J.} and Tyrer, {Jonathan P.}",

note = "Funding Information: The Australian Ovarian Cancer Study Management Group (D. Bowtell, G. Chenevix-Trench, A. deFazio, D. Gertig, A. Green, P. Webb) and ACS Investigators (A. Green, P. Parsons, N. Hayward, P. Webb, D. Whiteman) thank all the clinical and scientific collaborators (see http://www.aocstudy. org/) and the women for their contribution. The authors thank I. Jacobs, M. Widschwendter, E. Wozniak, A. Ryan, J. Ford, and N. Balogun for their contribution to the study. This work was supported by grants from the NIH Office of Research on Women''s Health (Building Interdisciplinary Careers in Women''s Health award K12HD065987; to S.J. Winham) and Genetic Associations and Mechanisms in Oncology (GAME-ON), an NCI Cancer Post-GWAS Initiative (U19-CA148112; to T.A. Sellers). G. Chenevix-Trench is supported by Fellowships from NHMRC. A. deFazio is supported by the University of Sydney Cancer Research Fund and the Cancer Institute NSW through the Sydney West Translational Cancer Research Centre. C.M. Phelan is funded in part by NIH R01 CA-149429. A. Pirie is funding in part by a Medical Research Council Studentship. A. Gentry-Maharaj is supported by Eve Appeal and the Oak Foundation. In addition, the individual study sites were supported by: AUS: U.S. Army Medical Research and Materiel Command (DAMD17-01-1-0729; to G. Chenevix-Trench), National Health & Medical Research Council of Australia (199600 and 400281; to G. Chenevix-Trench), Cancer Councils of New South Wales, Victoria, Queensland, South Australia, and Tasmania, Cancer Foundation of Western Australia. DOV: Funding for this study was provided by U19-CA148112 (to T. Sellers); HAW: NIH (R01-CA58598, N01-CN-55424, and N01-PC-67001; to M.T. Goodman); HOP: US Army Medical Research and Material Command DAMD17-02-1-0669 (to F. Modugno); NCI K07-CA080668, R01-CA95023, R01-CA126841 (to F. Modugno); P50-CA159981 (to F. Modugno); NIH/National Center for Research Resources/General Clinical Research Center grant M01-RR000056 (to F. Modugno); LAX: American Cancer Society Early Detection Professorship (SIOP-06-258-01-COUN; to B.Y. Karlan) and the National Center for Advancing Translational Sciences (NCATS), grant UL1TR000124 (to B.Y. Karlan); MAL: funding for this study was provided by research grant R01-CA61107 from the NCI, Bethesda, MD (to S.K. Kjaer and A. Jensen); research grant 94 222 52 from the Danish Cancer Society, Copenhagen, Denmark (to S.K. Kjaer and A. Jensen); and the Mermaid I project (to S.K. Kjaer and A. Jenesn); MAC and MAY: NIH (R01-CA122443, P30-CA15083, P50-CA136393; to E.L. Goode); NCO: Department of Defense (DAMD17-02-1-0666; to J.M. Schildkraut); NEC: NIH R01-CA54419 and P50-CA105009 and Department of Defense W81XWH-10-1-02802 (to K.L. Terry); NJO: NCI (NIH-K07 CA095666, NIH-K22-CA138563, and P30-CA072720; to E.V. Bandera) and the Cancer Institute of New Jersey (to E.V. Bandera); ORE: OHSU Foundation (to T. Pejovic); POC: Pomeranian Medical University (to J. Gronwald); RMH: Cancer Research UK (no grant number is available), Royal Marsden Hospital (to P.D. Pharoah); SEA: Cancer Research UK (C490/A10119 C490/A10124; to P.D. Pharoah); UK National Institute for Health Research Biomedical Research Centres at the University of Cambridge, SEARCH team, Craig Luccarini, Caroline Baynes, Don Conroy; UKO: The UKOPS study was funded by The Eve Appeal (The Oak Foundation) and supported by the National Institute for Health Research University College London Hospitals Biomedical Research Centre (to U. Menon and S.A. Gayther). USC: P01-CA17054, P30-CA14089, R01-CA61132, N01-PC67010, N01-CN025403 (to M.C. Pike), R03-CA113148, R03-CA115195 (to C.L. Pearce), and California Cancer Research Program (00-01389V-20170, 2II0200; to A. Wu); POL: Intramural Research Program of the NCI. Publisher Copyright: {\textcopyright} 2016 AACR.",

year = "2016",

month = mar,

doi = "10.1158/1055-9965.EPI-15-0240",

language = "English (US)",

volume = "25",

pages = "446--454",

journal = "Cancer Epidemiology Biomarkers and Prevention",

issn = "1055-9965",

publisher = "American Association for Cancer Research Inc.",

number = "3",

}

TY - JOUR

T1 - Investigation of exomic variants associated with overall survival in ovarian cancer

AU - The Australian Ovarian Cancer Study Group

AU - ACS Investigators

AU - Winham, Stacey J.

AU - Pirie, Ailith

AU - Chen, Yian Ann

AU - Larson, Melissa C.

AU - Fogarty, Zachary C.

AU - Earp, Madalene A.

AU - Anton-Culver, Hoda

AU - Bandera, Elisa V.

AU - Cramer, Daniel

AU - Doherty, Jennifer A.

AU - Goodman, Marc T.

AU - Gronwald, Jacek

AU - Karlan, Beth Y.

AU - Kjaer, Susanne K.

AU - Levine, Douglas A.

AU - Menon, Usha

AU - Ness, Roberta B.

AU - Pearce, Celeste L.

AU - Pejovic, Tanja

AU - Rossing, Mary Anne

AU - Wentzensen, Nicolas

AU - Bean, Yukie T.

AU - Bisogna, Maria

AU - Brinton, Louise A.

AU - Carney, Michael E.

AU - Cunningham, Julie M.

AU - Cybulski, Cezary

AU - DeFazio, Anna

AU - Dicks, Ed M.

AU - Edwards, Robert P.

AU - Gayther, Simon A.

AU - Gentry-Maharaj, Aleksandra

AU - Gore, Martin

AU - Iversen, Edwin S.

AU - Jensen, Allan

AU - Johnatty, Sharon E.

AU - Lester, Jenny

AU - Lin, Hui Yi

AU - Lissowska, Jolanta

AU - Lubinski, Jan

AU - Menkiszak, Janusz

AU - Modugno, Francesmary

AU - Moysich, Kirsten B.

AU - Orlow, Irene

AU - Pike, Malcolm C.

AU - Ramus, Susan J.

AU - Song, Honglin

AU - Terry, Kathryn L.

AU - Thompson, Pamela J.

AU - Tyrer, Jonathan P.

N1 - Funding Information: The Australian Ovarian Cancer Study Management Group (D. Bowtell, G. Chenevix-Trench, A. deFazio, D. Gertig, A. Green, P. Webb) and ACS Investigators (A. Green, P. Parsons, N. Hayward, P. Webb, D. Whiteman) thank all the clinical and scientific collaborators (see http://www.aocstudy. org/) and the women for their contribution. The authors thank I. Jacobs, M. Widschwendter, E. Wozniak, A. Ryan, J. Ford, and N. Balogun for their contribution to the study. This work was supported by grants from the NIH Office of Research on Women''s Health (Building Interdisciplinary Careers in Women''s Health award K12HD065987; to S.J. Winham) and Genetic Associations and Mechanisms in Oncology (GAME-ON), an NCI Cancer Post-GWAS Initiative (U19-CA148112; to T.A. Sellers). G. Chenevix-Trench is supported by Fellowships from NHMRC. A. deFazio is supported by the University of Sydney Cancer Research Fund and the Cancer Institute NSW through the Sydney West Translational Cancer Research Centre. C.M. Phelan is funded in part by NIH R01 CA-149429. A. Pirie is funding in part by a Medical Research Council Studentship. A. Gentry-Maharaj is supported by Eve Appeal and the Oak Foundation. In addition, the individual study sites were supported by: AUS: U.S. Army Medical Research and Materiel Command (DAMD17-01-1-0729; to G. Chenevix-Trench), National Health & Medical Research Council of Australia (199600 and 400281; to G. Chenevix-Trench), Cancer Councils of New South Wales, Victoria, Queensland, South Australia, and Tasmania, Cancer Foundation of Western Australia. DOV: Funding for this study was provided by U19-CA148112 (to T. Sellers); HAW: NIH (R01-CA58598, N01-CN-55424, and N01-PC-67001; to M.T. Goodman); HOP: US Army Medical Research and Material Command DAMD17-02-1-0669 (to F. Modugno); NCI K07-CA080668, R01-CA95023, R01-CA126841 (to F. Modugno); P50-CA159981 (to F. Modugno); NIH/National Center for Research Resources/General Clinical Research Center grant M01-RR000056 (to F. Modugno); LAX: American Cancer Society Early Detection Professorship (SIOP-06-258-01-COUN; to B.Y. Karlan) and the National Center for Advancing Translational Sciences (NCATS), grant UL1TR000124 (to B.Y. Karlan); MAL: funding for this study was provided by research grant R01-CA61107 from the NCI, Bethesda, MD (to S.K. Kjaer and A. Jensen); research grant 94 222 52 from the Danish Cancer Society, Copenhagen, Denmark (to S.K. Kjaer and A. Jensen); and the Mermaid I project (to S.K. Kjaer and A. Jenesn); MAC and MAY: NIH (R01-CA122443, P30-CA15083, P50-CA136393; to E.L. Goode); NCO: Department of Defense (DAMD17-02-1-0666; to J.M. Schildkraut); NEC: NIH R01-CA54419 and P50-CA105009 and Department of Defense W81XWH-10-1-02802 (to K.L. Terry); NJO: NCI (NIH-K07 CA095666, NIH-K22-CA138563, and P30-CA072720; to E.V. Bandera) and the Cancer Institute of New Jersey (to E.V. Bandera); ORE: OHSU Foundation (to T. Pejovic); POC: Pomeranian Medical University (to J. Gronwald); RMH: Cancer Research UK (no grant number is available), Royal Marsden Hospital (to P.D. Pharoah); SEA: Cancer Research UK (C490/A10119 C490/A10124; to P.D. Pharoah); UK National Institute for Health Research Biomedical Research Centres at the University of Cambridge, SEARCH team, Craig Luccarini, Caroline Baynes, Don Conroy; UKO: The UKOPS study was funded by The Eve Appeal (The Oak Foundation) and supported by the National Institute for Health Research University College London Hospitals Biomedical Research Centre (to U. Menon and S.A. Gayther). USC: P01-CA17054, P30-CA14089, R01-CA61132, N01-PC67010, N01-CN025403 (to M.C. Pike), R03-CA113148, R03-CA115195 (to C.L. Pearce), and California Cancer Research Program (00-01389V-20170, 2II0200; to A. Wu); POL: Intramural Research Program of the NCI. Publisher Copyright: © 2016 AACR.

PY - 2016/3

Y1 - 2016/3

N2 - Background: While numerous susceptibility loci for epithelial ovarian cancer (EOC) have been identified, few associations have been reported with overall survival. In the absence of common prognostic genetic markers, we hypothesize that rare coding variants may be associated with overall EOC survival and assessed their contribution in two exome-based genotyping projects of the Ovarian Cancer Association Consortium (OCAC). Methods: The primary patient set (Set 1) included 14 independentEOCstudies (4,293 patients) and 227,892 variants, and a secondary patient set (Set 2) included six additional EOC studies (1,744 patients) and 114,620 variants. Because power to detect rare variants individually is reduced, gene-level tests were conducted. Sets were analyzed separately at individual variants and by gene, and then combined with meta-analyses (73,203 variants and 13,163 genes overlapped). Results: No individual variant reached genome-wide statistical significance. A SNP previously implicated to be associated with EOC risk and, to a lesser extent, survival, rs8170, showed the strongest evidence of association with survival and similar effect size estimates across sets (Pmeta=1.1E-6,HRSet1=1.17,HRSet2= 1.14). Rare variants in ATG2B, an autophagy gene important for apoptosis, were significantly associated with survival after multiple testing correction (Pmeta = 1.1E-6; Pcorrected = 0.01). Conclusions: Common variant rs8170 and rare variants in ATG2B may be associated with EOC overall survival, although further study is needed. Impact: This study represents the first exome-wide association study of EOCsurvival to include rare variant analyses, and suggests that complementary single variant and gene-level analyses in large studies are needed to identify rare variants that warrant follow-up study. Cancer Epidemiol Biomarkers Prev; 25(3); 446-54.

AB - Background: While numerous susceptibility loci for epithelial ovarian cancer (EOC) have been identified, few associations have been reported with overall survival. In the absence of common prognostic genetic markers, we hypothesize that rare coding variants may be associated with overall EOC survival and assessed their contribution in two exome-based genotyping projects of the Ovarian Cancer Association Consortium (OCAC). Methods: The primary patient set (Set 1) included 14 independentEOCstudies (4,293 patients) and 227,892 variants, and a secondary patient set (Set 2) included six additional EOC studies (1,744 patients) and 114,620 variants. Because power to detect rare variants individually is reduced, gene-level tests were conducted. Sets were analyzed separately at individual variants and by gene, and then combined with meta-analyses (73,203 variants and 13,163 genes overlapped). Results: No individual variant reached genome-wide statistical significance. A SNP previously implicated to be associated with EOC risk and, to a lesser extent, survival, rs8170, showed the strongest evidence of association with survival and similar effect size estimates across sets (Pmeta=1.1E-6,HRSet1=1.17,HRSet2= 1.14). Rare variants in ATG2B, an autophagy gene important for apoptosis, were significantly associated with survival after multiple testing correction (Pmeta = 1.1E-6; Pcorrected = 0.01). Conclusions: Common variant rs8170 and rare variants in ATG2B may be associated with EOC overall survival, although further study is needed. Impact: This study represents the first exome-wide association study of EOCsurvival to include rare variant analyses, and suggests that complementary single variant and gene-level analyses in large studies are needed to identify rare variants that warrant follow-up study. Cancer Epidemiol Biomarkers Prev; 25(3); 446-54.

UR - http://www.scopus.com/inward/record.url?scp=84961262486&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=84961262486&partnerID=8YFLogxK

U2 - 10.1158/1055-9965.EPI-15-0240

DO - 10.1158/1055-9965.EPI-15-0240

M3 - Article

C2 - 26747452

AN - SCOPUS:84961262486

SN - 1055-9965

VL - 25

SP - 446

EP - 454

JO - Cancer Epidemiology Biomarkers and Prevention

JF - Cancer Epidemiology Biomarkers and Prevention

IS - 3

ER -

Investigation of exomic variants associated with overall survival in ovarian cancer

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