Large-scale genome-wide association meta-analysis of endometriosis reveals 13 novel loci and genetically-associated comorbidity with other pain conditions

Rahmioglu Nilufer(Centre for Human Genetics), Banasik Karina(Medical University of Lublin), Christofidou Paraskevi(St Thomas' Hospital), D. Larson Rebecca(Brigham and Women's Hospital), Galarneau Genevieve(RGenix (United States)), Giri Ayush(Institute of Public Health), Stuart MacGregor(QIMR Berghofer Medical Research Institute), Mortlock Sally(The University of Queensland), Sapkota Yadav(St. Jude Children's Research Hospital), Schork J Andrew(Mental Health Services), Sobalska-Kwapis Marta(University of Łódź), Stefansdottir Lilja(deCODE Genetics (Iceland)), T. J. Constance(Medical University of Lublin), Uimari Outi(Oulu University Hospital), Sosuke Adachi(Niigata University), Andrews Shan(University of California, San Francisco), Arnadottir Ragnheidur(Reykjavík University), Kristoffer Sølvsten Burgdorf(Medical University of Lublin), Campbell Archie(Western General Hospital), Cheuk SK Cecilia(Centre for Human Genetics), Clementi Caterina(RGenix (United States)), Cook James(University of Liverpool), De Vivo Immaculata(Harvard University), D. Amy(Brigham and Women's Hospital), O Dorien(Leuven Institute for Fertility and Embryology), Edwards Todd(Vanderbilt University Medical Center), Fontanillas Pierre(Mountain View College), Fung N Jenny(The University of Queensland), Geirsson T Reynir(Reykjavík University), Jane E. Girling(Royal Women's Hospital), Harris R Holly(Fred Hutch Cancer Center), Holdsworth-Carson Sarah(Royal Women's Hospital), Houshdaran Sahar(University of California, San Francisco), Hu-Seliger Tina(RGenix (United States)), Jaqrvelin Marjo-Riitta(Oulu University Hospital), Kepka Ewa(University of Łódź), Kulig Bartosz(Polish Mother’s Memorial Hospital Research Institute), Laufer R Marc(Brigham and Women's Hospital), Law Matthew(QIMR Berghofer Medical Research Institute), Low Siew-Kee(RIKEN Center for Integrative Medical Sciences), Mangino Massimo(St Thomas' Hospital), Marciniak Blazej(University of Łódź), Charoula Matalliotaki(The General Hospital of Heraklion "Venizeleio-Pananio"), Michail Matalliotakis(The General Hospital of Heraklion "Venizeleio-Pananio"), Murray D Alison(University of Aberdeen), Nezhat Camran(Center for Special Minimally Invasive and Robotic Surgery), Nõukas Margit(University of Tartu), O Sainte Catherine(QIMR Berghofer Medical Research Institute), Padmanabhan Sandosh(University of Glasgow), Paranjpe Manish(University of California, San Francisco), Parfitt David-Emlyn(RGenix (United States)), Peters Maire(Competence Centre on Health Technologies (Estonia)), Polak Grzegorz(Medical University of Lublin), Porteous David(Western General Hospital), Hanna Romanowicz(Polish Mother’s Memorial Hospital Research Institute), Saare Merli(Competence Centre on Health Technologies (Estonia)), Shafrir Amy(Brigham and Women's Hospital), Siewierska-Górska Anna(University of Łódź), Sini Skarp(Imperial College London), Slomka Marcin(University of Łódź), Smith Blair(University of Dundee), Beata Smolarz(Polish Mother’s Memorial Hospital Research Institute), Szaflik Tomasz(Polish Mother’s Memorial Hospital Research Institute), S. Krzysztof(Polish Mother’s Memorial Hospital Research Institute), Terry Kathyrn(Brigham and Women's Hospital), Guðmar Þorleifsson(deCODE Genetics (Iceland)), Carla Tomassetti(Leuven Institute for Fertility and Embryology), Vanhie Arne(Leuven Institute for Fertility and Embryology), Vincent Katy(John Radcliffe Hospital), Vitonis Allison(Brigham and Women's Hospital), Werge Thomas(University of Copenhagen), S Andersen(Centre for Human Genetics), Karina Banasik(John Radcliffe Hospital), Søren Brunak(John Radcliffe Hospital), KS Burgdorf(University of Copenhagen), Christian Erikstrup(St Thomas' Hospital), TF Hansen(Harvard University), Helle Hjalgrim(Brigham and Women's Hospital), Gregor B. E. Jemec(RGenix (United States)), Poul Jennum(Vanderbilt University Medical Center), KR Nielsen(QIMR Berghofer Medical Research Institute), Mette Nyegaard(The University of Queensland), HM Paarup(St. Jude Children's Research Hospital), Ole Birger Pedersen(Mental Health Services), Maria Skaalum Petersen(Lundbeck Foundation), Erik Sørensen(University of Copenhagen), Henrik Ullum(University of Copenhagen), Thomas Werge(University of Łódź), Daníel F. Guðbjartsson, Kāri Stefánsson, Hreinn Stefánsson, Unnur Þorsteinsdóttir, PB Mortensen(Centre for Human Genetics), DM Hougaard(John Radcliffe Hospital), AD Borglum(University of Copenhagen), Chasman Daniel(Brigham and Women's Hospital), D. Thomas(Merck KGaA, Darmstadt (Germany)), Giudice C Linda(University of California, San Francisco), Goulielmos N George(University of Crete), Hapangama K Dharani(University of Liverpool), Hayward Caroline(Western General Hospital), Horne W Andrew(MRC Centre for Reproductive Health), Kamatani Yoichiro(RIKEN Center for Integrative Medical Sciences), Michiaki Kubo(RIKEN Center for Integrative Medical Sciences), Martikainen Hannu(Oulu University Hospital), Rogers AW Peter(Royal Women's Hospital), Saunders T Philippa(Centre for Inflammation Research), Sirota Marina(University of California, San Francisco), Spector Tim(St Thomas' Hospital), Dominik Strapagiel(University of Łódź), Tung Y Joyce(Mountain View College), W. G. Stanton David(QIMR Berghofer Medical Research Institute), Becker M Christian(John Radcliffe Hospital), Salumets Andres(University of Helsinki), Mägi Reedik(University of Tartu), Kraft Peter(Harvard University), Mette Nyegaard(Aarhus University), Nyholt R Dale(Queensland University of Technology), Steinthorsdottir Valgerdur(deCODE Genetics (Iceland)), Kāri Stefánsson(deCODE Genetics (Iceland)), Velez-Edwards R Digna(Vanderbilt University Medical Center), Yurttas Beim Piraye(RGenix (United States)), Missmer A Stacey(Brigham and Women's Hospital), Montgomery W Grant(The University of Queensland), Morris P Andrew(Centre for Human Genetics), Krina T. Zondervan(Centre for Human Genetics)
bioRxiv (Cold Spring Harbor Laboratory)
September 7, 2018
10.1101/406967
Cited by 46Open Access
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Abstract

Abstract Endometriosis is a common complex inflammatory condition characterised by the presence of endometrium-like tissue outside the uterus, mainly in the pelvic area. It is associated with chronic pelvic pain and infertility, and its pathogenesis remains poorly understood. The disease is typically classified according to the revised American Fertility Society (rAFS) 4-stage surgical assessment system, although stage does not correlate well with symptomatology or prognosis. Previously identified genetic variants mainly are associated with stage III/IV disease, highlighting the need for further phenotype-stratified analysis that requires larger datasets. We conducted a meta-analysis of 15 genome-wide association studies (GWAS) and a replication analysis, including 58,115 cases and 733,480 controls in total, and sub-phenotype analyses of stage I/II, stage III/IV and infertility-associated endometriosis cases. This revealed 27 genetic loci associated with endometriosis at the genome-wide p-value threshold (P<5×10 −8 ), 13 of which are novel and an additional 8 novel genes identified from gene-based association analyses. Of the 27 loci, 21 (78%) had greater effect sizes in stage III/IV disease compared to stage I/II, 1 (4%) had greater effect size in stage I/II compared to stage III/IV and 17 (63%) had greater effect sizes when restricted to infertility-associated endometriosis cases compared to overall endometriosis. These results suggest that specific variants may confer risk for different sub-types of endometriosis through distinct pathways. Analyses of genetic variants underlying different pain symptoms reported in the UK Biobank showed that 7/9 had positive significant (p<1.28×10 3 ) positive genetic correlations with endometriosis, suggesting a genetic basis for sensitivity to pain in general. Additional conditions with significant positive genetic correlations with endometriosis included uterine fibroids, excessive and irregular menstrual bleeding, osteoarthritis, diabetes as well as menstrual cycle length and age at menarche. These results provide a basis for fine-mapping of the causal variants at these 27 loci, and for functional follow-up to understand their contribution to endometriosis and its potential subtypes.

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