A methylome-wide association study of major depression with out-of-sample case-control classification and trans-ancestry comparison
Author:
Shen XueyiORCID, Barbu MirunaORCID, Caramaschi DorettaORCID, Arathimos RyanORCID, Czamara DarinaORCID, David Friederike S.ORCID, Dearman AnnaORCID, Dilkes EvelynORCID, Herrera-Rivero MarisolORCID, Huider FlorisORCID, Kühn LuiseORCID, Lu Kuan-Chen, Palviainen TeemuORCID, Schowe Alicia MarieORCID, Shireby GemmaORCID, Weihs AntoineORCID, Wong Chloe C. Y.ORCID, Davyson EleanorORCID, Casey HannahORCID, Adams Mark JORCID, Allgaier Antje-KathrinORCID, Barber Michael, Burrage Joe, Caspi AvshalomORCID, Costeira RicardoORCID, Dunn Erin C.ORCID, Feldmann Lisa, Frank JosefORCID, Freisleder Franz Joseph, Gadd Danni A.ORCID, Greimel EllenORCID, Hannon EilisORCID, Harris Sarah EORCID, Homuth GeorgORCID, Howard David M.ORCID, Iurato Stella, Korhonen TellervoORCID, Lu Tzu-Pin, Martin Nicholas GORCID, Martins JadeORCID, McDermott Edel, Meinert Susanne, Navarro PauORCID, Ollikainen MiinaORCID, Pehl Verena, Piechaczek Charlotte, Scherff Aline D.ORCID, Stein Frederike, Streit FabianORCID, Teumer AlexanderORCID, Völzke Henry, van Dongen JennyORCID, Walker Rosie M.ORCID, Yusupov Natan, Arseneault LouiseORCID, Bell Jordana T.ORCID, Berger KlausORCID, Binder ElisabethORCID, Boomsma Dorret I.ORCID, Cox Simon RORCID, Dannlowski UdoORCID, Evans Kathryn L.ORCID, Fisher Helen L.ORCID, Forstner Andreas J.ORCID, Grabe Hans J., Kaprio JaakkoORCID, Kircher TiloORCID, Kopf-Beck JohannesORCID, Kumari MeenaORCID, Kuo Po-HsiuORCID, Li Qingqin SORCID, Moffitt Terrie E.ORCID, Mulcahy Hugh, Murphy Therese M.ORCID, Schulte-Körne GerdORCID, Mill JonathanORCID, Lewis Cathryn M.ORCID, Group OPTIMA Working, Wray Naomi RORCID, McIntosh Andrew MORCID, ,
Abstract
AbstractMajor Depression (MD) is a leading cause of global disease burden, and both experimental and population-based studies suggest that differences in DNA methylation (DNAm) may be associated with the condition. However, previous DNAm studies have not so far been widely replicated, suggesting a need for larger meta-analysis studies. In the present study, the Psychiatric Genomics Consortium Major Depressive Disorder working group conducted a meta-analysis of methylome-wide association analysis (MWAS) for life-time MD across 18 studies of 24,754 European-ancestry participants (5,443 MD cases) and an East Asian sample (243 cases, 1846 controls). We identified fifteen CpG sites associated with lifetime MD with methylome-wide significance (p < 6.42×10-8). Top CpG effect sizes in European ancestries were positively correlated with those from an independent East Asian MWAS (r = 0.482 and p = 0.068 for significant CpG sites, r = 0.261 and p = 0.009 for the top 100 CpG sites). Methylation score (MS) created using the MWAS summary statistics was significantly associated with MD status in an out-of-sample classification analysis (β = 0.122, p = 0.005, AUC = 0.53). MS was also associated with five inflammatory markers, with the strongest association found with Tumor Necrosis Factor Beta (β=-0.154, p=1.5×10-5). Mendelian randomisation (MR) analysis demonstrated that 23 CpG sites were potentially causally associated with MD and six of those were replicated in an independent mQTL dataset (Wald’s ratio test, absolute β ranged from 0.056 to 0.932, p ranged from 7×10-3to 4.58×10-6). CpG sites located in the Major Histocompatibility complex (MHC) region showed the strongest evidence from MR analysis of being associated with MD. Our study provides evidence that variations in DNA methylation are associated with MD, and further evidence supporting involvement of the immune system. Larger sample sizes in diverse ancestries are likely to reveal replicable associations to improve mechanistic inferences with the potential to inform molecular target identification.
Publisher
Cold Spring Harbor Laboratory
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