Genome-wide meta-analysis of depression identifies 102 independent variants and highlights the importance of the prefrontal brain regions

David M. Howard; Mark J. Adams; Toni‐Kim Clarke; Jonathan D. Hafferty; Jude Gibson; Masoud Shirali; Jonathan R. I. Coleman; Saskia P. Hagenaars; Joey Ward; Eleanor M. Wigmore; Clara Alloza; Xueyi Shen; Miruna C. Barbu; Eileen Y. Xu; Heather C. Whalley; Riccardo E. Marioni; David J. Porteous; Gail Davies; Ian J. Deary; Gibran Hemani; Klaus Berger; Henning Teismann; Rajesh Rawal; Volker Arolt; Bernhard T. Baune; Udo Dannlowski; Katharina Domschke; Chao Tian; David A. Hinds; Maciej Trzaskowski; Enda M. Byrne; Stephan Ripke; Daniel J. Smıth; Patrick F. Sullivan; Naomi R. Wray; Gerome Breen; Cathryn M. Lewis; Andrew M. McIntosh

doi:10.1038/s41593-018-0326-7

Genome-wide meta-analysis of depression identifies 102 independent variants and highlights the importance of the prefrontal brain regions

David M. Howard(Royal Edinburgh Hospital), Mark J. Adams(Royal Edinburgh Hospital), Toni‐Kim Clarke(Royal Edinburgh Hospital), Jonathan D. Hafferty(Royal Edinburgh Hospital), Jude Gibson(Royal Edinburgh Hospital), Masoud Shirali(Royal Edinburgh Hospital), Jonathan R. I. Coleman(King's College London), Saskia P. Hagenaars(King's College London), Joey Ward(University of Glasgow), Eleanor M. Wigmore(Royal Edinburgh Hospital), Clara Alloza(Royal Edinburgh Hospital), Xueyi Shen(Royal Edinburgh Hospital), Miruna C. Barbu(Royal Edinburgh Hospital), Eileen Y. Xu(Royal Edinburgh Hospital), Heather C. Whalley(Royal Edinburgh Hospital), Riccardo E. Marioni(University of Edinburgh), David J. Porteous(University of Edinburgh), Gail Davies(University of Edinburgh), Ian J. Deary(University of Edinburgh), Gibran Hemani(University of Bristol), Klaus Berger(University of Münster), Henning Teismann(University of Münster), Rajesh Rawal(University of Münster), Volker Arolt(University of Münster), Bernhard T. Baune(The University of Melbourne), Udo Dannlowski(University of Münster), Katharina Domschke(University of Freiburg), Chao Tian(23andMe (United States)), David A. Hinds(23andMe (United States)), Maciej Trzaskowski(The University of Queensland), Enda M. Byrne(The University of Queensland), Stephan Ripke(Broad Institute), Daniel J. Smıth(University of Glasgow), Patrick F. Sullivan(University of North Carolina at Chapel Hill), Naomi R. Wray(The University of Queensland), Gerome Breen(King's College London), Cathryn M. Lewis(King's College London), Andrew M. McIntosh(Royal Edinburgh Hospital)

Nature Neuroscience

February 4, 2019

10.1038/s41593-018-0326-7

Cited by 2,773Open Access

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Abstract

Major depression is a debilitating psychiatric illness that is typically associated with low mood and anhedonia. Depression has a heritable component that has remained difficult to elucidate with current sample sizes due to the polygenic nature of the disorder. To maximize sample size, we meta-analyzed data on 807,553 individuals (246,363 cases and 561,190 controls) from the three largest genome-wide association studies of depression. We identified 102 independent variants, 269 genes, and 15 genesets associated with depression, including both genes and gene pathways associated with synaptic structure and neurotransmission. An enrichment analysis provided further evidence of the importance of prefrontal brain regions. In an independent replication sample of 1,306,354 individuals (414,055 cases and 892,299 controls), 87 of the 102 associated variants were significant after multiple testing correction. These findings advance our understanding of the complex genetic architecture of depression and provide several future avenues for understanding etiology and developing new treatment approaches.

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