The Landscape of Shared and Divergent Genetic Influences across 14 Psychiatric Disorders

dc.contributor.authorGrotzinger, Andrew D.
dc.contributor.authorWerme, Josefin
dc.contributor.authorPeyrot, Wouter J.
dc.contributor.authorFrei, Oleksandr
dc.contributor.authorde Leeuw, Christiaan
dc.contributor.authorBicks, Lucy K.
dc.contributor.authorGuo, Qiuyu
dc.contributor.authorMargolis, Michael P.
dc.contributor.authorCoombes, Brandon J.
dc.contributor.authorBatzler, Anthony
dc.contributor.authorPazdernik, Vanessa
dc.contributor.authorBiernacka, Joanna M.
dc.contributor.authorAndreassen, Ole A.
dc.contributor.authorAnttila, Verneri
dc.contributor.authorBørglum, Anders D.
dc.contributor.authorCai, Na
dc.contributor.authorDemontis, Ditte
dc.contributor.authorEdenberg, Howard J.
dc.contributor.authorFaraone, Stephen V.
dc.contributor.authorFranke, Barbara
dc.contributor.authorGandal, Michael J.
dc.contributor.authorGelernter, Joel
dc.contributor.authorHettema, John M.
dc.contributor.authorJonas, Katherine G.
dc.contributor.authorKnowles, James A.
dc.contributor.authorKoenen, Karestan C.
dc.contributor.authorMaihofer, Adam X.
dc.contributor.authorMallard, Travis T.
dc.contributor.authorMattheisen, Manuel
dc.contributor.authorMitchell, Karen S.
dc.contributor.authorNeale, Benjamin M.
dc.contributor.authorNievergelt, Caroline M.
dc.contributor.authorNurnberger, John I.
dc.contributor.authorO'Connell, Kevin S.
dc.contributor.authorRobinson, Elise B.
dc.contributor.authorSanchez-Roige, Sandra S.
dc.contributor.authorSantangelo, Susan L.
dc.contributor.authorStefansson, Hreinn
dc.contributor.authorStefansson, Kari
dc.contributor.authorStein, Murray B.
dc.contributor.authorStrom, Nora I.
dc.contributor.authorThornton, Laura M.
dc.contributor.authorTucker-Drob, Elliot M.
dc.contributor.authorVerhulst, Brad
dc.contributor.authorWaldman, Irwin D.
dc.contributor.authorWalters, G. Bragi
dc.contributor.authorWray, Naomi R.
dc.contributor.authorAnxiety Disorders Working Group
dc.contributor.authorAttention-Deficit/Hyperactivity Disorder (ADHD) Working Group
dc.contributor.authorAutism Spectrum Disorders Working Group
dc.contributor.authorBipolar Disorder Working Group
dc.contributor.authorEating Disorders Working Group
dc.contributor.authorMajor Depressive Disorder Working Group
dc.contributor.authorNicotine Dependence GenOmics (iNDiGO) Consortium
dc.contributor.authorObsessive-Compulsive Disorder Working Group
dc.contributor.authorPost-Traumatic Stress Disorder Working Group
dc.contributor.authorSchizophrenia Working Group
dc.contributor.authorSubstance Use Disorders Working Group
dc.contributor.authorTourette Syndrome Working Group
dc.contributor.authorLee, Phil H.
dc.contributor.authorKendler, Kenneth S.
dc.contributor.authorSmoller, Jordan W.
dc.contributor.departmentBiochemistry and Molecular Biology, School of Medicine
dc.date.accessioned2025-07-15T12:26:05Z
dc.date.available2025-07-15T12:26:05Z
dc.date.issued2025-01-15
dc.description.abstractPsychiatric disorders display high levels of comorbidity and genetic overlap 1,2. Genomic methods have shown that even for schizophrenia and bipolar disorder, two disorders long-thought to be etiologically distinct 3, the majority of genetic signal is shared 4. Furthermore, recent cross-disorder analyses have uncovered over a hundred pleiotropic loci shared across eight disorders 5. However, the full scope of shared and disorder-specific genetic basis of psychopathology remains largely uncharted. Here, we address this gap by triangulating across a suite of cutting-edge statistical genetic and functional genomic analyses applied to 14 childhood- and adult-onset psychiatric disorders (1,056,201 cases). Our analyses identify and characterize five underlying genomic factors 6 that explain the majority of the genetic variance of the individual disorders (~66% on average) and are associated with 268 pleiotropic loci. We observed particularly high levels of polygenic overlap 7 and local genetic correlation 8 and very few disorder-specific loci 9 for two factors defined by: (i) schizophrenia and bipolar disorder ("SB factor"), and by (ii) major depression, PTSD, and anxiety ("internalizing factor"). At the functional level, we applied multiple methods 10-12 which demonstrated that the shared genetic signal across the SB factor was substantially enriched in genes expressed in excitatory neurons, whereas the internalizing factor was associated with oligodendrocyte biology. By comparison, the genetic signal shared across all 14 disorders was enriched for broad biological processes (e.g., transcriptional regulation). These results indicate increasing differentiation of biological function at different levels of shared cross-disorder risk, from quite general vulnerability to more specific pathways associated with subsets of disorders. These observations may inform a more neurobiologically valid psychiatric nosology and implicate novel targets for therapeutic developments designed to treat commonly occurring comorbid presentations.
dc.eprint.versionPreprint
dc.identifier.citationGrotzinger AD, Werme J, Peyrot WJ, et al. The Landscape of Shared and Divergent Genetic Influences across 14 Psychiatric Disorders. Preprint. medRxiv. 2025;2025.01.14.25320574. Published 2025 Jan 15. doi:10.1101/2025.01.14.25320574
dc.identifier.urihttps://hdl.handle.net/1805/49474
dc.language.isoen_US
dc.publishermedRxiv
dc.relation.isversionof10.1101/2025.01.14.25320574
dc.rightsAttribution-NonCommercial-NoDerivatives 4.0 Internationalen
dc.rights.urihttp://creativecommons.org/licenses/by-nc-nd/4.0/
dc.sourcePMC
dc.subjectPsychiatric disorders
dc.subjectComorbidity
dc.subjectGenetic overlap
dc.subjectCross-disorder risk
dc.titleThe Landscape of Shared and Divergent Genetic Influences across 14 Psychiatric Disorders
dc.typeArticle
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