GWAS Study

Genome-wide association study identifies 30 loci associated with bipolar disorder.

Name: DNAGENICS DNA Analysis Platform
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Author: DNAGENICS

Stahl EA, Breen G, Forstner AJ et al.

31043756 PubMed ID

GWAS Study Type

46237 Participants

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Chapter I

Publication Details

Comprehensive information about this research publication

Journal Nat Genet

Publication Date 2019-05-01

Disease/Trait Bipolar I disorder

DOI 10.1038/s41588-019-0397-8

ISSN 1546-1718

Authors

Stahl EA

Breen G

Forstner AJ

McQuillin A

Ripke S

Trubetskoy V

Mattheisen M

Wang Y

Coleman JRI

Gaspar HA

de Leeuw CA

Steinberg S

Pavlides JMW

Trzaskowski M

Byrne EM

Pers TH

Holmans PA

Richards AL

Abbott L

Agerbo E

Akil H

Albani D

Alliey-Rodriguez N

Als TD

Anjorin A

Antilla V

Awasthi S

Badner JA

Bækvad-Hansen M

Barchas JD

Bass N

Bauer M

Belliveau R

Bergen SE

Pedersen CB

Bøen E

Boks MP

Boocock J

Budde M

Bunney W

Burmeister M

Bybjerg-Grauholm J

Byerley W

Casas M

Cerrato F

Cervantes P

Chambert K

Charney AW

Chen D

Churchhouse C

Clarke TK

Coryell W

Craig DW

Cruceanu C

Curtis D

Czerski PM

Dale AM

de Jong S

Degenhardt F

Del-Favero J

DePaulo JR

Djurovic S

Dobbyn AL

Dumont A

Elvsåshagen T

Escott-Price V

Fan CC

Fischer SB

Flickinger M

Foroud TM

Forty L

Frank J

Fraser C

Freimer NB

Frisén L

Gade K

Gage D

Garnham J

Giambartolomei C

Pedersen MG

Goldstein J

Gordon SD

Gordon-Smith K

Green EK

Green MJ

Greenwood TA

Grove J

Guan W

Guzman-Parra J

Hamshere ML

Hautzinger M

Heilbronner U

Herms S

Hipolito M

Hoffmann P

Holland D

Huckins L

Jamain S

Johnson JS

Juréus A

Kandaswamy R

Karlsson R

Kennedy JL

Kittel-Schneider S

Knowles JA

Kogevinas M

Koller AC

Kupka R

Lavebratt C

Lawrence J

Lawson WB

Leber M

Lee PH

Levy SE

Li JZ

Liu C

Lucae S

Maaser A

MacIntyre DJ

Mahon PB

Maier W

Martinsson L

McCarroll S

McGuffin P

McInnis MG

McKay JD

Medeiros H

Medland SE

Meng F

Milani L

Montgomery GW

Morris DW

Mühleisen TW

Mullins N

Nguyen H

Nievergelt CM

Adolfsson AN

Nwulia EA

O'Donovan C

Loohuis LMO

Ori APS

Oruc L

ÖU

Ösby U

Perlis RH

Perry A

Pfennig A

Potash JB

Purcell SM

Regeer EJ

Reif A

Reinbold CS

Rice JP

Rivas F

Rivera M

Roussos P

Ruderfer DM

Ryu E

Sánchez-Mora C

Schatzberg AF

Scheftner WA

Schork NJ

Shannon Weickert C

Shehktman T

Shilling PD

Sigurdsson E

Slaney C

Smeland OB

Sobell JL

Søholm Hansen C

Spijker AT

St Clair D

Steffens M

Strauss JS

Streit F

Strohmaier J

Szelinger S

Thompson RC

Thorgeirsson TE

Treutlein J

Vedder H

Wang W

Watson SJ

Weickert TW

Witt SH

Xi S

Xu W

Young AH

Zandi P

Zhang P

Zöllner S

Adolfsson R

Agartz I

Alda M

Backlund L

Baune BT

Bellivier F

Berrettini WH

Biernacka JM

Blackwood DHR

Boehnke M

Børglum AD

Corvin A

Craddock N

Daly MJ

Dannlowski U

Esko T

Etain B

Frye M

Fullerton JM

Gershon ES

Gill M

Goes F

Grigoroiu-Serbanescu M

Hauser J

Hougaard DM

Hultman CM

Jones I

Jones LA

Kahn RS

Kirov G

Landén M

Leboyer M

Lewis CM

Li QS

Lissowska J

Martin NG

Mayoral F

McElroy SL

McIntosh AM

McMahon FJ

Melle I

Metspalu A

Mitchell PB

Morken G

Mors O

Mortensen PB

Müller-Myhsok B

Myers RM

Neale BM

Nimgaonkar V

Nordentoft M

Nöthen MM

O'Donovan MC

Oedegaard KJ

Owen MJ

Paciga SA

Pato C

Pato MT

Posthuma D

Ramos-Quiroga JA

Ribasés M

Rietschel M

Rouleau GA

Schalling M

Schofield PR

Schulze TG

Serretti A

Smoller JW

Stefansson H

Stefansson K

Stordal E

Sullivan PF

Turecki G

Vaaler AE

Vieta E

Vincent JB

Werge T

Nurnberger JI

Wray NR

Di Florio A

Edenberg HJ

Cichon S

Ophoff RA

Scott LJ

Andreassen OA

Kelsoe J

Sklar P

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Chapter II

Abstract

Summary of the research findings

Bipolar disorder is a highly heritable psychiatric disorder. We performed a genome-wide association study (GWAS) including 20,352 cases and 31,358 controls of European descent, with follow-up analysis of 822 variants with P < 1 × 10-4 in an additional 9,412 cases and 137,760 controls. Eight of the 19 variants that were genome-wide significant (P < 5 × 10-8) in the discovery GWAS were not genome-wide significant in the combined analysis, consistent with small effect sizes and limited power but also with genetic heterogeneity. In the combined analysis, 30 loci were genome-wide significant, including 20 newly identified loci. The significant loci contain genes encoding ion channels, neurotransmitter transporters and synaptic components. Pathway analysis revealed nine significantly enriched gene sets, including regulation of insulin secretion and endocannabinoid signaling. Bipolar I disorder is strongly genetically correlated with schizophrenia, driven by psychosis, whereas bipolar II disorder is more strongly correlated with major depressive disorder. These findings address key clinical questions and provide potential biological mechanisms for bipolar disorder.

14,879 European ancestry cases, 31,358 European ancestry controls

Chapter III

Study Statistics

Key metrics and study information

46237

Total Participants

GWAS

Study Type

Yes

Replicated

9,412 European ancestry cases, 137,760 European ancestry controls

Replication Participants

European

Ancestry

Canada, U.S., Australia, France, Germany, Netherlands, Bulgaria, Poland, Romania, Republic of Ireland, Norway, Sweden, U.K., Spain, Denmark, Iceland

Recruitment Country

Chapter IV

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Genome-wide association study identifies 30 loci associated with bipolar disorder.

Publication Details

Authors

Abstract

Study Statistics

AI-Generated Summary

AI Summary In Progress

Summary

Key Findings

Health Insights

Disease Analysis

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Clinical Relevance

Explore More Research

Genome-wide association study identifies 30 loci associated with bipolar disorder.

Publication Details

Authors

Abstract

Study Statistics

AI-Generated Summary

AI Summary In Progress

Summary

Key Findings

Health Insights

Disease Analysis

Genetic Trait Analysis

Clinical Relevance

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