Trans-ancestry genome-wide study of depression identifies 697 associations implicating cell types and pharmacotherapies

Andrew M. Mcintosh; Cathryn M. Lewis; Mark J. Adams; Fabian Streit; Xiangrui Meng; Swapnil Awasthi; Brett N. Adey; Karmel W. Choi; V. Kartik Chundru; Jonathan R. I. Coleman; Bart Ferwerda; Jerome C. Foo; Zachary F. Gerring; Olga Giannakopoulou; Priya Gupta; Alisha S. M. Hall; Arvid Harder; David M. Howard; Christopher Hubel; Alex S. F. Kwong; Daniel F. Levey; Brittany L. Mitchell; Guiyan Ni; Vanessa K. Ota; Oliver Pain; Gita A. Pathak; Eva C. Schulte; Xueyi Shen; Jackson G. Thorp; Alicia Walker; Shuyang Yao; Jian Zeng; Johan Zvrskovec; Dag Aarsland; Ky'Era V. Actkins; Mazda Adli; Esben Agerbo; Mareike Aichholzer; Allison Aiello; Tracy M. Air; Thomas D. Als; Evelyn Andersson; Till F. M. Andlauer; Volker Arolt; Helga Ask; Julia Backman; Sunita Badola; Clive Ballard; Karina Banasik; Major Depressive Disorder Working Group of the Psychiatric Genomics Consortium; Jurjen J. Luykx

doi:10.1016/j.cell.2024.12.002

Trans-ancestry genome-wide study of depression identifies 697 associations implicating cell types and pharmacotherapies

Andrew M. Mcintosh^*
, Cathryn M. Lewis^*
, Mark J. Adams
, Fabian Streit
, Xiangrui Meng
, Swapnil Awasthi
, Brett N. Adey
, Karmel W. Choi
, V. Kartik Chundru
, Jonathan R. I. Coleman
, Bart Ferwerda
, Jerome C. Foo
, Zachary F. Gerring
, Olga Giannakopoulou
, Priya Gupta
, Alisha S. M. Hall
, Arvid Harder
, David M. Howard
, Christopher Hubel
, Alex S. F. Kwong

Daniel F. Levey, Brittany L. Mitchell, Guiyan Ni, Vanessa K. Ota, Oliver Pain, Gita A. Pathak, Eva C. Schulte, Xueyi Shen, Jackson G. Thorp, Alicia Walker, Shuyang Yao, Jian Zeng, Johan Zvrskovec, Dag Aarsland, Ky'Era V. Actkins, Mazda Adli, Esben Agerbo, Mareike Aichholzer, Allison Aiello, Tracy M. Air, Thomas D. Als, Evelyn Andersson, Till F. M. Andlauer, Volker Arolt, Helga Ask, Julia Backman, Sunita Badola, Clive Ballard, Karina Banasik, Major Depressive Disorder Working Group of the Psychiatric Genomics Consortium, Jurjen J. Luykx

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

In a genome-wide association study (GWAS) meta-analysis of 688,808 individuals with major depression (MD) and 4,364,225 controls from 29 countries across diverse and admixed ancestries, we identify 697 associations at 635 loci, 293 of which are novel. Using fine-mapping and functional tools, we find 308 high-confidence gene associations and enrichment of postsynaptic density and receptor clustering. A neural cell-type enrichment analysis utilizing single-cell data implicates excitatory, inhibitory, and medium spiny neurons and the involvement of amygdala neurons in both mouse and human single-cell analyses. The associations are enriched for antidepressant targets and provide potential repurposing opportunities. Polygenic scores trained using European or multi-ancestry data predicted MD status across all ancestries, explaining up to 5.8% of MD liability variance in Europeans. These findings advance our global understanding of MD and reveal biological targets that may be used to target and develop pharmacotherapies addressing the unmet need for effective treatment.

Original language	English
Pages (from-to)	640-652.e9
Number of pages	23
Journal	Cell
Volume	188
Issue number	3
Early online date	1 Feb 2025
DOIs	https://doi.org/10.1016/j.cell.2024.12.002
Publication status	Published - 6 Feb 2025
Externally published	Yes

Keywords

GENERALIZED ANXIETY DISORDER
HIPPOCAMPAL NEUROGENESIS
PREGABALIN AUGMENTATION
MAJOR DEPRESSION
GENE-EXPRESSION
ANTIDEPRESSANTS
METAANALYSIS
LOCI
HERITABILITY
REWARD

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Mcintosh, A. M., Lewis, C. M., Adams, M. J., Streit, F., Meng, X., Awasthi, S., Adey, B. N., Choi, K. W., Chundru, V. K., Coleman, J. R. I., Ferwerda, B., Foo, J. C., Gerring, Z. F., Giannakopoulou, O., Gupta, P., Hall, A. S. M., Harder, A., Howard, D. M., Hubel, C., ... Luykx, J. J. (2025). Trans-ancestry genome-wide study of depression identifies 697 associations implicating cell types and pharmacotherapies. Cell, 188(3), 640-652.e9. https://doi.org/10.1016/j.cell.2024.12.002

@article{8138f494a6134082ab5ebf3e3eb5103a,

title = "Trans-ancestry genome-wide study of depression identifies 697 associations implicating cell types and pharmacotherapies",

abstract = "In a genome-wide association study (GWAS) meta-analysis of 688,808 individuals with major depression (MD) and 4,364,225 controls from 29 countries across diverse and admixed ancestries, we identify 697 associations at 635 loci, 293 of which are novel. Using fine-mapping and functional tools, we find 308 high-confidence gene associations and enrichment of postsynaptic density and receptor clustering. A neural cell-type enrichment analysis utilizing single-cell data implicates excitatory, inhibitory, and medium spiny neurons and the involvement of amygdala neurons in both mouse and human single-cell analyses. The associations are enriched for antidepressant targets and provide potential repurposing opportunities. Polygenic scores trained using European or multi-ancestry data predicted MD status across all ancestries, explaining up to 5.8\% of MD liability variance in Europeans. These findings advance our global understanding of MD and reveal biological targets that may be used to target and develop pharmacotherapies addressing the unmet need for effective treatment.",

keywords = "GENERALIZED ANXIETY DISORDER, HIPPOCAMPAL NEUROGENESIS, PREGABALIN AUGMENTATION, MAJOR DEPRESSION, GENE-EXPRESSION, ANTIDEPRESSANTS, METAANALYSIS, LOCI, HERITABILITY, REWARD",

author = "Mcintosh, \{Andrew M.\} and Lewis, \{Cathryn M.\} and Adams, \{Mark J.\} and Fabian Streit and Xiangrui Meng and Swapnil Awasthi and Adey, \{Brett N.\} and Choi, \{Karmel W.\} and Chundru, \{V. Kartik\} and Coleman, \{Jonathan R. I.\} and Bart Ferwerda and Foo, \{Jerome C.\} and Gerring, \{Zachary F.\} and Olga Giannakopoulou and Priya Gupta and Hall, \{Alisha S. M.\} and Arvid Harder and Howard, \{David M.\} and Christopher Hubel and Kwong, \{Alex S. F.\} and Levey, \{Daniel F.\} and Mitchell, \{Brittany L.\} and Guiyan Ni and Ota, \{Vanessa K.\} and Oliver Pain and Pathak, \{Gita A.\} and Schulte, \{Eva C.\} and Xueyi Shen and Thorp, \{Jackson G.\} and Alicia Walker and Shuyang Yao and Jian Zeng and Johan Zvrskovec and Dag Aarsland and Actkins, \{Ky'Era V.\} and Mazda Adli and Esben Agerbo and Mareike Aichholzer and Allison Aiello and Air, \{Tracy M.\} and Als, \{Thomas D.\} and Evelyn Andersson and Andlauer, \{Till F. M.\} and Volker Arolt and Helga Ask and Julia Backman and Sunita Badola and Clive Ballard and Karina Banasik and \{Major Depressive Disorder Working Group of the Psychiatric Genomics Consortium\} and Luykx, \{Jurjen J.\}",

year = "2025",

month = feb,

day = "6",

doi = "10.1016/j.cell.2024.12.002",

language = "English",

volume = "188",

pages = "640--652.e9",

journal = "Cell",

issn = "0092-8674",

publisher = "Elsevier B.V.",

number = "3",

}

Mcintosh, AM, Lewis, CM, Adams, MJ, Streit, F, Meng, X, Awasthi, S, Adey, BN, Choi, KW, Chundru, VK, Coleman, JRI, Ferwerda, B, Foo, JC, Gerring, ZF, Giannakopoulou, O, Gupta, P, Hall, ASM, Harder, A, Howard, DM, Hubel, C, Kwong, ASF, Levey, DF, Mitchell, BL, Ni, G, Ota, VK, Pain, O, Pathak, GA, Schulte, EC, Shen, X, Thorp, JG, Walker, A, Yao, S, Zeng, J, Zvrskovec, J, Aarsland, D, Actkins, KEV, Adli, M, Agerbo, E, Aichholzer, M, Aiello, A, Air, TM, Als, TD, Andersson, E, Andlauer, TFM, Arolt, V, Ask, H, Backman, J, Badola, S, Ballard, C, Banasik, K, Major Depressive Disorder Working Group of the Psychiatric Genomics Consortium & Luykx, JJ 2025, 'Trans-ancestry genome-wide study of depression identifies 697 associations implicating cell types and pharmacotherapies', Cell, vol. 188, no. 3, pp. 640-652.e9. https://doi.org/10.1016/j.cell.2024.12.002

TY - JOUR

T1 - Trans-ancestry genome-wide study of depression identifies 697 associations implicating cell types and pharmacotherapies

AU - Mcintosh, Andrew M.

AU - Lewis, Cathryn M.

AU - Adams, Mark J.

AU - Streit, Fabian

AU - Meng, Xiangrui

AU - Awasthi, Swapnil

AU - Adey, Brett N.

AU - Choi, Karmel W.

AU - Chundru, V. Kartik

AU - Coleman, Jonathan R. I.

AU - Ferwerda, Bart

AU - Foo, Jerome C.

AU - Gerring, Zachary F.

AU - Giannakopoulou, Olga

AU - Gupta, Priya

AU - Hall, Alisha S. M.

AU - Harder, Arvid

AU - Howard, David M.

AU - Hubel, Christopher

AU - Kwong, Alex S. F.

AU - Levey, Daniel F.

AU - Mitchell, Brittany L.

AU - Ni, Guiyan

AU - Ota, Vanessa K.

AU - Pain, Oliver

AU - Pathak, Gita A.

AU - Schulte, Eva C.

AU - Shen, Xueyi

AU - Thorp, Jackson G.

AU - Walker, Alicia

AU - Yao, Shuyang

AU - Zeng, Jian

AU - Zvrskovec, Johan

AU - Aarsland, Dag

AU - Actkins, Ky'Era V.

AU - Adli, Mazda

AU - Agerbo, Esben

AU - Aichholzer, Mareike

AU - Aiello, Allison

AU - Air, Tracy M.

AU - Als, Thomas D.

AU - Andersson, Evelyn

AU - Andlauer, Till F. M.

AU - Arolt, Volker

AU - Ask, Helga

AU - Backman, Julia

AU - Badola, Sunita

AU - Ballard, Clive

AU - Banasik, Karina

AU - Major Depressive Disorder Working Group of the Psychiatric Genomics Consortium

AU - Luykx, Jurjen J.

PY - 2025/2/6

Y1 - 2025/2/6

N2 - In a genome-wide association study (GWAS) meta-analysis of 688,808 individuals with major depression (MD) and 4,364,225 controls from 29 countries across diverse and admixed ancestries, we identify 697 associations at 635 loci, 293 of which are novel. Using fine-mapping and functional tools, we find 308 high-confidence gene associations and enrichment of postsynaptic density and receptor clustering. A neural cell-type enrichment analysis utilizing single-cell data implicates excitatory, inhibitory, and medium spiny neurons and the involvement of amygdala neurons in both mouse and human single-cell analyses. The associations are enriched for antidepressant targets and provide potential repurposing opportunities. Polygenic scores trained using European or multi-ancestry data predicted MD status across all ancestries, explaining up to 5.8% of MD liability variance in Europeans. These findings advance our global understanding of MD and reveal biological targets that may be used to target and develop pharmacotherapies addressing the unmet need for effective treatment.

AB - In a genome-wide association study (GWAS) meta-analysis of 688,808 individuals with major depression (MD) and 4,364,225 controls from 29 countries across diverse and admixed ancestries, we identify 697 associations at 635 loci, 293 of which are novel. Using fine-mapping and functional tools, we find 308 high-confidence gene associations and enrichment of postsynaptic density and receptor clustering. A neural cell-type enrichment analysis utilizing single-cell data implicates excitatory, inhibitory, and medium spiny neurons and the involvement of amygdala neurons in both mouse and human single-cell analyses. The associations are enriched for antidepressant targets and provide potential repurposing opportunities. Polygenic scores trained using European or multi-ancestry data predicted MD status across all ancestries, explaining up to 5.8% of MD liability variance in Europeans. These findings advance our global understanding of MD and reveal biological targets that may be used to target and develop pharmacotherapies addressing the unmet need for effective treatment.

KW - GENERALIZED ANXIETY DISORDER

KW - HIPPOCAMPAL NEUROGENESIS

KW - PREGABALIN AUGMENTATION

KW - MAJOR DEPRESSION

KW - GENE-EXPRESSION

KW - ANTIDEPRESSANTS

KW - METAANALYSIS

KW - LOCI

KW - HERITABILITY

KW - REWARD

U2 - 10.1016/j.cell.2024.12.002

DO - 10.1016/j.cell.2024.12.002

M3 - Article

SN - 0092-8674

VL - 188

SP - 640-652.e9

JO - Cell

JF - Cell

IS - 3

ER -

Trans-ancestry genome-wide study of depression identifies 697 associations implicating cell types and pharmacotherapies

Abstract

Keywords

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