Genetic identification of cell types underlying brain complex traits yields insights into the etiology of Parkinson's disease

Julien Bryois; Patrick F Sullivan; Eating Disorders Working Group of the Psychiatric Genomics Consortium; B. Lin; P. Eline Slagboom; M.C.T. op Landt Slof; D.I. Boomsma; Lannie Ligthart; Danielle Posthuma

doi:10.1038/s41588-020-0610-9

Genetic identification of cell types underlying brain complex traits yields insights into the etiology of Parkinson's disease

Julien Bryois, Patrick F Sullivan, Eating Disorders Working Group of the Psychiatric Genomics Consortium, B. Lin, P. Eline Slagboom, M.C.T. op Landt Slof, D.I. Boomsma, Lannie Ligthart, Danielle Posthuma

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Abstract

Genome-wide association studies have discovered hundreds of loci associated with complex brain disorders, but it remains unclear in which cell types these loci are active. Here we integrate genome-wide association study results with single-cell transcriptomic data from the entire mouse nervous system to systematically identify cell types underlying brain complex traits. We show that psychiatric disorders are predominantly associated with projecting excitatory and inhibitory neurons. Neurological diseases were associated with different cell types, which is consistent with other lines of evidence. Notably, Parkinson's disease was genetically associated not only with cholinergic and monoaminergic neurons (which include dopaminergic neurons) but also with enteric neurons and oligodendrocytes. Using post-mortem brain transcriptomic data, we confirmed alterations in these cells, even at the earliest stages of disease progression. Our study provides an important framework for understanding the cellular basis of complex brain maladies, and reveals an unexpected role of oligodendrocytes in Parkinson's disease.

Original language	English
Pages (from-to)	482-493
Number of pages	12
Journal	Nature Genetics
Volume	52
Issue number	5
Early online date	27 Apr 2020
DOIs	https://doi.org/10.1038/s41588-020-0610-9
Publication status	Published - May 2020

Funding

J.B. was funded by a grant from the Swiss National Science Foundation (P400PB_180792). N.G.S. was supported by the Wellcome Trust (108726/Z/15/Z). N.G.S. and L.B. performed part of the work at the Systems Genetics of Neurodegeneration summer school funded by BMBF as part of the e:Med programme (FKZ 01ZX1704). J.H.-L. was funded by the Swedish Research Council (Vetenskapsr\u00E5det, award 2014-3863), StratNeuro, the Wellcome Trust (108726/Z/15/Z) and the Swedish Brain Foundation (Hj\u00E4rnfonden). P.F.S. was supported by the Swedish Research Council (Vetenskapsr\u00E5det, award D0886501), the Horizon 2020 Program of the European Union (COSYN, RIA grant agreement no. 610307) and US NIMH (U01 MH109528 and R01 MH077139). E.A. was supported by the Swedish Research Council (VR 2016-01526), Swedish Foundation for Strategic Research (SLA SB16-0065), Karolinska Institutet (SFO Strat. Regen., Senior grant 2018), Cancerfonden (CAN 2016/572), Hj\u00E4rnfonden (FO2017-0059) and Chen Zuckeberg Initiative: Neurodegeneration Challenge Network (2018-191929-5022). C.M.B. acknowledges funding from the Swedish Research Council (Vetenskapsr\u00E5det, award: 538-2013-8864) and the Klarman Family Foundation. This work is supported by the UK Dementia Research Institute, which receives its funding from UK DRI Ltd, funded by the UK Medical Research Council, Alzheimer\u2019s Society and Alzheimer\u2019s Research UK. We thank the research participants from 23andMe and other cohorts for their contribution to this study. P.F.S. reports the following potentially competing financial interests: current\u2014Lundbeck (advisory committee, grant recipient); past three years\u2014Pfizer (scientific advisory board), Element Genomics (consultation fee) and Roche (speaker reimbursement). C.M.B. reports: Shire (grant recipient, Scientific Advisory Board member); Pearson and Walker (author, royalty recipient).

Funders	Funder number
COSYN
Cancerfonden	CAN 2016/57
Hjärnfonden	FO2017-0059
Horizon 2020 Framework Programme	RIA grant agreement n° 610307
Karolinska Institutet	SFO Strat. Regen, Senior grant 2018
National Institute of Mental Health	MH077139
Schweizerischer Nationalfonds zur Förderung der Wissenschaftlichen Forschung
Stiftelsen för Strategisk Forskning
Swedish Brain Foundation	D0886501
UK Medical Research Council
US NIMH	R01 MH077139, U01 MH109528
Vetenskapsrådet
Wellcome Trust Centre for Mitochondrial Research
National Institute of General Medical Sciences	T32GM007337
Roche
Klarman Family Foundation
Wellcome Trust	108726/Z/15/Z
European Commission
Royal Irish Academy	610307
Schweizerischer Nationalfonds zur Förderung der Wissenschaftlichen Forschung	P400PB_180792
Stiftelsen för Strategisk Forskning	SLA SB16-0065
Alzheimer’s Research UK
Bundesministerium für Bildung und Forschung	FKZ 01ZX1704
Karolinska Institutet	538-2013-8864
Vetenskapsrådet	2014-3863, VR 2016-01526
Horizon 2020
Alzheimer’s Society
UK Dementia Research Institute

Cohort Studies

Netherlands Twin Register (NTR)

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1038/s41588-020-0610-9

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Bryois, J., Sullivan, P. F., Eating Disorders Working Group of the Psychiatric Genomics Consortium, Lin, B., Slagboom, P. E., op Landt Slof, M. C. T., Boomsma, D. I., Ligthart, L., & Posthuma, D. (2020). Genetic identification of cell types underlying brain complex traits yields insights into the etiology of Parkinson's disease. Nature Genetics, 52(5), 482-493. https://doi.org/10.1038/s41588-020-0610-9

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abstract = "Genome-wide association studies have discovered hundreds of loci associated with complex brain disorders, but it remains unclear in which cell types these loci are active. Here we integrate genome-wide association study results with single-cell transcriptomic data from the entire mouse nervous system to systematically identify cell types underlying brain complex traits. We show that psychiatric disorders are predominantly associated with projecting excitatory and inhibitory neurons. Neurological diseases were associated with different cell types, which is consistent with other lines of evidence. Notably, Parkinson's disease was genetically associated not only with cholinergic and monoaminergic neurons (which include dopaminergic neurons) but also with enteric neurons and oligodendrocytes. Using post-mortem brain transcriptomic data, we confirmed alterations in these cells, even at the earliest stages of disease progression. Our study provides an important framework for understanding the cellular basis of complex brain maladies, and reveals an unexpected role of oligodendrocytes in Parkinson's disease.",

author = "Julien Bryois and Skene, {Nathan G} and Hansen, {Thomas Folkmann} and Kogelman, {Lisette J A} and Watson, {Hunna J} and Zijing Liu and Leo Brueggeman and Gerome Breen and Bulik, {Cynthia M} and Ernest Arenas and Jens Hjerling-Leffler and Sullivan, {Patrick F} and {Eating Disorders Working Group of the Psychiatric Genomics Consortium} and B. Lin and Slagboom, {P. Eline} and {op Landt Slof}, M.C.T. and D.I. Boomsma and Lannie Ligthart and Danielle Posthuma",

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Bryois, J, Sullivan, PF, Eating Disorders Working Group of the Psychiatric Genomics Consortium, Lin, B, Slagboom, PE, op Landt Slof, MCT, Boomsma, DI , Ligthart, L & Posthuma, D 2020, 'Genetic identification of cell types underlying brain complex traits yields insights into the etiology of Parkinson's disease', Nature Genetics, vol. 52, no. 5, pp. 482-493. https://doi.org/10.1038/s41588-020-0610-9

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AU - Watson, Hunna J

AU - Liu, Zijing

AU - Brueggeman, Leo

AU - Breen, Gerome

AU - Bulik, Cynthia M

AU - Arenas, Ernest

AU - Hjerling-Leffler, Jens

AU - Sullivan, Patrick F

AU - Eating Disorders Working Group of the Psychiatric Genomics Consortium

AU - Lin, B.

AU - Slagboom, P. Eline

AU - op Landt Slof, M.C.T.

AU - Boomsma, D.I.

AU - Ligthart, Lannie

AU - Posthuma, Danielle

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AB - Genome-wide association studies have discovered hundreds of loci associated with complex brain disorders, but it remains unclear in which cell types these loci are active. Here we integrate genome-wide association study results with single-cell transcriptomic data from the entire mouse nervous system to systematically identify cell types underlying brain complex traits. We show that psychiatric disorders are predominantly associated with projecting excitatory and inhibitory neurons. Neurological diseases were associated with different cell types, which is consistent with other lines of evidence. Notably, Parkinson's disease was genetically associated not only with cholinergic and monoaminergic neurons (which include dopaminergic neurons) but also with enteric neurons and oligodendrocytes. Using post-mortem brain transcriptomic data, we confirmed alterations in these cells, even at the earliest stages of disease progression. Our study provides an important framework for understanding the cellular basis of complex brain maladies, and reveals an unexpected role of oligodendrocytes in Parkinson's disease.

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Genetic identification of cell types underlying brain complex traits yields insights into the etiology of Parkinson's disease

Abstract

Funding

Cohort Studies

UN SDGs

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