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Gene expression elucidates functional impact of polygenic risk for schizophrenia.

Authors :
Fromer M
Roussos P
Sieberts SK
Johnson JS
Kavanagh DH
Perumal TM
Ruderfer DM
Oh EC
Topol A
Shah HR
Klei LL
Kramer R
Pinto D
Gümüş ZH
Cicek AE
Dang KK
Browne A
Lu C
Xie L
Readhead B
Stahl EA
Xiao J
Parvizi M
Hamamsy T
Fullard JF
Wang YC
Mahajan MC
Derry JM
Dudley JT
Hemby SE
Logsdon BA
Talbot K
Raj T
Bennett DA
De Jager PL
Zhu J
Zhang B
Sullivan PF
Chess A
Purcell SM
Shinobu LA
Mangravite LM
Toyoshiba H
Gur RE
Hahn CG
Lewis DA
Haroutunian V
Peters MA
Lipska BK
Buxbaum JD
Schadt EE
Hirai K
Roeder K
Brennand KJ
Katsanis N
Domenici E
Devlin B
Sklar P
Source :
Nature neuroscience [Nat Neurosci] 2016 Nov; Vol. 19 (11), pp. 1442-1453. Date of Electronic Publication: 2016 Sep 26.
Publication Year :
2016

Abstract

Over 100 genetic loci harbor schizophrenia-associated variants, yet how these variants confer liability is uncertain. The CommonMind Consortium sequenced RNA from dorsolateral prefrontal cortex of people with schizophrenia (N = 258) and control subjects (N = 279), creating a resource of gene expression and its genetic regulation. Using this resource, ∼20% of schizophrenia loci have variants that could contribute to altered gene expression and liability. In five loci, only a single gene was involved: FURIN, TSNARE1, CNTN4, CLCN3 or SNAP91. Altering expression of FURIN, TSNARE1 or CNTN4 changed neurodevelopment in zebrafish; knockdown of FURIN in human neural progenitor cells yielded abnormal migration. Of 693 genes showing significant case-versus-control differential expression, their fold changes were ≤ 1.33, and an independent cohort yielded similar results. Gene co-expression implicates a network relevant for schizophrenia. Our findings show that schizophrenia is polygenic and highlight the utility of this resource for mechanistic interpretations of genetic liability for brain diseases.

Details

Language :
English
ISSN :
1546-1726
Volume :
19
Issue :
11
Database :
MEDLINE
Journal :
Nature neuroscience
Publication Type :
Academic Journal
Accession number :
27668389
Full Text :
https://doi.org/10.1038/nn.4399