DRD2 co-expression network and a related polygenic index predict imaging, behavioral and clinical phenotypes linked to schizophrenia

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作者
G Pergola
P Di Carlo
E D'Ambrosio
B Gelao
L Fazio
M Papalino
A Monda
G Scozia
B Pietrangelo
M Attrotto
J A Apud
Q Chen
V S Mattay
A Rampino
G Caforio
D R Weinberger
G Blasi
A Bertolino
机构
[1] Neuroscience and Sense Organs,Department of Basic Medical Science
[2] University of Bari Aldo Moro,Departments of Neurology and Radiology
[3] Lieber Institute for Brain Development,Department of Neuroscience
[4] Johns Hopkins Medical Campus,Departments of Psychiatry
[5] National Institutes of Health,undefined
[6] National Institute of Mental Health,undefined
[7] Clinical and Translational Neuroscience Branch,undefined
[8] NIMH,undefined
[9] Johns Hopkins School of Medicine,undefined
[10] Institute of Psychiatry,undefined
[11] Sense Organs and Locomotive System,undefined
[12] Bari University Hospital,undefined
[13] Neurology,undefined
[14] Neuroscience and The Mckusick-Nathans Institute of Genomic Medicine,undefined
[15] Johns Hopkins School of Medicine,undefined
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摘要
Genetic risk for schizophrenia (SCZ) is determined by many genetic loci whose compound biological effects are difficult to determine. We hypothesized that co-expression pathways of SCZ risk genes are associated with system-level brain function and clinical phenotypes of SCZ. We examined genetic variants related to the dopamine D2 receptor gene DRD2 co-expression pathway and associated them with working memory (WM) behavior, the related brain activity and treatment response. Using two independent post-mortem prefrontal messenger RNA (mRNA) data sets (total N=249), we identified a DRD2 co-expression pathway enriched for SCZ risk genes. Next, we identified non-coding single-nucleotide polymorphisms (SNPs) associated with co-expression of this pathway. These SNPs were associated with regulatory genetic loci in the dorsolateral prefrontal cortex (P<0.05). We summarized their compound effect on co-expression into a Polygenic Co-expression Index (PCI), which predicted DRD2 pathway co-expression in both mRNA data sets (all P<0.05). We associated the PCI with brain activity during WM performance in two independent samples of healthy individuals (total N=368) and 29 patients with SCZ who performed the n-back task. Greater predicted DRD2 pathway prefrontal co-expression was associated with greater prefrontal activity and longer WM reaction times (all corrected P<0.05), thus indicating inefficient WM processing. Blind prediction of treatment response to antipsychotics in two independent samples of patients with SCZ suggested better clinical course of patientswith greater PCI (total N=87; P<0.05). The findings on this DRD2 co-expression pathway are a proof of concept that gene co-expression can parse SCZ risk genes into biological pathways associated with intermediate phenotypes as well as with clinically meaningful information.
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页码:e1006 / e1006
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