Genetic variation in the G72 (DAOA) gene affects temporal lobe and amygdala structure in subjects affected by bipolar disorder

Riccardo Zuliani; Bill Moorhead; Dominic Job; James McKirdy; Jessika E. D. Sussmann; Eve C. Johnstone; Stephen M. Lawrie; Paolo Brambilla; Jeremy Hall; Andrew M. McIntosh

doi:10.1111/j.1399-5618.2009.00731.x

Genetic variation in the G72 (DAOA) gene affects temporal lobe and amygdala structure in subjects affected by bipolar disorder

Riccardo Zuliani, Bill Moorhead, Dominic Job, James McKirdy, Jessika E. D. Sussmann, Eve C. Johnstone, Stephen M. Lawrie, Paolo Brambilla, Jeremy Hall, Andrew M. McIntosh

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

Abstract

Background
Variation in the G72 (DAOA) gene is understood to convey susceptibility for bipolar disorder through an uncertain mechanism. Little is known about the structural brain phenotypes associated with this gene. We hypothesised that reductions in temporal lobe and amygdala gray matter would be associated with variation at two loci in the gene for which evidence of genetic linkage has been repeatedly demonstrated.

Methods
We examined the temporal lobe and amygdala gray matter associations of the risk variants M23 and M24 at the 5' end of the gene encoding G72 in 81 controls and 38 people with bipolar disorder.

Results
Genetic variation at both the M23 and M24 loci in G72 were associated with decreased gray matter density within the left temporal pole in people with bipolar disorder. M23 was also associated with reductions in right amygdala gray matter density. The genetic imaging associations were found only in patients with bipolar disorder.

Conclusions
Genetic variation at single nucleotide polymorphisms in the G72 gene previously associated with bipolar disorder is related to reductions in temporal pole and amygdala gray matter structure in people with bipolar disorder.

Original language	English
Pages (from-to)	621-627
Number of pages	7
Journal	Bipolar Disorders
Volume	11
Issue number	6
DOIs	https://doi.org/10.1111/j.1399-5618.2009.00731.x
Publication status	Published - Sept 2009

Keywords / Materials (for Non-textual outputs)

bipolar disorder
DAOA
G72
voxel based morphometry
MRI

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10.1111/j.1399-5618.2009.00731.x

http://onlinelibrary.wiley.com/doi/10.1111/j.1399-5618.2009.00731.x/abstract

Cite this

@article{c88be512cb6c43599763bd91cfd57e33,

title = "Genetic variation in the G72 (DAOA) gene affects temporal lobe and amygdala structure in subjects affected by bipolar disorder",

abstract = "Background Variation in the G72 (DAOA) gene is understood to convey susceptibility for bipolar disorder through an uncertain mechanism. Little is known about the structural brain phenotypes associated with this gene. We hypothesised that reductions in temporal lobe and amygdala gray matter would be associated with variation at two loci in the gene for which evidence of genetic linkage has been repeatedly demonstrated. Methods We examined the temporal lobe and amygdala gray matter associations of the risk variants M23 and M24 at the 5' end of the gene encoding G72 in 81 controls and 38 people with bipolar disorder. Results Genetic variation at both the M23 and M24 loci in G72 were associated with decreased gray matter density within the left temporal pole in people with bipolar disorder. M23 was also associated with reductions in right amygdala gray matter density. The genetic imaging associations were found only in patients with bipolar disorder. Conclusions Genetic variation at single nucleotide polymorphisms in the G72 gene previously associated with bipolar disorder is related to reductions in temporal pole and amygdala gray matter structure in people with bipolar disorder.",

keywords = "bipolar disorder, DAOA, G72, voxel based morphometry, MRI",

author = "Riccardo Zuliani and Bill Moorhead and Dominic Job and James McKirdy and Sussmann, \{Jessika E. D.\} and Johnstone, \{Eve C.\} and Lawrie, \{Stephen M.\} and Paolo Brambilla and Jeremy Hall and McIntosh, \{Andrew M.\}",

year = "2009",

month = sep,

doi = "10.1111/j.1399-5618.2009.00731.x",

language = "English",

volume = "11",

pages = "621--627",

journal = "Bipolar Disorders",

issn = "1398-5647",

publisher = "Blackwell Munksgaard",

number = "6",

}

TY - JOUR

T1 - Genetic variation in the G72 (DAOA) gene affects temporal lobe and amygdala structure in subjects affected by bipolar disorder

AU - Zuliani, Riccardo

AU - Moorhead, Bill

AU - Job, Dominic

AU - McKirdy, James

AU - Sussmann, Jessika E. D.

AU - Johnstone, Eve C.

AU - Lawrie, Stephen M.

AU - Brambilla, Paolo

AU - Hall, Jeremy

AU - McIntosh, Andrew M.

PY - 2009/9

Y1 - 2009/9

N2 - Background Variation in the G72 (DAOA) gene is understood to convey susceptibility for bipolar disorder through an uncertain mechanism. Little is known about the structural brain phenotypes associated with this gene. We hypothesised that reductions in temporal lobe and amygdala gray matter would be associated with variation at two loci in the gene for which evidence of genetic linkage has been repeatedly demonstrated. Methods We examined the temporal lobe and amygdala gray matter associations of the risk variants M23 and M24 at the 5' end of the gene encoding G72 in 81 controls and 38 people with bipolar disorder. Results Genetic variation at both the M23 and M24 loci in G72 were associated with decreased gray matter density within the left temporal pole in people with bipolar disorder. M23 was also associated with reductions in right amygdala gray matter density. The genetic imaging associations were found only in patients with bipolar disorder. Conclusions Genetic variation at single nucleotide polymorphisms in the G72 gene previously associated with bipolar disorder is related to reductions in temporal pole and amygdala gray matter structure in people with bipolar disorder.

AB - Background Variation in the G72 (DAOA) gene is understood to convey susceptibility for bipolar disorder through an uncertain mechanism. Little is known about the structural brain phenotypes associated with this gene. We hypothesised that reductions in temporal lobe and amygdala gray matter would be associated with variation at two loci in the gene for which evidence of genetic linkage has been repeatedly demonstrated. Methods We examined the temporal lobe and amygdala gray matter associations of the risk variants M23 and M24 at the 5' end of the gene encoding G72 in 81 controls and 38 people with bipolar disorder. Results Genetic variation at both the M23 and M24 loci in G72 were associated with decreased gray matter density within the left temporal pole in people with bipolar disorder. M23 was also associated with reductions in right amygdala gray matter density. The genetic imaging associations were found only in patients with bipolar disorder. Conclusions Genetic variation at single nucleotide polymorphisms in the G72 gene previously associated with bipolar disorder is related to reductions in temporal pole and amygdala gray matter structure in people with bipolar disorder.

KW - bipolar disorder

KW - DAOA

KW - G72

KW - voxel based morphometry

KW - MRI

U2 - 10.1111/j.1399-5618.2009.00731.x

DO - 10.1111/j.1399-5618.2009.00731.x

M3 - Article

C2 - 19689504

SN - 1398-5647

VL - 11

SP - 621

EP - 627

JO - Bipolar Disorders

JF - Bipolar Disorders

IS - 6

ER -

Genetic variation in the G72 (DAOA) gene affects temporal lobe and amygdala structure in subjects affected by bipolar disorder

Abstract

Keywords / Materials (for Non-textual outputs)

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