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Reduced aggression in mice lacking GABA transporter subtype 1

✍ Scribed by Guo-Xiang Liu; Shuai Liu; Guo-Qiang Cai; Zhe-Jing Sheng; You-Qing Cai; Jie Jiang; Xia Sun; Sun-Kai Ma; Long Wang; Zhu-Gang Wang; Jian Fei


Book ID
102381665
Publisher
John Wiley and Sons
Year
2007
Tongue
English
Weight
310 KB
Volume
85
Category
Article
ISSN
0360-4012

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✦ Synopsis


Abstract

Dysregulation of the brain GABAergic system has been implicated in the pathophysiology of violence and aggression. As a key regulator of central GABAergic activity, dysfunction of the GABA transporter subtype 1 (GAT1) represents a potential mechanism mediating pathologic aggression. We provide evidence that GAT1βˆ’/βˆ’ mice and GAT1+/βˆ’ mice exhibit lower aggressive behavior both in home cage resident–intruder test and neutral arena resident–intruder test, compared to wild‐type mice (GAT1+/+). The pharmacologic effects of the GAT1 inhibitor, tiagabine and the GABA~A~ receptor antagonist, bicuculline have been assessed in GAT1+/+ mice: tiagabine inhibits attacks but bicuculline induces attacks. Compared to GAT1+/βˆ’ and +/+ mice, the GAT1βˆ’/βˆ’ mice displayed a normal circadian pattern of home cage activity, but more activity overall. Meanwhile, reduced testosterone concentration was found in GAT1βˆ’/βˆ’ mice compared to GAT1+/+ mice but not in GAT1+/+ mice treated with tiagabine, suggesting that testosterone is not directly involved in GAT1 mediated aggressive behavior regulation. These results showed that GAT1 is an important target involved in the regulation of aggressive behavior in mice, and long‐term dysfunction of GAT1 may also result in the alteration of testosterone secretion. Β© 2006 Wiley‐Liss, Inc.


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