Mice with genetically altered GABA transporter subtype I (GAT1) expression show altered behavioral responses to ethanol

You Qing Cai; Guo Qiang Cai; Guo Xiang Liu; Qing Cai; Jia Hao Shi; Jun Shi; Sun Kai Ma; Xia Sun; Zhe Jin Sheng; Zhen Tong Mei; Dafu Cui; Lihe Guo; Zhugang Wang; Jian Fei

doi:10.1002/jnr.20884

Mice with genetically altered GABA transporter subtype I (GAT1) expression show altered behavioral responses to ethanol

You Qing Cai, Guo Qiang Cai, Guo Xiang Liu, Qing Cai, Jia Hao Shi, Jun Shi, Sun Kai Ma, Xia Sun, Zhe Jin Sheng, Zhen Tong Mei, Dafu Cui, Lihe Guo, Zhugang Wang, Jian Fei

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

40 Scopus citations

Abstract

It is widely accepted that the GABAergic system plays an important role in the action of ethanol in vivo. GABA transporter subtype 1 (GAT1) constructs high affinity reuptake sites in the CNS and regulates GABAergic transmissions. In this study, mice lacking the GAT1 were developed by homologous recombination. Both hetero- and homozygous GAT1 mutant mice were tested for ethanol, saccharin or quinine consumption, ethanol-conditioned place preference, ethanol-conditioned taste aversion, ethanol-simulated motor activity, and ethanol-induced sedation/hypnosis. The GAT1^-/- mice showed decreased ethanol aversion and ethanol reward, and insensitivity to both the sedative/hypnotic and the motor stimulant effects of ethanol, along with increased avoidance of quinine preference and consumption. GAT1^+/- mice showed significantly increased consumption of ethanol and saccharin, however, enhanced the rewarding and preference effect of ethanol, increased avoidance of quinine, and higher sensitivity to the motor stimulant effect of ethanol. These results demonstrate that GAT1, perhaps in a bi-directional way, modulates some behavioral effects of ethanol. The GAT1 mutant mice provided us a very useful model to investigate the mechanisms of ethanol action in vivo.

Original language	English (US)
Pages (from-to)	255-267
Number of pages	13
Journal	Journal of neuroscience research
Volume	84
Issue number	2
DOIs	https://doi.org/10.1002/jnr.20884
State	Published - Aug 1 2006
Externally published	Yes

Keywords

Behavioral
Ethanol
GABA transporter
Knockout
Reward

ASJC Scopus subject areas

Cellular and Molecular Neuroscience

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10.1002/jnr.20884

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title = "Mice with genetically altered GABA transporter subtype I (GAT1) expression show altered behavioral responses to ethanol",

abstract = "It is widely accepted that the GABAergic system plays an important role in the action of ethanol in vivo. GABA transporter subtype 1 (GAT1) constructs high affinity reuptake sites in the CNS and regulates GABAergic transmissions. In this study, mice lacking the GAT1 were developed by homologous recombination. Both hetero- and homozygous GAT1 mutant mice were tested for ethanol, saccharin or quinine consumption, ethanol-conditioned place preference, ethanol-conditioned taste aversion, ethanol-simulated motor activity, and ethanol-induced sedation/hypnosis. The GAT1-/- mice showed decreased ethanol aversion and ethanol reward, and insensitivity to both the sedative/hypnotic and the motor stimulant effects of ethanol, along with increased avoidance of quinine preference and consumption. GAT1+/- mice showed significantly increased consumption of ethanol and saccharin, however, enhanced the rewarding and preference effect of ethanol, increased avoidance of quinine, and higher sensitivity to the motor stimulant effect of ethanol. These results demonstrate that GAT1, perhaps in a bi-directional way, modulates some behavioral effects of ethanol. The GAT1 mutant mice provided us a very useful model to investigate the mechanisms of ethanol action in vivo.",

keywords = "Behavioral, Ethanol, GABA transporter, Knockout, Reward",

author = "Cai, {You Qing} and Cai, {Guo Qiang} and Liu, {Guo Xiang} and Qing Cai and Shi, {Jia Hao} and Jun Shi and Ma, {Sun Kai} and Xia Sun and Sheng, {Zhe Jin} and Mei, {Zhen Tong} and Dafu Cui and Lihe Guo and Zhugang Wang and Jian Fei",

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AU - Cai, You Qing

AU - Cai, Guo Qiang

AU - Liu, Guo Xiang

AU - Cai, Qing

AU - Shi, Jia Hao

AU - Shi, Jun

AU - Ma, Sun Kai

AU - Sun, Xia

AU - Sheng, Zhe Jin

AU - Mei, Zhen Tong

AU - Cui, Dafu

AU - Guo, Lihe

AU - Wang, Zhugang

AU - Fei, Jian

PY - 2006/8/1

Y1 - 2006/8/1

N2 - It is widely accepted that the GABAergic system plays an important role in the action of ethanol in vivo. GABA transporter subtype 1 (GAT1) constructs high affinity reuptake sites in the CNS and regulates GABAergic transmissions. In this study, mice lacking the GAT1 were developed by homologous recombination. Both hetero- and homozygous GAT1 mutant mice were tested for ethanol, saccharin or quinine consumption, ethanol-conditioned place preference, ethanol-conditioned taste aversion, ethanol-simulated motor activity, and ethanol-induced sedation/hypnosis. The GAT1-/- mice showed decreased ethanol aversion and ethanol reward, and insensitivity to both the sedative/hypnotic and the motor stimulant effects of ethanol, along with increased avoidance of quinine preference and consumption. GAT1+/- mice showed significantly increased consumption of ethanol and saccharin, however, enhanced the rewarding and preference effect of ethanol, increased avoidance of quinine, and higher sensitivity to the motor stimulant effect of ethanol. These results demonstrate that GAT1, perhaps in a bi-directional way, modulates some behavioral effects of ethanol. The GAT1 mutant mice provided us a very useful model to investigate the mechanisms of ethanol action in vivo.

AB - It is widely accepted that the GABAergic system plays an important role in the action of ethanol in vivo. GABA transporter subtype 1 (GAT1) constructs high affinity reuptake sites in the CNS and regulates GABAergic transmissions. In this study, mice lacking the GAT1 were developed by homologous recombination. Both hetero- and homozygous GAT1 mutant mice were tested for ethanol, saccharin or quinine consumption, ethanol-conditioned place preference, ethanol-conditioned taste aversion, ethanol-simulated motor activity, and ethanol-induced sedation/hypnosis. The GAT1-/- mice showed decreased ethanol aversion and ethanol reward, and insensitivity to both the sedative/hypnotic and the motor stimulant effects of ethanol, along with increased avoidance of quinine preference and consumption. GAT1+/- mice showed significantly increased consumption of ethanol and saccharin, however, enhanced the rewarding and preference effect of ethanol, increased avoidance of quinine, and higher sensitivity to the motor stimulant effect of ethanol. These results demonstrate that GAT1, perhaps in a bi-directional way, modulates some behavioral effects of ethanol. The GAT1 mutant mice provided us a very useful model to investigate the mechanisms of ethanol action in vivo.

KW - Behavioral

KW - Ethanol

KW - GABA transporter

KW - Knockout

KW - Reward

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Mice with genetically altered GABA transporter subtype I (GAT1) expression show altered behavioral responses to ethanol

Abstract

Keywords

ASJC Scopus subject areas

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