Use of a Novel Mouse Genotype to Model Acute Benzodiazepine Withdrawal

被引:0
作者
Pamela Metten
Kari J. Buck
Catherine M. Merrill
Amanda J. Roberts
Chia-Hua Yu
John C. Crabbe
机构
[1] Oregon Health & Science University,Department of Behavioral Neuroscience, Portland Alcohol Research Center
[2] R&D-12,Department of Veterans Affairs Medical Center
[3] R&D-40,Department of Veterans Affairs Medical Center
[4] The Scripps Research Institute,Molecular and Integrative Neurosciences Department
来源
Behavior Genetics | 2007年 / 37卷
关键词
Withdrawal; Substance abuse; Benzodiazepines; Diazepam; Alprazolam; Abecarnil; Clonazepam; Lorazepam; Midazolam; Triazolam; Zolpidem; Handling-induced convulsions; Mouse; Selected lines;
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摘要
Withdrawal from benzodiazepines in physically dependent rodents often requires that the drug be dislodged from its receptor with a competitive antagonist. Withdrawal Seizure-Prone (WSP) mice were selectively bred for their susceptibility to handling-induced withdrawal convulsions following chronic treatment with ethanol. Reflecting pleiotropic genetic influences, they also experience more severe withdrawal from other sedative-hypnotics including the benzodiazepine, diazepam. We used this susceptible genotype to test whether other benzodiazepine receptor (BZR) agonists also produce physical dependence following acute administration, comparing studies of spontaneous withdrawal with those where convulsions were precipitated by a BZR antagonist (flumazenil). Separate groups of mice were tested following a single injection of one of eight BZR agonists. Several doses of each drug were tested for spontaneous withdrawal, and a single dose of each drug was tested for precipitated withdrawal. Withdrawal convulsions were seen after all of the drugs by at least one method, suggesting that BZR agonists as a class elicit acute physical dependence in this susceptible genotype.
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页码:160 / 170
页数:10
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