首页> 外文OA文献 >Prazosin + Naltrexone Decreases Alcohol Drinking More Effectively Than Does Either Drug Alone in P Rats with a Protracted History of Extensive Voluntary Alcohol Drinking, Dependence, and Multiple Withdrawals
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Prazosin + Naltrexone Decreases Alcohol Drinking More Effectively Than Does Either Drug Alone in P Rats with a Protracted History of Extensive Voluntary Alcohol Drinking, Dependence, and Multiple Withdrawals

机译:比起单独使用一种药物,Prazosin +纳曲酮可以更有效地减少长期酗酒,依赖和多次戒断的长期饮酒的P大鼠的饮酒

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摘要

BackgroundPrazosin (PRZ, an α1-adrenergic receptor antagonist) and naltrexone (NTX, a non-specific opioid receptor antagonist) each decrease alcohol drinking when administered to rats selectively-bred for high voluntary alcohol drinking (alcohol-preferring, or “P”), and the combination of PRZ+NTX decreases alcohol drinking more effectively than does either drug alone. Since drug responsiveness can depend on history of alcohol drinking and dependence, we investigated whether various schedules of PRZ and NTX administration, alone or in combination, are effective in decreasing alcohol drinking in male P rats with a history of protracted voluntary alcohol drinking, dependence and repeated withdrawals closely resembling human alcoholism.MethodsMale P rats became alcohol-dependent during 1 year of ad libitum 24 h/day access to food, water and 20% alcohol with repetitive temporary alcohol withdrawals. Four sequential studies then addressed effects of oral PRZ (2 mg/kg) and NTX (10 mg/kg), alone or together, on alcohol drinking during: 1) daily alcohol access with daily drug treatment, 2) intermittent alcohol access with daily drug treatment, 3) intermittent alcohol access with occasional drug treatment, and 4) post-deprivation reinstatement of alcohol access.ResultsThe combination of PRZ+NTX consistently suppressed alcohol drinking during daily or intermittent alcohol access conditions and when drug treatment was either daily or occasional. PRZ+NTX was consistently more effective than either drug alone. The reduction in alcohol drinking was not due to sedation, motor effects or malaise.ConclusionsBoth daily and “as-needed” treatment with PRZ+NTX are highly effective in suppressing daily, intermittent and post-deprivation alcohol drinking in male P rats with a protracted history of alcohol dependence and repeated withdrawals. This drug combination may be especially effective for treating individuals with long histories of heavy alcohol abuse, dependence and repeated relapse, as commonly encountered in clinical practice.
机译:背景当对选择性饲养的大鼠进行高自愿性饮酒后,Prazosin(PRZ,一种α1-肾上腺素能受体拮抗剂)和纳曲酮(NTX,一种非特异性阿片受体拮抗剂)各自都会减少饮酒(首选饮酒,或称“ P”) ,并且PRZ + NTX的组合比单独使用任何一种药物都能更有效地减少饮酒。由于药物反应性可能取决于饮酒和依赖的病史,因此我们调查了不同的PRZ和NTX给药方案(单独或联合使用)是否有效减少了长期饮酒,依赖和长期饮酒的雄性P大鼠的饮酒。方法:雄性P大鼠在任意一年(每天24小时/天)获取食物,水和20%的酒精后,会暂时依赖酒精,并反复暂时戒酒。然后进行了四项顺序研究,研究了口服PRZ(2 mg / kg)和NTX(10 mg / kg)单独或一起对以下期间饮酒的影响:1)每日饮酒与每日药物治疗,2)间歇饮酒与每日药物治疗,3)间歇性饮酒和偶尔的药物治疗以及4)剥夺后恢复饮酒的结果。PRZ+ NTX的组合在每天或间歇性饮酒条件下以及每天或偶尔进行药物治疗时均能持续抑制饮酒。 PRZ + NTX始终比单独使用任何一种药物更有效。减少饮酒不是由于镇静,运动作用或不适引起的。结论每天和“按需”用PRZ + NTX进行治疗均能有效抑制长期,长期服用的雄性P大鼠的每日,间歇性和剥夺性饮酒。有酒精依赖和反复戒断的病史。如在临床实践中经常遇到的那样,这种药物组合对于治疗长期酗酒,依赖和反复复发的患者特别有效。

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