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内源性神经甾体别孕烯醇酮会改变乙醇的强化作用。

The reinforcing effects of ethanol are altered by the endogenous neurosteroid, allopregnanolone.

作者信息

Janak P H, Redfern J E, Samson H H

机构信息

Department of Physiology and Pharmacology, Wake Forest University School of Medicine, Winston-Salem, North Carolina, USA.

出版信息

Alcohol Clin Exp Res. 1998 Aug;22(5):1106-12.

PMID:9726282
Abstract

We examined the effect of systemic administration of the endogenously occurring progesterone metabolite, allopregnanolone, on oral self-administration of ethanol by male rats. Rats were trained to perform an operant response for presentation of 0.1 ml of a solution of 10% ethanol in water using the sucrose fading technique. After acquisition of stable lever-press responding on a fixed-ratio 4 schedule, subjects received subcutaneous injections of 1, 3, or 10 mg/kg of allopregnanolone, or vehicle, 20 min prior to the self-administration session. Pretreatment with 3 mg/kg, but not 1 or 10 mg/kg, increased the mean total number of lever press responses made to obtain ethanol, and therefore increased the mean total number of ethanol presentations. The number of responses and response rate were examined as a function of the number of "runs" within the 30-min session; a "run" was defined as a series of consecutive responses with an interresponse interval of <1 min. The increase in total responses after 3 mg/kg was due in part to an increased number of responses for the first run of the session, with no effect on response rates. However, the higher dose of 10 mg/kg decreased response rates within the first run. Thus, allopregnanolone alters ethanol-reinforced responding at concentrations lower than those that depress rates of responding. The effects of administration of the benzodiazepene, diazepam, were determined for comparison with those of the neurosteroid. The subcutaneous injection of 0.3, 1.0, or 3.0 mg/kg of diazepam did not produce any clear dose-dependent changes in measures of ethanol-reinforced operant responding, supporting the suggestion of differences in the contribution of the benzodiazepene and neurosteroid binding sites to GABA(A) receptor function. The results indicate that exogenous administration of allopregnanolone dose-dependently alters ethanol-reinforced operant responding, and suggest that this endogenously occurring neurosteroid could mediate some of the reinforcing effects of ethanol.

摘要

我们研究了内源性孕酮代谢物别孕烯醇酮全身给药对雄性大鼠口服乙醇自我给药行为的影响。采用蔗糖消退技术训练大鼠对呈现0.1 ml含10%乙醇的水溶液进行操作性反应。在固定比率4的条件下获得稳定的杠杆按压反应后,在自我给药实验前20分钟,给实验对象皮下注射1、3或10 mg/kg的别孕烯醇酮或赋形剂。3 mg/kg预处理可增加为获取乙醇而进行的杠杆按压反应的平均总数,从而增加乙醇呈现的平均总数,但1或10 mg/kg预处理则无此效果。将反应次数和反应速率作为30分钟实验时段内“连续反应串”数量的函数进行检测;“连续反应串”定义为一系列连续反应,反应间隔时间<1分钟。3 mg/kg给药后总反应增加部分归因于实验时段首个连续反应串的反应次数增加,而对反应速率无影响。然而,10 mg/kg的较高剂量降低了首个连续反应串内的反应速率。因此,别孕烯醇酮在低于抑制反应速率的浓度下改变乙醇强化反应。为与神经甾体的作用进行比较,测定了苯二氮䓬类药物地西泮给药的效果。皮下注射0.3、1.0或3.0 mg/kg的地西泮未在乙醇强化操作性反应指标上产生任何明显的剂量依赖性变化,这支持了苯二氮䓬类药物和神经甾体结合位点对GABA(A)受体功能贡献存在差异的观点。结果表明,外源性给予别孕烯醇酮剂量依赖性地改变乙醇强化操作性反应,并提示这种内源性神经甾体可能介导乙醇的一些强化作用。

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