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Long-Evans Rats Acquire Operant Self-Administration of 20% Ethanol Without Sucrose Fading

机译:长埃文斯大鼠获得20%乙醇的操作性自我给药,而蔗糖不褪色

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摘要

A major obstacle in the development of new medications for the treatment of alcohol use disorders (AUDs) has been the lack of preclinical, oral ethanol consumption paradigms that elicit high consumption. We have previously shown that rats exposed to 20% ethanol intermittently in a two-bottle choice paradigm will consume two times more ethanol than those given continuous access without the use of water deprivation or sucrose fading (5–6 g/kg every 24 h vs 2–3 g/kg every 24 h, respectively). In this study, we have adapted the model to an operant self-administration paradigm. Long-Evans rats were given access to 20% ethanol in overnight sessions on one of two schedules: (1) intermittent (Monday, Wednesday, and Friday) or (2) daily (Monday through Friday). With the progression of the overnight sessions, both groups showed a steady escalation in drinking (3–6 g/kg every 14 h) without the use of a sucrose-fading procedure. Following the acquisition phase, the 20% ethanol groups consumed significantly more ethanol than did animals trained to consume 10% ethanol with a sucrose fade (1.5 vs 0.7 g/kg every 30 min) and reached significantly higher blood ethanol concentrations. In addition, training history (20% ethanol vs 10% ethanol with sucrose fade) had a significant effect on the subsequent self-administration of higher concentrations of ethanol. Administration of the pharmacological stressor yohimbine following extinction caused a significant reinstatement of ethanol-seeking behavior. Both 20% ethanol models show promise and are amenable to the study of maintenance, motivation, and reinstatement. Furthermore, training animals to lever press for ethanol without the use of sucrose fading removes a potential confound from self-administration studies.
机译:开发用于治疗酒精使用障碍(AUDs)的新药物的主要障碍是缺乏临床前的口服乙醇消费范例,这些范例引起了高消费。我们以前的研究表明,在两瓶选择范例中间歇性地暴露于20%乙醇的大鼠,其乙醇消耗量比不使用缺水或蔗糖褪色的连续摄入的大鼠多两倍(每24h摄入5-6μg/ kg,而每24 h分别减少2–3 g / kg)。在这项研究中,我们将模型调整为可操作的自我管理范式。在以下两个时间表之一中,整夜为Long-Evans大鼠提供了20%的乙醇:(1)间歇性(星期一,星期三和星期五)或(2)每天(星期一至星期五)。随着隔夜会议的进行,两组的饮酒量均呈稳定上升趋势(每14h升3-6μg/ kg),而未使用蔗糖褪色程序。在采集阶段之后,20%的乙醇组消耗的乙醇比受过训练的消耗10%的乙醇且蔗糖褪色的动物要多得多(每30?min 1.5 vs 0.7?g / kg),并且血液中的乙醇浓度明显升高。此外,训练史(20%的乙醇与10%的乙醇伴随蔗糖褪色)对随后的更高浓度乙醇的自我给药具有重大影响。灭绝后给予药理应激源育亨宾可显着恢复寻求乙醇的行为。两种20%的乙醇模型都显示出希望,并且适用于维护,动力和恢复的研究。此外,训练动物在不使用蔗糖褪色的情况下杠杆按压乙醇,可以消除自我管理研究中的潜在混淆。

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