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暴露于与可卡因相关的情境刺激后,条件性增加的类焦虑行为由促肾上腺皮质激素释放因子介导。

Conditioned increases in anxiogenic-like behavior following exposure to contextual stimuli associated with cocaine are mediated by corticotropin-releasing factor.

作者信息

DeVries A C, Pert A

机构信息

Biological Psychiatry Branch, National Institute of Mental Health, Bethesda, MD 20892, USA.

出版信息

Psychopharmacology (Berl). 1998 Jun;137(4):333-40. doi: 10.1007/s002130050627.

Abstract

Although cocaine is a powerful reinforcer, it has been reported to produce anxiety in humans and anxiogenic-like behavior in animals. The goal of this study was three-fold: (1) to determine the doses of cocaine that induce anxiogenic-like behavior in the elevated plus-maze in rats, (2) to determine if cocaine-associated contextual cues are capable of eliciting anxiogenic-like behavior in the absence of the drug, and (3) to identify possible mechanisms through which cocaine-associated cues affect behavior in the elevated plus-maze. Measurement of the amount of time that the animals spend exploring the open arms of the maze provides a sensitive index of anxiogenic-like behavior in rats. In experiment 1, rats were injected with 10 mg/kg, 20 mg/kg, or 30 mg/kg cocaine HCl or saline for 6 days. On day 6, the rats were tested in the elevated plus-maze 25 min after injection with cocaine or saline. The animals chronically treated with the three doses of cocaine exhibited a dose-dependent increase in anxiogenic-like behavior in the elevated plus-maze, compared to the saline-treated group. In experiment 2, cocaine-induced (30 mg/kg) conditioning was achieved using a simple contextual design. On the final day of the experiment (day 6), after 5 days of conditioning, the rats were exposed for 25 min to the cocaine-associated contextual cues, then placed in the elevated plus-maze. Animals that had been exposed to cocaine-associated contextual cues prior to being placed in the elevated plus-maze exhibited a significant increase in anxiogenic-like behavior compared to the control groups. However, pretreatment of the rats with the CRF antagonist, alpha-helical CRF9-41 (1 microg, i.c.v.), on the test day, prior to exposure to cocaine-associated contextual cues, attenuated the subsequent anxiogenic-like behavioral response in the elevated plus-maze (experiment 3). The results suggest that contextual cues associated with repeated treatment with 30 mg/kg cocaine are capable of eliciting anxiogenic-like behavior in the absence of the drug and that CRF mediates the expression of anxiogenic-like behaviors in the elevated plus-maze following exposure to cocaine-associated cues. The conditioned anxiogenic action elicited by cocaine-associated cues may have relevance for understanding the complex addictive nature of this drug and some of the clinical phenomena related to its use.

摘要

尽管可卡因是一种强效强化剂,但据报道它会在人类中引发焦虑,并在动物中引发类焦虑行为。本研究的目的有三个:(1)确定能在高架十字迷宫中诱发大鼠类焦虑行为的可卡因剂量;(2)确定与可卡因相关的情境线索在无药物情况下是否能够引发类焦虑行为;(3)确定可卡因相关线索影响高架十字迷宫中行为的可能机制。测量动物在迷宫开放臂中探索的时间,可提供大鼠类焦虑行为的敏感指标。在实验1中,大鼠连续6天注射10mg/kg、20mg/kg或30mg/kg的盐酸可卡因或生理盐水。在第6天,大鼠在注射可卡因或生理盐水后25分钟,在高架十字迷宫中进行测试。与生理盐水处理组相比,用三种剂量可卡因长期处理的动物在高架十字迷宫中表现出剂量依赖性的类焦虑行为增加。在实验2中,使用简单的情境设计实现了可卡因诱导(30mg/kg)的条件反射。在实验的最后一天(第6天),经过5天的条件反射后,将大鼠暴露于与可卡因相关的情境线索25分钟,然后放入高架十字迷宫。与对照组相比,在放入高架十字迷宫之前暴露于与可卡因相关的情境线索的动物,类焦虑行为显著增加。然而,在测试当天,在暴露于与可卡因相关的情境线索之前,用促肾上腺皮质激素释放因子(CRF)拮抗剂α-螺旋CRF9-41(1μg,脑室内注射)预处理大鼠,可减弱随后在高架十字迷宫中的类焦虑行为反应(实验3)。结果表明,与30mg/kg可卡因重复处理相关的情境线索在无药物情况下能够引发类焦虑行为,并且CRF介导了暴露于与可卡因相关的线索后在高架十字迷宫中的类焦虑行为表达。可卡因相关线索引发的条件性焦虑作用可能与理解该药物复杂的成瘾性质以及与其使用相关的一些临床现象有关。

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