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地西泮对自我刺激有影响,但对逃避刺激没有影响,这表明其具有享乐调节作用。

Diazepam's impact on self-stimulation but not stimulation-escape suggests hedonic modulation.

作者信息

Carden S E, Coons E E

机构信息

New York University.

出版信息

Behav Neurosci. 1990 Feb;104(1):56-61. doi: 10.1037//0735-7044.104.1.56.

Abstract

In rats that self-administered lateral hypothalamic (LH) stimulation through chronically implanted electrodes, ip diazepam (DZ) increased rates and decreased thresholds of self-stimulation (SS) in a dose-related manner. Stimulation-escape (SE), however, was refractory to the drug. There was a complete dichotomy in electrode placements along the anterior/posterior plane. Every pure-reward electrode location was posterior to every reward-escape electrode. DZ-sensitive SS appears to be mediated by a reward substrate common to both pure-reward and reward-escape rats, whereas SE is supported by an aversive system unaffected by DZ and stimulated only in those rats with anterior placements. The lack of control over SE suggests that the drug's effect on stimulation-induced conduct is to increase reward rather than to decrease aversion. This hypothesis is discussed in the context of DZ's interactions with drugs of abuse.

摘要

在通过长期植入电极自我给予下丘脑外侧(LH)刺激的大鼠中,腹腔注射地西泮(DZ)以剂量相关的方式增加了自我刺激(SS)的速率并降低了其阈值。然而,刺激逃避(SE)对该药物具有抗性。沿着前后平面的电极放置存在完全的二分法。每个纯奖励电极位置都在每个奖励逃避电极的后方。对DZ敏感的SS似乎由纯奖励和奖励逃避大鼠共有的奖励底物介导,而SE由不受DZ影响且仅在那些电极置于前方的大鼠中被刺激的厌恶系统支持。对SE缺乏控制表明该药物对刺激诱导行为的作用是增加奖励而非减少厌恶。在DZ与滥用药物的相互作用背景下讨论了这一假设。

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