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Fos Protein Expression and Cocaine-Seeking Behavior in Rats after Exposure to a Cocaine Self-Administration Environment

机译:暴露于可卡因自我管理环境中的大鼠中Fos蛋白的表达和可卡因的寻找行为

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摘要

To examine neuronal activation associated with incentive motivation for cocaine, cocaine-seeking behavior (operant responding without cocaine reinforcement) and Fos expression were examined in rats exposed to saline and cocaine priming injections and/or a self-administration environment. Rats were first trained to self-administer cocaine or received yoked saline administration (“control”). They then received 21 daily exposures to either the self-administration environment (“extinction”) or a different environment (“no extinction”) without cocaine available. Extinction training, used to decrease incentive motivation for cocaine elicited by the self-administration environment, decreased cocaine-seeking behavior elicited by both the environment and the cocaine priming injection. Exposure to the self-administration environment enhanced Fos expression in the no extinction group relative to control and extinction groups in the anterior cingulate, basolateral amygdala, hippocampal CA1 region, dentate gyrus, nucleus accumbens shell and core, and central gray area, regardless of whether or not priming injections were given. The priming injections enhanced Fos expression in the ventral tegmental area, caudate putamen, substantia nigra pars reticulata, entorhinal cortex, central amygdala, lateral amygdala, arcuate nucleus, and central gray area, regardless of group. Thus, these changes likely reflect an unconditioned effect from either cocaine or injection stress. The priming injections also enhanced Fos expression in the anterior cingulate, but only in cocaine-experienced groups, suggesting that this enhancement reflects an experience-dependent motivational effect of the priming injections. The results suggest that different neural circuits may be involved in the incentive motivational effects of cocaine-paired environmental stimuli versus priming injections and that the anterior cingulate may be part of a common pathway for both.
机译:为了检查与可卡因刺激动机相关的神经元活化,在暴露于盐水和可卡因初次注射和/或自我给药环境的大鼠中检查了可卡因寻找行为(操作者响应而无需可卡因强化)和Fos表达。首先训练大鼠自我给药可卡因或接受轭铁盐溶液给药(“对照”)。然后,他们每天接受21次暴露于自我管理环境(“灭绝”)或其他环境(“不灭绝”)的可卡因暴露。灭绝训练用于减少自我管理环境引起的可卡因激励动机,减少了环境和可卡因引发注射引起的可卡因寻求行为。相对于对照组和前扣带回,基底外侧杏仁核,海马CA1区,齿状回,伏隔核和壳核以及中央灰色区域,无管理组的暴露,自我管理环境的暴露增强了Fos表达。或不进行灌注注射。初次注射增强了腹侧被盖区,尾状壳核,黑质网状体,内嗅皮层,中央杏仁核,外侧杏仁核,弓形核和中央灰色区域的Fos表达。因此,这些变化可能反映了可卡因或注射应力的无条件影响。初免注射剂还增强了前扣带回中的Fos表达,但仅在可卡因经验丰富的组中增强,表明这种增强反应了初次注射剂的经验依赖性激励作用。结果表明,可卡因对环境刺激与初次注射相比,不同的神经回路可能参与了激励动机,前扣带回可能是两者共同途径的一部分。

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