The place conditioning paradigm has proven successful in identifying the neural mechanisms of drug reinforcement. Two classes of drugs, opiates and psychomotor stimulants, have received the most study, and in each case an important role for DA neurons of the mesolimbic system has been established. Moreover, both receptor subtypes, D1 and D2, appear to be involved. Despite this progress, the substrates of drug reward are not completely understood. First, a role for DA has not been established for all stimulants: DA receptor blockade failed to affect conditioned place preferences produced by the stimulants methylphenidate, nomifensine, or bupropion. Second, preliminary evidence suggests that intact serotonergic transmission is important in morphine place conditioning, but a similar consistent finding has not been observed with amphetamine place conditioning. Further study may reveal an interesting dissociation of serotonin's role in the rewarding effects of psychomotor stimulants and opiates. Finally, the role of the opiate receptor subtype kappa is not known; also, the significance of the several anatomical sites that support opiate place conditioning remains unclear.

译文

:场所调节范例已被证明可以成功地识别药物增强的神经机制。研究最多的两类药物是阿片类药物和精神运动兴奋剂,在每种情况下,均已确立了中脑边缘系统DA神经元的重要作用。而且,两个受体亚型D1和D2似乎都参与了。尽管取得了这一进展,但尚未完全了解药物奖励的底物。首先,并不是所有兴奋剂都具有DA的作用:DA受体阻滞不能影响兴奋剂哌醋甲酯,诺米芬或安非他酮产生的条件性位置偏爱。第二,初步证据表明完整的血清素能传递在吗啡位置调节中很重要,但是在苯丙胺位置调节中未观察到类似的一致发现。进一步的研究可能揭示5-羟色胺在精神运动兴奋剂和鸦片制剂的奖励作用中的作用有一个有趣的分解。最后,阿片受体亚型κ的作用尚不清楚。同样,支持鸦片位置调节的几个解剖部位的意义仍然不清楚。

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