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对可卡因强化特性的敏化作用的发展与表达:NMDA受体的作用

Development and expression of sensitization to cocaine's reinforcing properties: role of NMDA receptors.

作者信息

Schenk S, Valadez A, McNamara C, House D T, Higley D, Bankson M G, Gibbs S, Horger B A

机构信息

Texas A&M University, Department of Psychology, College Station 77843.

出版信息

Psychopharmacology (Berl). 1993;111(3):332-8. doi: 10.1007/BF02244949.

Abstract

Acquisition of cocaine self-administration (0.125, 0.25 or 0.5 mg/kg/infusion) was assessed in rats that had received prior exposure to either saline or amphetamine (2.0 mg/kg). Acquisition of self-administration was dose-dependent, with the highest dose leading to the shortest latency to reliably discriminate between depression of a lever that resulted in drug delivery and an inactive lever. Latency to acquisition of the lever discrimination for rats that had received prior exposure to amphetamine was shorter than for the saline-pretreated counterparts in each cocaine dosage group. This suggests that repeated exposure to this drug prior to self-administration testing sensitized the rats to the reinforcing effects of cocaine. Co-administration of MK-801 (0.25 mg/kg, IP), a non-competitive NMDA antagonist, blocked the ability of chronic exposure to amphetamine to sensitize rats to cocaine. In experienced self-administering rats, acute pretreatment with MK-801 resulted in a loss of discriminative responding. The number of inactive lever responses was consistently higher than the number of active lever responses across all cocaine dosage groups. These data suggest that the NMDA receptor, possibly through interactions with dopamine systems, is critical for both the development and expression of sensitization to cocaine's reinforcing effects produced by intermittent preexposures to amphetamine.

摘要

在事先接触过生理盐水或苯丙胺(2.0毫克/千克)的大鼠中评估了可卡因自我给药(0.125、0.25或0.5毫克/千克/输注)的情况。自我给药的习得具有剂量依赖性,最高剂量导致在可靠区分导致药物递送的杠杆下压和无活性杠杆方面的潜伏期最短。在每个可卡因剂量组中,事先接触过苯丙胺的大鼠对杠杆辨别反应的习得潜伏期比接受生理盐水预处理的大鼠短。这表明在自我给药测试之前反复接触这种药物使大鼠对可卡因的强化作用敏感。共同给予非竞争性NMDA拮抗剂MK-801(0.25毫克/千克,腹腔注射)可阻断慢性接触苯丙胺使大鼠对可卡因敏感的能力。在有经验的自我给药大鼠中,MK-801急性预处理导致辨别反应丧失。在所有可卡因剂量组中,无活性杠杆反应的数量始终高于活性杠杆反应的数量。这些数据表明,NMDA受体可能通过与多巴胺系统相互作用,对于间歇性预先接触苯丙胺所产生的对可卡因强化作用的敏感化的发展和表达至关重要。

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