不同心理状态维持药物诱导的可卡因条件位置偏好的再激活

T. Maurice, J. Espallergues, C. Zussy, J. Meunier, Clémence Borys, Elodie George, P. Romieu
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引用次数: 0

摘要

使用条件位置偏好(CPP)范式可以研究啮齿类动物的可卡因寻求行为。CPP可以熄灭,然后使用可卡因启动重新激活。为了研究多巴胺能受体在CPP恢复中的作用,用可卡因(30 mg/kg / ip)诱导瑞士小鼠CPP,并用生理盐水灭活CPP。D1受体拮抗剂SCH23,390 (0.03-1 mg/kg)、D2受体拮抗剂raclopride (0.1-3 mg/kg)或D3受体拮抗剂U-99,194A (20-40 mg/kg)单独或在可卡因(15 mg/kg)之前治疗,以检测CPP的再激活。可卡因启动重新激活CPP高达220%的后条件反应。0.3 mg/kg剂量下,SCH23,390和雷氯pride单独诱导可卡因诱导的CPP再激活,但只有SCH23,390阻断可卡因诱导的CPP再激活。U99,194A不能单独促进CPP的再激活或影响可卡因的反应。CPP再激活涉及情境学习,可以在消失后使用单次修复会话诱导。用可卡因或氯氯pride治疗,而不是用SCH23,390治疗,诱导CPP再激活。最后,在升高迷宫过程中,在药物治疗的再激活过程中测试小鼠的情绪状态,并在0.3 mg/kg SCH23,390后测量小鼠的焦虑状态。这些观察结果表明,在可卡因条件下的动物中,D1受体的阻断诱导了一种类似焦虑的状态,能够促进可卡因敏感的CPP的再激活。阻断D2受体可促进仿可卡因CPP的再激活。因此,两种不同的心理状态是药物启动CPP再激活的基础:由多巴胺系统介导的焦虑引起的“药物渴望CPP”和由激励学习过程促进的“药物检索CPP”。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Different Psychological States Sustain Drug-Induced Reactivation of Cocaine Conditioned Place Preference in the Mouse
Cocaine-seeking behavior can be investigated in rodents using the conditioned place preference (CPP) paradigm. CPP can be extinguished and then reactivated using cocaine priming. To study the role of dopaminergic receptors in CPP reinstatement, CPP was induced in Swiss mice using cocaine (30 mg/kg ip) and extinguished with saline. CPP reactivation was examined by treatment with the D1 receptor antagonist SCH23,390 (0.03-1 mg/kg), the D2 antagonist raclopride (0.1-3 mg/kg) or the D3 antagonist U-99,194A (20-40 mg/kg), alone or before cocaine (15 mg/kg). Cocaine priming reactivated CPP up to 220% of the post-conditioning response. SCH23,390 and raclopride induced, alone at 0.3 mg/kg, reactivation of cocaine-induced CPP, but only SCH23,390 blocked the cocaine-induced reactivation. U99,194A failed to promote CPP reactivation alone or to affect the cocaine response. CPP reactivation involving contextual learning could be induced using a single-reconditioning session after extinction. Treatment with cocaine or raclopride, but not SCH23,390, induced CPP reactivation. Finally, the emotional state of mice was tested during reactivation under drug treatments in the elevated maze procedure and an anxiety state was measured after 0.3 mg/kg SCH23,390. These observations showed that in cocaine-conditioned animals and then extinguished, blockade of D1 receptors induces an anxiogeniclike state, able to promote a cocaine-sensitive CPP reactivation. Blockade of D2 receptor promoted a cocaine-mimetic CPP reactivation. Therefore, two different psychological states underlie CPP reactivation by drug priming: a 'drug craving CPP' induced by dopamine systems-mediated anxiety and a 'drug retrieval CPP' promoted by incentive learning processes.
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