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Role of the orbitofrontal cortex and the dorsal striatum in incentive motivation for cocaine

麝香醇 巴氯芬 纹状体 心理学 自我管理 眶额皮质 兴奋剂 生理盐水 麻醉 神经科学 药理学 内科学 医学 多巴胺 前额叶皮质 受体 认知
作者
Ellie-Anna Minogianis,Alice Servonnet,M. Filion,Anne‐Noël Samaha
出处
期刊:Behavioural Brain Research [Elsevier BV]
卷期号:372: 112026-112026 被引量:13
标识
DOI:10.1016/j.bbr.2019.112026
摘要

Drug addiction involves increased incentive motivation for drug. Intermittent access to cocaine (IntA; 5–6 minutes ON, 25–26 minutes OFF, for 5–6 hours/session) enhances motivation to take the drug. The orbitofrontal cortex (OFC) and the dorsal striatum (DS) are part of a corticolimbic circuit that encodes incentive value and regulates reward-directed behaviour. We predicted that inactivation of the OFC, DS or both suppresses incentive motivation for cocaine after IntA experience. Male Wistar rats had IntA to cocaine (0.25 mg/kg/infusion) for 10 sessions. The rats developed a ‘loading’ pattern of intake, taking most of their cocaine in the first minute of each drug-available period. They also developed psychomotor sensitization to self-administered cocaine. We then measured incentive motivation for cocaine using a progressive ratio schedule of reinforcement (PR). Before some PR sessions, rats received microinfusions of a baclofen/muscimol cocktail (0.3 and 0.03 nmol/hemisphere, respectively, or saline) to temporarily inactivate the OFC or DS, or to disconnect the two regions. None of these treatments changed spontaneous locomotion in cocaine-naïve rats. However, both baclofen/muscimol and saline infusions influenced cocaine self-administration behaviour. Infusing baclofen/muscimol or saline into the OFC or into the OFC and contralateral DS decreased responding for cocaine under PR, with baclofen/muscimol and saline having similar effects, except that only OFC-DS disconnection with baclofen/muscimol slowed the pace of cocaine intake. Baclofen/muscimol or saline into the DS also reduced responding for cocaine under PR, but baclofen/muscimol was more effective. We conclude that neuronal activity in the OFC and DS might regulate incentive motivation for cocaine.

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