Glucocorticoid regulation of dopamine clearance, cocaine seeking, and reward

糖皮质激素对多巴胺清除、可卡因寻求和奖励的调节

• 批准号: 8920526
• 负责人: DAVID A BAKER
• 金额: $ 37.06万
• 依托单位: MARQUETTE UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2014
• 资助国家: 美国
• 起止时间: 2014-09-15 至 2019-05-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8920526
• 关键词: Abstinence; Acute; Animals; Behavior; Behavioral; Behavioral Genetics; Brain; Brain region; Cells; Chemosensitization; Cocaine; Cocaine Dependence; Cognition; Corticosterone; Disease; Dopamine; Dose; Event; Extracellular Space; Functional disorder; Genetically Modified Animals; Glucocorticoids; Health; Hormones; Individual; Intake; Knockout Mice; Lead; Life; Measures; Mediating; Microdialysis; Motivation; Nucleus Accumbens; Organic Cation Transporter; Peripheral; Pharmaceutical Preparations; Positioning Attribute; Process; RNA Interference; Rattus; Regulation; Relapse; Rewards; Risk; Rodent; Role; Scanning; Series; Signal Transduction; Staging; Stimulus; Stress; System; Techniques; Testing; Tissues; addiction; behavioral response; cocaine use; dopamine transporter; drug abstinence; drug relapse; drug seeking behavior; extracellular; genetic approach; in vivo; inhibitor/antagonist; monoamine; motivated behavior; neurobiological mechanism; neurochemistry; neuropsychiatry; neuroregulation; neurotransmission; non-drug; novel; presynaptic; receptor; response; reward processing; taste stimuli

DESCRIPTION (provided by applicant): An insidious aspect of addiction is that afflicted individuals are at risk of relapse even after extended periods of abstinence. Stressful life events are important contributors to relapse in recovering cocaine addicts, but the mechanisms by which they influence motivational systems are poorly understood. Studies suggest that stress may "set the stage" for relapse by increasing the sensitivity of brain reward circuits to drug-associated stimuli. This proposal seeks to elucidate the mechanisms by which stress, through increases in glucocorticoid hormones, influences relapse vulnerability. We have previously shown that treatment of rodents with stress levels of glucocorticoids does not lead to reinstatement of drug-seeking behavior, but potentiates reinstatement in response to a dose of cocaine that, by itself, is not sufficient to trigger relapse. In parallel to its behavioral effect, corticosterone pretreatment also potentiates the effects of low-dose cocaine on extracellular dopamine concentration in the nucleus accumbens, suggesting that glucocorticoids may potentiate drug seeking by enhancing dopaminergic neurotransmission in this critical reward-processing brain region. We are examining the role of organic cation transporter 3, a high-capacity dopamine transporter that is acutely and directly inhibited by glucocorticoids, in mediating the effects of glucocorticoids on dopaminergic neurotransmission, cocaine relapse, and motivated behavior in rodents. Because of a lack of pharmacologically specific inhibitors for OCT3, we are using two different genetic approaches to test the hypothesis that corticosterone potentiates cocaine-induced dopaminergic neurotransmission and drug-seeking behavior by inhibiting OCT3-mediated clearance of dopamine in the nucleus accumbens. In the first aim, we will determine the impact of corticosterone-induced inhibition of dopamine clearance in the nucleus accumbens on dopamine signaling and drug relapse by using in vivo microdialysis and fast-scan cyclic voltammetry to measure dopamine concentration and clearance in cocaine-seeking animals. In the second aim, we will determine the role of OCT3 in the behavioral and neurochemical effects of corticosterone by examining corticosterone effects on drug-seeking behavior and nucleus accumbens dopamine signaling in animals genetically modified to lack OCT3 expression either globally or specifically in the nucleus accumbens. In the third aim, we will test the hypothesis that corticosterone-induced decreases in dopamine clearance modulate reward sensitivity and natural reward processing. These findings will thoroughly characterize a novel mechanism by which stress hormones can rapidly regulate dopamine signaling and contribute to the impact of stress on drug intake and motivated behavior in general.

描述（由申请人提供）：成瘾的一个阴险的方面是，即使在长期禁欲后，受影响的个体仍有复发的风险。应激性生活事件 是可卡因成瘾者复吸的重要因素，但对它们影响动机系统的机制知之甚少。研究表明，压力可能会增加大脑奖赏回路对药物相关刺激的敏感性，从而为复发“设置舞台”。该建议旨在阐明应激通过增加糖皮质激素影响复发脆弱性的机制。我们以前已经表明，用糖皮质激素的应激水平治疗啮齿动物不会导致寻求药物行为的恢复，但会增强对可卡因剂量的反应，而可卡因本身不足以引发复发。与其行为效应平行，皮质酮预处理也增强了低剂量可卡因对延髓核细胞外多巴胺浓度的影响，这表明糖皮质激素可能通过增强这一关键奖励处理脑区的多巴胺能神经传递来增强药物寻找。我们正在研究有机阳离子转运蛋白3（一种高容量多巴胺转运蛋白，可被糖皮质激素急性直接抑制）在介导糖皮质激素对多巴胺能神经传递、可卡因复发和啮齿动物动机行为的影响中的作用。由于缺乏OCT 3的特异性抑制剂，我们使用两种不同的遗传方法来测试皮质酮通过抑制OCT 3介导的多巴胺在丘脑核中的清除来增强可卡因诱导的多巴胺能神经传递和药物寻求行为的假设。在第一个目标中，我们将确定皮质酮诱导的多巴胺清除抑制在多巴胺信号传导和药物复发的多巴胺神经核的影响，通过使用体内微透析和快速扫描循环伏安法来测量多巴胺浓度和清除可卡因寻求动物。在第二个目标中，我们将通过检查皮质酮对药物寻求行为和神经核多巴胺信号传导的影响来确定OCT 3在皮质酮的行为和神经化学作用中的作用，这些作用是通过遗传修饰而缺乏OCT 3表达的动物在神经核中的表达来实现的。在第三个目标中，我们将测试皮质酮诱导的多巴胺清除率降低调节奖励敏感性和自然奖励处理的假设。这些发现将彻底描述一种新的机制，通过这种机制，压力激素可以快速调节多巴胺信号，并有助于压力对药物摄入和动机行为的影响。