Nicotinic Modulation of the Mesoaccumbens Dopamine System

中伏多巴胺系统的烟碱调节

• 批准号: 7172327
• 负责人: Daniel S McGehee
• 金额: $ 36.15万
• 依托单位: UNIVERSITY OF CHICAGO
• 依托单位国家: 美国
• 财政年份: 2003
• 资助国家: 美国
• 起止时间: 2003-02-01 至 2008-11-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7172327
• 关键词: Acute; Address; Adrenalectomy; Adult; Affect; Animals; Area; Bathing; Behavior; Behavioral; Binding; Biological Assay; Brain; Brain region; Cell Nucleus; Cells; Cellular Assay; Cholinergic Agents; Chromosome Pairing; Chronic; Chronic stress; Daily; Data; Disinhibition; Dopamine; Drosophila acetylcholine receptor alpha-subunit; Drug Addiction; Electrophysiology (science); Environment; Excitatory Synapse; Exhibits; Exposure to; Fire - disasters; Glucocorticoids; Glutamates; Hormones; Immunoblotting; Individual; Infusion procedures; Inhibitory Synapse; Injection of therapeutic agent; Investigation; Ligand Binding; Ligands; Mediating; Membrane; Mental Depression; Midbrain structure; Neonatal; Neurons; Nicotine; Nicotinic Agonists; Nicotinic Receptors; Nucleus Accumbens; Numbers; Pharmaceutical Preparations; Physiological; Physiology; Predisposition; Prevalence; Property; Rate; Rattus; Research Personnel; Rest; Rewards; Self Administration; Self-Administered; Slice; Sprague-Dawley Rats; Stimulus; Stress; Stress Tests; Suggestion; Synapses; Synaptic Transmission; Testing; Time; Tissues; Up-Regulation; Ventral Tegmental Area; addiction; base; cholinergic; day; desensitization; design; dopamine system; dopaminergic neuron; epibatidine; gamma-Aminobutyric Acid; insight; interest; juvenile animal; male; motivated behavior; neurochemistry; novel; presynaptic; programs; protein expression; radioligand; receptor; receptor function; research study; response; transmission process

DESCRIPTION (provided by applicant): Nicotinic acetylcholine receptors (nAChRs) can modify synaptic transmission in many brain regions. Our recent studies show that nAChRs contribute to midbrain dopamine (DA) neuron excitability through modulation of both inhibitory GABAergic and excitatory glutamatergic inputs. The nAChR enhancement of glutamate inputs can contribute to LTP induction at this synapse. Interestingly, the nicotinic modulation of GABA transmission exhibits a transient enhancement, followed by a depression of activity. Apparently, desensitization of the nAChRs on GABA neurons inhibits endogenous cholinergic input to these cells, thus leading to a 'disinhibition' of the DA neurons. These studies were carried out in neonatal rats, primarily for technical reasons. Experiments in this proposal will extend these tests to tissue slices from adult rats that have undergone behavioral and pharmacological testing. The activity that an animal displays in a novel environment can predict nicotine self-administration in rats. The advantage of this screen is that animals predisposed to nicotine self-administration can be identified without nicotine exposure, which is known to alter sensitivity. Our preliminary results indicate differences in nAChR expression between high and low responders to novelty. We will extend these observations to test the differences in cellular and synaptic effects of nAChR activation associated with the predisposition to nicotine self-administration. The activity response to novelty has also been correlated with differences in stress hormone levels between individuals, leading to the suggestion that stress hormones contribute to the predisposition to drug-taking. Preliminary data indicate that stress hormones inhibit nAChRs through a direct interaction. We will test the hypothesis that this interaction upregulates the expression of nAChRs within the reward area, strengthens the cellular response to nicotine and thus, enhances the motivating effects of the drug. Nicotine exposure also enhances the acquisition of self-administration behavior, presumably through upregulation of nAChR expression. We will test nAChR effects on DA neuron excitability from animals that have been pre-exposed to nicotine by passive injection and self-administration testing. These studies of nAChR function within the brain reward center will provide important insights into the cellular basis of addiction.

描述（由申请人提供）：烟碱乙酰胆碱受体（nAChR）可以改变许多脑区的突触传递。我们最近的研究表明，nAChRs通过调节抑制性GABA能和兴奋性多巴胺能输入，促进中脑多巴胺（DA）神经元的兴奋性。谷氨酸输入的nAChR增强可以有助于该突触处的LTP诱导。有趣的是，GABA传输的烟碱调制表现出短暂的增强，随后是活动的抑制。显然，GABA神经元上的nAChRs的脱敏抑制了对这些细胞的内源性胆碱能输入，从而导致DA神经元的“去抑制”。这些研究在新生大鼠中进行，主要是出于技术原因。本提案中的实验将把这些测试扩展到经过行为和药理学测试的成年大鼠的组织切片。动物在新环境中表现出的活动可以预测大鼠的尼古丁自我给药。这种筛选的优点是，可以在没有尼古丁暴露的情况下识别出倾向于尼古丁自我给药的动物，尼古丁暴露已知会改变敏感性。我们的初步研究结果表明，高和低响应新奇性之间的nAChR表达的差异。我们将扩展这些观察结果，以测试与尼古丁自我给药倾向相关的nAChR激活的细胞和突触效应的差异。对新奇事物的活动反应也与个体之间应激激素水平的差异有关，这导致了应激激素有助于吸毒倾向的建议。初步数据表明，应激激素通过直接相互作用抑制nAChR。我们将测试这一假设，即这种相互作用上调奖赏区内nAChR的表达，加强细胞对尼古丁的反应，从而增强药物的激励作用。尼古丁暴露也增强了自我管理行为的获得，可能是通过上调nAChR表达。我们将通过被动注射和自我给药试验，检测nAChR对预先暴露于尼古丁的动物DA神经元兴奋性的影响。这些对大脑奖励中心内nAChR功能的研究将为成瘾的细胞基础提供重要的见解。

项目成果

Nicotine and behavioral sensitization.

• DOI: 10.1007/s12031-009-9230-7
• 发表时间: 2010-01
• 期刊: JOURNAL OF MOLECULAR NEUROSCIENCE
• 影响因子: 3.1
• 作者: Mao, Danyan;McGehee, Daniel S.
• 通讯作者: McGehee, Daniel S.

Nicotine potentiation of excitatory inputs to ventral tegmental area dopamine neurons.

• DOI: 10.1523/jneurosci.5671-10.2011
• 发表时间: 2011-05-04
• 期刊: The Journal of neuroscience : the official journal of the Society for Neuroscience
• 作者: Mao D;Gallagher K;McGehee DS
• 通讯作者: McGehee DS