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首页> 外文期刊>Biological psychiatry >From Signaling Molecules to Circuits and Behaviors: Cell-Type-Specific Adaptations to Psychostimulant Exposure in the Striatum
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From Signaling Molecules to Circuits and Behaviors: Cell-Type-Specific Adaptations to Psychostimulant Exposure in the Striatum

机译:从信号分子到电路和行为:细胞类型特异性适应纹理中的精神疗法暴露

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摘要

Addiction is characterized by a compulsive pattern of drug seeking and consumption and a high risk of relapse after withdrawal that are thought to result from persistent adaptations within brain reward circuits. Drugs of abuse increase dopamine (DA) concentration in these brain areas, including the striatum, which shapes an abnormal memory trace of drug consumption that virtually highjacks reward processing. Long-term neuronal adaptations of gamma-aminobutyric acidergic striatal projection neurons (SPNs) evoked by drugs of abuse are critical for the development of addiction. These neurons form two mostly segregated populations, depending on the DA receptor they express and their output projections, constituting the so-called direct (D-1 receptor) and indirect (D-2 receptor) SPN pathways. Both SPN subtypes receive converging glutamate inputs from limbic and cortical regions, encoding contextual and emotional information, together with DA, which mediates reward prediction and incentive values. DA differentially modulates the efficacy of glutamate synapses onto direct and indirect SPN pathways by recruiting distinct striatal signaling pathways, epigenetic and genetic responses likely involved in the transition from casual drug use to addiction. Herein we focus on recent studies that have assessed psychostimulant-induced alterations in a cell-type-specific manner, from remodeling of input projections to the characterization of specific molecular events in each SPN subtype and their impact on long-lasting behavioral adaptations. We discuss recent evidence revealing the complex and concerted action of both SPN populations on drug-induced behavioral responses, as these studies can contribute to the design of future strategies to alleviate specific behavioral components of addiction.
机译:成瘾的特征是,戒断后的药物寻求和消费的强迫模式和高风险,被认为是脑奖励电路内的持续改编。滥用药物增加了这些脑区域中的多巴胺(DA)浓度,包括纹状体,这造成了几乎高速公路的药物消耗的异常记忆迹线,几乎高速公堂奖励处理。由滥用药物引起的γ-氨基丁基型纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹纹状体这些神经元形成两个大多数隔离的群体,这取决于它们表达的DA受体及其输出突起,构成所谓的直接(D-1受体)和间接(D-2受体)SPN途径。 SPN亚型均接收来自林和皮质地区的谷氨酸输入,与DA一起编码上下文和情绪信息,介导奖励预测和激励价值。 Da差异地调节谷氨酸突触通过募集从休闲药用法过渡到成瘾的不同纹状体信号通路,表观遗传和遗传反应来调节直接和间接的SPN途径。在此,我们专注于最近的研究,这些研究以细胞类型特异性方式评估了精神潜力诱导的改变,从重塑输入突起对每个SPN亚型的特定分子事件的表征及其对长期行为适应的影响。我们讨论最近的证据表明SPN群体对药物引起的行为反应的复杂和协调一致的作用,因为这些研究可以促进未来策略的设计,以减轻成瘾的特定行为组成部分。

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