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Activators of G-protein signaling 3: a drug addiction molecular gateway.

机译:G蛋白信号激活因子3:药物成瘾分子通道。

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Drug addiction is marked by continued drug-seeking behavior despite deleterious consequences and a heightened propensity to relapse not withstanding long, drug-free periods. The enduring nature of addiction has been hypothesized to arise from perturbations in intracellular signaling, gene expression, and brain circuitry induced by substance abuse. Ameliorating some of these aberrations should abate behavioral and neurochemical markers associated with an 'addiction phenotype'. This review summarizes data showing that protein expression and signaling through the nonreceptor activator of G-protein signaling 3 (AGS3) are altered by commonly abused substances in rat and in in-vitro addiction models. AGS3 structure and function are unrelated to the more broadly studied regulator of G-protein signaling family. Thus, the unique role of AGS3 is the focus of this review. Intriguingly, AGS3 protein changes persist into drug abstinence. Accordingly, studies probing the role of AGS3 in the neurochemistry of drug-seeking behavior and relapse are studied in detail. To illuminate this study, AGS3 structure, cellular localization, and function are covered so that an idealized AGS3-targeted pharmacotherapy can be proposed.
机译:药物成瘾的特征是尽管有有害后果,但仍继续寻求药物,即使没有长期无毒品的时期,其复发的可能性也增加。据推测,成瘾的持久性是由药物滥用引起的细胞内信号传导,基因表达和大脑回路的扰动引起的。改善其中一些畸变应减轻与“成瘾表型”有关的行为和神经化学标记。这篇综述总结了数据,显示在大鼠和体外成瘾模型中,常见的滥用物质会改变G蛋白信号传导3(AGS3)的非受体激活物的蛋白表达和信号传导。 AGS3的结构和功能与更广泛研究的G蛋白信号转导家族无关。因此,AGS3的独特作用是本综述的重点。有趣的是,AGS3蛋白的变化持续存在于药物戒断中。因此,详细研究了探索AGS3在药物寻找行为和复发的神经化学中的作用的研究。为了阐明本研究,本文涵盖了AGS3的结构,细胞定位和功能,因此可以提出理想的AGS3靶向药物治疗。

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