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多巴胺转运体蛋白质组

The dopamine transporter proteome.

作者信息

Torres Gonzalo E

机构信息

Department of Neurobiology, University of Pittsburgh School of Medicine, Pittsburgh, PA 15261, USA.

出版信息

J Neurochem. 2006 Apr;97 Suppl 1:3-10. doi: 10.1111/j.1471-4159.2006.03719.x.

DOI:10.1111/j.1471-4159.2006.03719.x
PMID:16635244
Abstract

Dopamine (DA) uptake through the neuronal plasma membrane DA transporter (DAT) is essential for the maintenance of normal DA homeostasis in the brain. The DAT-mediated re-uptake system limits not only the intensity but also the duration of DA actions at presynaptic and postsynaptic receptors. This protein is the primary target for cocaine and amphetamine, both highly addictive and major substances of abuse worldwide. DAT is also the molecular target for therapeutic agents used in the treatment of mental disorders, such as attention deficit hyperactivity disorder and depression. Given the role played by the DAT in regulation of DA neurotransmission and its contribution to the abuse potential of psychostimulants, it becomes not only important but also necessary to understand the functional regulation of this protein. To investigate the cellular and molecular mechanisms associated with DAT function and regulation, our laboratory and others have embarked on a systematic search for DAT protein-protein interactions. Recently, a growing number of proteins have been shown to interact with DAT. These novel interactions might be important in the assembly, targeting, trafficking and/or regulation of transporter function. In this review, I summarize the main findings obtained from the characterization of DAT-interacting proteins and discuss the functional implications of these novel interactions. Based on these new data, I propose to use the term DAT proteome to explain how interacting proteins regulate DAT function. These novel interactions might help define new mechanisms associated with the function of the transporter.

摘要

多巴胺(DA)通过神经元质膜多巴胺转运体(DAT)的摄取对于维持大脑中正常的DA稳态至关重要。DAT介导的再摄取系统不仅限制了DA在前突触和后突触受体处作用的强度,还限制了其作用持续时间。该蛋白是可卡因和苯丙胺的主要作用靶点,这两种物质都极易成瘾,是全球主要的滥用物质。DAT也是用于治疗精神障碍(如注意力缺陷多动障碍和抑郁症)的治疗药物的分子靶点。鉴于DAT在调节DA神经传递中的作用及其对精神兴奋剂滥用潜力的影响了解该蛋白的功能调节不仅变得重要而且必要。为了研究与DAT功能和调节相关的细胞和分子机制,我们实验室和其他实验室已着手系统地寻找DAT蛋白-蛋白相互作用。最近,越来越多的蛋白已被证明与DAT相互作用。这些新的相互作用可能在转运体功能的组装、靶向、运输和/或调节中起重要作用。在这篇综述中,我总结了从DAT相互作用蛋白的表征中获得的主要发现,并讨论了这些新相互作用的功能意义。基于这些新数据,我建议使用术语DAT蛋白质组来解释相互作用蛋白如何调节DAT功能。这些新的相互作用可能有助于定义与转运体功能相关的新机制。

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