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脑内有机阳离子转运体概述。

General Overview of Organic Cation Transporters in Brain.

机构信息

Institute of Anatomy and Cell Biology, University Würzburg, Würzburg, Germany.

出版信息

Handb Exp Pharmacol. 2021;266:1-39. doi: 10.1007/164_2021_449.

DOI:10.1007/164_2021_449
PMID:33782773
Abstract

Inhibitors of Na/Cl dependent high affinity transporters for norepinephrine (NE), serotonin (5-HT), and/or dopamine (DA) represent frequently used drugs for treatment of psychological disorders such as depression, anxiety, obsessive-compulsive disorder, attention deficit hyperactivity disorder, and addiction. These transporters remove NE, 5-HT, and/or DA after neuronal excitation from the interstitial space close to the synapses. Thereby they terminate transmission and modulate neuronal behavioral circuits. Therapeutic failure and undesired central nervous system side effects of these drugs have been partially assigned to neurotransmitter removal by low affinity transport. Cloning and functional characterization of the polyspecific organic cation transporters OCT1 (SLC22A1), OCT2 (SLC22A2), OCT3 (SLC22A3) and the plasma membrane monoamine transporter PMAT (SLC29A4) revealed that every single transporter mediates low affinity uptake of NE, 5-HT, and DA. Whereas the organic transporters are all located in the blood brain barrier, OCT2, OCT3, and PMAT are expressed in neurons or in neurons and astrocytes within brain areas that are involved in behavioral regulation. Areas of expression include the dorsal raphe, medullary motoric nuclei, hypothalamic nuclei, and/or the nucleus accumbens. Current knowledge of the transport of monoamine neurotransmitters by the organic cation transporters, their interactions with psychotropic drugs, and their locations in the brain is reported in detail. In addition, animal experiments including behavior tests in wildtype and knockout animals are reported in which the impact of OCT2, OCT3, and/or PMAT on regulation of salt intake, depression, mood control, locomotion, and/or stress effect on addiction is suggested.

摘要

Na+/Cl-依赖性高亲和力转运体抑制剂可用于治疗去甲肾上腺素 (NE)、5-羟色胺 (5-HT) 和/或多巴胺 (DA) 相关的心理障碍,如抑郁症、焦虑症、强迫症、注意缺陷多动障碍和成瘾。这些转运体将神经元兴奋后释放到突触附近细胞间隙的 NE、5-HT 和/或 DA 摄取回细胞内,从而终止神经递质传递并调节神经元行为回路。这些药物治疗失败和中枢神经系统不良反应部分归因于低亲和力转运体对神经递质的摄取。多药和有机阳离子转运体 OCT1(SLC22A1)、OCT2(SLC22A2)、OCT3(SLC22A3)和单胺转运体 PMAT(SLC29A4)的克隆和功能特征表明,每一种转运体都可以低亲和力摄取 NE、5-HT 和 DA。虽然有机转运体均位于血脑屏障,但 OCT2、OCT3 和 PMAT 均在脑内参与行为调节的神经元或神经元-星形胶质细胞中表达。表达区域包括中缝背核、延髓运动核、下丘脑核和/或伏隔核。本文详细报道了单胺神经递质经有机阳离子转运体的转运、转运体与精神药物的相互作用及其在脑中的分布情况。此外,还报道了一些动物实验,包括野生型和敲除动物的行为测试,提示 OCT2、OCT3 和/或 PMAT 可能影响盐摄入、抑郁、情绪控制、运动和/或应激对成瘾的调节。

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