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有机阳离子转运体 2 控制大脑去甲肾上腺素和 5-羟色胺的清除和抗抑郁反应。

Organic cation transporter 2 controls brain norepinephrine and serotonin clearance and antidepressant response.

机构信息

INSERM U952, Paris, France.

出版信息

Mol Psychiatry. 2012 Sep;17(9):926-39. doi: 10.1038/mp.2011.87. Epub 2011 Jul 19.

Abstract

High-affinity transporters for norepinephrine (NE) and serotonin (5-HT), which ensure neurotransmitter clearance at the synapse, are the principal targets of widely used antidepressant drugs. Antidepressants targeting these high-affinity transporters, however, do not provide positive treatment outcomes for all patients. Other monoamine transport systems, with lower affinity, have been detected in the brain, but their role is largely unknown. Here we report that OCT2, a member of the polyspecific organic cation transporter (OCT) family, is expressed notably in the limbic system and implicated in anxiety and depression-related behaviors in the mouse. Genetic deletion of OCT2 in mice produced a significant reduction in brain tissue concentrations of NE and 5-HT and in ex vivo uptake of both these neurotransmitters in the presence of the dual 5-HT-NE transport blocker, venlafaxine. In vivo clearance of NE and 5-HT evaluated using microiontophoretic electrophysiology was diminished in the hippocampus of OCT2(-/-) mice in the presence of venlafaxine, thereby affecting postsynaptic neuronal activity. OCT2(-/-) mice displayed an altered sensitivity to acute treatments with NE- and/or 5-HT-selective transport blockers in the forced-swim test. Moreover, the mutant mice were insensitive to long-term venlafaxine treatment in a more realistic, corticosterone-induced, chronic depression model. Our findings identify OCT2 as an important postsynaptic determinant of aminergic tonus and mood-related behaviors and a potential pharmacological target for mood disorders therapy.

摘要

高亲和力去甲肾上腺素 (NE) 和 5-羟色胺 (5-HT) 转运体可确保突触间隙神经递质的清除,是广泛使用的抗抑郁药的主要作用靶点。然而,针对这些高亲和力转运体的抗抑郁药并不能为所有患者提供积极的治疗效果。大脑中还检测到了具有较低亲和力的其他单胺转运系统,但它们的作用在很大程度上尚不清楚。在这里,我们报告多药/有机阳离子转运体(OCT)家族成员 OCT2 在边缘系统中表达显著,并与小鼠的焦虑和抑郁相关行为有关。OCT2 基因敲除小鼠的脑内 NE 和 5-HT 浓度显著降低,在 5-HT-NE 双转运体阻滞剂文拉法辛存在的情况下,对这两种神经递质的体外摄取也显著减少。使用微电泳电生理学评估体内 NE 和 5-HT 的清除率时,文拉法辛存在时,OCT2(-/-) 小鼠的海马区清除率降低,从而影响突触后神经元的活性。OCT2(-/-) 小鼠在强迫游泳试验中对 NE 和/或 5-HT 选择性转运体阻滞剂的急性处理表现出不同的敏感性。此外,在更现实的皮质酮诱导的慢性抑郁模型中,突变小鼠对长期文拉法辛治疗不敏感。我们的研究结果表明,OCT2 是胺能张力和与情绪相关行为的重要突触后决定因素,也是治疗情绪障碍的潜在药理学靶点。

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