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多巴胺转运体和囊泡单胺转运体-2功能的年龄依赖性差异及其对甲基苯丙胺神经毒性的影响。

Age-dependent differences in dopamine transporter and vesicular monoamine transporter-2 function and their implications for methamphetamine neurotoxicity.

作者信息

Volz Trent J, Farnsworth Sarah J, Rowley Shane D, Hanson Glen R, Fleckenstein Annette E

机构信息

Department of Pharmacology and Toxicology, University of Utah, Salt Lake City, Utah 84112, USA.

出版信息

Synapse. 2009 Feb;63(2):147-51. doi: 10.1002/syn.20580.

DOI:10.1002/syn.20580
PMID:19021208
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2605157/
Abstract

The abuse of methamphetamine (METH) is a serious public health problem because METH can cause persistent dopaminergic deficits in the brains of both animal models and humans. Surprisingly, adolescent postnatal day (PND)40 rats are resistant to these METH-induced deficits, whereas young adult PND90 rats are not. Studies described in this report used rotating disk electrode voltammetry and western blotting techniques to investigate whether there are age-dependent differences in monoamine transporter function in PND38-42 and PND88-92 rats that could contribute to this phenomenon. The initial velocities of dopamine (DA) transport into, METH-induced DA efflux from, and DA transporter (DAT) immunoreactivity in striatal suspensions are greater in PND38-42 rats than in PND88-92 rats. DA transport velocities into vesicles that cofractionate with synaptosomal membranes after osmotic lysis are also greater in PND38-42 rats. However, there is no difference in vesicular monoamine transporter-2 (VMAT-2) immunoreactivity between the two age groups in this fraction. This suggests that younger rats have a greater capacity to sequester cytoplasmic DA into membrane-associated vesicles due to kinetically upregulated VMAT-2 and also have increased levels of functionally active DAT. In the presence of METH, these may provide additional routes of cellular efflux for DA that is released from vesicles into the cytoplasm and thereby prevent cytoplasmic DA concentrations in younger rats from rising to neurotoxic levels after drug administration. These findings provide novel insight into the age-dependent physiological regulation of neuronal DA sequestration and may advance the treatment of disorders involving abnormal DA disposition including substance abuse and Parkinson's disease.

摘要

甲基苯丙胺(METH)的滥用是一个严重的公共卫生问题,因为METH会在动物模型和人类大脑中导致持续性多巴胺能缺陷。令人惊讶的是,出生后第40天(PND)的青春期大鼠对这些METH诱导的缺陷具有抗性,而出生后第90天的年轻成年大鼠则不然。本报告中描述的研究使用旋转圆盘电极伏安法和蛋白质印迹技术,来研究在PND38 - 42和PND88 - 92大鼠中,单胺转运体功能是否存在年龄依赖性差异,这可能导致了这种现象。在纹状体悬浮液中,多巴胺(DA)转运进入、METH诱导的DA流出以及DA转运体(DAT)免疫反应性的初始速度,在PND38 - 42大鼠中比在PND88 - 92大鼠中更高。在渗透裂解后与突触体膜共分离的囊泡中,DA的转运速度在PND38 - 42大鼠中也更高。然而,在这一部分中,两个年龄组之间的囊泡单胺转运体2(VMAT - 2)免疫反应性没有差异。这表明,由于VMAT - 2在动力学上上调,年幼大鼠将细胞质DA隔离到膜相关囊泡中的能力更强,并且功能活跃的DAT水平也有所增加。在存在METH的情况下,这些可能为从囊泡释放到细胞质中的DA提供额外的细胞外排途径,从而防止年幼大鼠在给药后细胞质DA浓度上升到神经毒性水平。这些发现为神经元DA隔离的年龄依赖性生理调节提供了新的见解,并可能推进对涉及异常DA处置的疾病的治疗,包括药物滥用和帕金森病。

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