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表达明显减少的纹状体多巴胺转运体的小鼠表现出增加的运动活性、多巴胺摄取周转率和可卡因反应性。

Mice expressing markedly reduced striatal dopamine transporters exhibit increased locomotor activity, dopamine uptake turnover rate, and cocaine responsiveness.

机构信息

Department of Pharmacology, School of Medicine, University of Colorado, Anschutz Medical Campus, Aurora, Colorado, 80045, USA.

出版信息

Synapse. 2013 Oct;67(10):668-77. doi: 10.1002/syn.21671. Epub 2013 May 30.

Abstract

Variations in the expression levels of the dopamine transporter (DAT) can influence responsiveness to psychostimulant drugs like cocaine. To better understand this relationship, we studied a new DAT-low expresser (DAT-LE) mouse model and performed behavioral and biochemical studies with it. Immunoblotting and [(3) H]WIN 35,428 binding analyses revealed that these mice express ∼35% of wildtype (WT) mouse striatal DAT levels. Compared to WT mice, DAT-LE mice were hyperactive in a novel open-field environment. Despite their higher basal locomotor activity, cocaine (10 or 20 mg/kg, i.p.) induced greater locomotor activation in DAT-LE mice than in WT mice. The maximal velocity (Vmax ) of DAT-mediated [(3) H]DA uptake into striatal synaptosomes was reduced by 46% in DAT-LE mice, as compared to WT. Overall, considering the reduced number of DAT binding sites (Bmax ) along with the reduced Vmax in DAT-LE mice, a 2-fold increase in DA uptake turnover rate (Vmax /Bmax ) was found, relative to WT mice. This suggests that neuroadaptive changes have occurred in the DAT-LE mice that would help to compensate for their low DAT numbers. Interestingly, these changes do not include a reduction in tyrosine hydroxylase levels, as was previously reported in DAT knockout homozygous and heterozygous animals. Further, these changes are not sufficient to prevent elevated novelty- and cocaine-induced locomotor activity. Hence, these mice represent a unique model for studying changes of in vivo DAT function and regulation that result from markedly reduced levels of DAT expression.

摘要

多巴胺转运体(DAT)表达水平的变化会影响对可卡因等精神兴奋剂药物的反应。为了更好地理解这种关系,我们研究了一种新的多巴胺转运体低表达(DAT-LE)小鼠模型,并对其进行了行为和生化研究。免疫印迹和[3H]WIN 35,428 结合分析表明,这些小鼠表达的纹状体 DAT 水平约为野生型(WT)小鼠的 35%。与 WT 小鼠相比,DAT-LE 小鼠在新的开阔环境中表现出过度活跃。尽管它们的基础运动活性较高,但可卡因(10 或 20mg/kg,腹腔注射)在 DAT-LE 小鼠中引起的运动激活比 WT 小鼠更大。与 WT 相比,DAT-LE 小鼠纹状体突触小体中 DAT 介导的[3H]DA 摄取的最大速度(Vmax)降低了 46%。总的来说,考虑到 DAT-LE 小鼠中 DAT 结合位点(Bmax)数量减少以及 Vmax 降低,与 WT 小鼠相比,DA 摄取周转率(Vmax/Bmax)增加了 2 倍。这表明,DAT-LE 小鼠发生了神经适应性变化,这有助于补偿其低 DAT 数量。有趣的是,这些变化不包括酪氨酸羟化酶水平的降低,如之前在 DAT 敲除纯合和杂合动物中报道的那样。此外,这些变化不足以防止新奇感和可卡因诱导的运动活性升高。因此,这些小鼠代表了研究由于 DAT 表达水平明显降低而导致的体内 DAT 功能和调节变化的独特模型。

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