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长期口服哌醋甲酯治疗可使大鼠纹状体多巴胺转运体和多巴胺1型受体结合可逆性增加。

Chronic oral methylphenidate treatment reversibly increases striatal dopamine transporter and dopamine type 1 receptor binding in rats.

作者信息

Robison Lisa S, Ananth Mala, Hadjiargyrou Michael, Komatsu David E, Thanos Panayotis K

机构信息

Department of Psychology, Stony Brook University, 100 Nicolls Road, Stony Brook, NY, 11794, USA.

Department of Neurobiology, Stony Brook University, 100 Nicolls Road, Stony Brook, NY, 11794, USA.

出版信息

J Neural Transm (Vienna). 2017 May;124(5):655-667. doi: 10.1007/s00702-017-1680-4. Epub 2017 Jan 23.

Abstract

Previously, we created an 8-h limited-access dual bottle drinking paradigm to deliver methylphenidate (MP) to rats at two dosages that result in a pharmacokinetic profile similar to patients treated for attention deficit hyperactivity disorder. Chronic treatment resulted in altered behavior, with some effects persisting beyond treatment. In the current study, adolescent male Sprague-Dawley rats were split into three groups at four weeks of age: control (water), low-dose MP (LD), and high-dose MP (HD). Briefly, 4 mg/kg (low dose; LD) or 30 mg/kg (high dose; HD) MP was consumed during the first hour, and 10 mg/kg (LD) or 60 mg/kg (HD) MP during hours two through eight. Following three months of treatment, half of the rats in each group (n = 8-9/group) were euthanized, and remaining rats went through a 1-month abstinence period, then euthanized. In vitro receptor autoradiography was performed to quantify binding levels of dopamine transporter (DAT), dopamine type 1 (D1R)-like receptors, and dopamine type 2 (D2R)-like receptors using [H] WIN35,428, [H] SCH23390, and [H] Spiperone, respectively. Immediately following treatment, HD MP-treated rats had increased DAT and D1R-like binding in several subregions of the basal ganglia, particularly more caudal portions of the caudate putamen, which correlated with some previously reported behavioral changes. There were no differences between treatment groups in any measure following abstinence. These findings suggest that chronic treatment with a clinically relevant high dose of MP results in reversible changes in dopamine neurochemistry, which may underlie some effects on behavior.

摘要

此前,我们创建了一种8小时限时双瓶饮水范式,以两种剂量给大鼠投喂哌甲酯(MP),这两种剂量产生的药代动力学特征与接受注意力缺陷多动障碍治疗的患者相似。长期治疗导致行为改变,有些影响在治疗后仍持续存在。在当前研究中,青春期雄性斯普拉格-道利大鼠在4周龄时被分为三组:对照组(饮水)、低剂量MP组(LD)和高剂量MP组(HD)。简而言之,在第一个小时摄入4mg/kg(低剂量;LD)或30mg/kg(高剂量;HD)的MP,在第二至八小时摄入10mg/kg(LD)或60mg/kg(HD)的MP。经过三个月的治疗后,每组中的一半大鼠(每组n = 8 - 9)被安乐死,其余大鼠经历1个月的戒断期,然后被安乐死。使用[H] WIN35,428、[H] SCH23390和[H] 螺哌隆分别进行体外受体放射自显影,以量化多巴胺转运体(DAT)、多巴胺1型(D1R)样受体和多巴胺2型(D2R)样受体的结合水平。治疗后立即发现,高剂量MP治疗的大鼠在基底神经节的几个亚区域中DAT和D1R样结合增加,特别是尾状壳核的更尾端部分,这与一些先前报道的行为变化相关。戒断后,各治疗组在任何测量指标上均无差异。这些发现表明,临床相关高剂量的MP长期治疗会导致多巴胺神经化学的可逆变化,这可能是对行为产生某些影响的基础。

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