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全效D1多巴胺受体激动剂对体内苍白球和黑质致密部放电频率的影响:D1受体选择性测试及与部分激动剂SKF 38393的比较

Effects of full D1 dopamine receptor agonists on firing rates in the globus pallidus and substantia nigra pars compacta in vivo: tests for D1 receptor selectivity and comparisons to the partial agonist SKF 38393.

作者信息

Ruskin D N, Rawji S S, Walters J R

机构信息

Experimental Therapeutics Branch, National Institutes of Health, Bethesda, Maryland, USA.

出版信息

J Pharmacol Exp Ther. 1998 Jul;286(1):272-81.

PMID:9655869
Abstract

Many studies have used the D1 agonist SKF 38393 to characterize D1 receptor influences on firing rates in basal ganglia nuclei in vivo. However, SKF 38393 is a partial agonist and so may not be ideal for delineating D1 receptor effects. This study characterizes the effects of four full D1 agonists, SKF 82958 (chloro-APB), SKF 81297 (6-chloro-PB), dihydrexidine and A-77636, on the firing rates of midbrain dopamine and globus pallidus neurons. Recordings were done in fully anesthetized or paralyzed, locally anesthetized rats, and drugs were given systemically intravenously. Dihydrexidine, SKF 81297 and A-77636 were free of rate effects on midbrain dopamine neurons (up to 10.2 mg/kg) and also did not antagonize the inhibitory effects of quinpirole. In contrast, SKF 82958 strongly inhibited dopamine cells through activation of D2 autoreceptors (ED50 = 0.70 mg/kg). Of these drugs, SKF 82958 also was the only one to increase pallidal unit firing rates when given alone (at 5.0 but not 1.0 mg/kg); the other compounds appeared to be selective for postsynaptic D1 receptors. The results suggest that SKF 82958 may be more properly classified as a mixed D1/D2 agonist. In addition, all four agonists strongly potentiated the pallidal response to quinpirole, demonstrating a D1 receptor potentiation of D2 receptor effects. The results support the role of D1 receptors in the midbrain and globus pallidus as previously characterized with SKF 38393. The similar actions of partial and full D1 agonists in these systems support evidence for a D1 receptor reserve and possibly an effector system other than adenylate cyclase.

摘要

许多研究使用D1激动剂SKF 38393来表征D1受体对体内基底神经节核团放电率的影响。然而,SKF 38393是一种部分激动剂,因此可能不是描绘D1受体效应的理想药物。本研究表征了四种完全D1激动剂SKF 82958(氯-APB)、SKF 81297(6-氯-PB)、二氢麦角隐亭和A-77636对中脑多巴胺能神经元和苍白球神经元放电率的影响。实验在完全麻醉或麻痹、局部麻醉的大鼠中进行,药物通过静脉全身给药。二氢麦角隐亭、SKF 81297和A-77636对中脑多巴胺能神经元无放电率影响(高达10.2mg/kg),也不拮抗喹吡罗的抑制作用。相比之下,SKF 82958通过激活D2自身受体强烈抑制多巴胺能细胞(半数有效剂量=0.70mg/kg)。在这些药物中,SKF 82958也是唯一单独给药时(5.0mg/kg而非1.0mg/kg)能增加苍白球单位放电率的药物;其他化合物似乎对突触后D1受体具有选择性。结果表明,SKF 82958可能更恰当地归类为混合D1/D2激动剂。此外,所有四种激动剂均强烈增强了苍白球对喹吡罗的反应,表明D1受体对D2受体效应具有增强作用。结果支持了D1受体在中脑和苍白球中的作用,这与之前使用SKF 38393所表征的一致。部分和完全D1激动剂在这些系统中的相似作用支持了D1受体储备的证据,以及可能存在除腺苷酸环化酶以外的效应系统。

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