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向小脑小叶9/10微量注射多巴胺D2/D3受体激动剂和拮抗剂后运动活性降低:一种D3受体介导的效应?

Decreased locomotor activity after microinjection of dopamine D2/D3 receptor agonists and antagonists into lobule 9/10 of the cerebellum: a D3 receptor mediated effect?

作者信息

Boulay D, Depoortere R, Perrault G, Sanger D J

机构信息

Synthélabo Recherche, Bagneux, France.

出版信息

Prog Neuropsychopharmacol Biol Psychiatry. 2000 Jan;24(1):39-49. doi: 10.1016/s0278-5846(99)00079-2.

DOI:10.1016/s0278-5846(99)00079-2
PMID:10659982
Abstract

The restricted localization of dopamine (DA) D3 receptors in the rat cerebellum lobule 9/10 appears to provide a method for investigating the in vivo selectivity of dopaminergic compounds for the D3 receptor subtype. Sprague-Dawley rats implanted with a cannula aimed at lobule 9/10 were microinjected with DA receptor ligands and immediately placed into activity chambers to record their spontaneous locomotor activity for short term (0 to 20 min) and delayed (20 to 40 min) effects. The DA D2/D3 receptor agonists quinelorane (0.1 to 2.5 microg) and 7-OH-DPAT (0.1 to 10 microg) decreased locomotor activity in the first 20 min post-microinjection. In contrast, the DAD1, receptor agonist 6-Br-APB (0.1 to 10 microg) did not affect locomotor activity during this time period, but markedly increased locomotion between 20 and 40 min at the highest dose tested. The DA receptor antagonists haloperidol and raclopride (1 to 10 microg) were also found to reduce locomotor activity. Furthermore, quinelorane and 7-OH-DPAT, but not haloperidol, when microinjected into lobules 1/2 or 6/7 (where no DA D3 receptors have been detected) decreased locomotor scores. These results show that both DA receptor agonists and antagonists decrease locomotor activity when microinjected into lobule 9/10 of the cerebellum. Additionally, DA receptor agonists can reduce spontaneous locomotion when microinjected outside of lobule 9/10. This would suggest that, at least for quinelorane and 7-OH-DPAT, the locomotor decreasing effects following microinjection into cerebellar lobule 9/10 may not be mediated by activity at DA D3 receptors, and that this behavioural assay is unlikely to provide a means for studying the in vivo pharmacology of the DA D3 receptor.

摘要

多巴胺(DA)D3受体在大鼠小脑9/10小叶中的局限性定位似乎为研究多巴胺能化合物对D3受体亚型的体内选择性提供了一种方法。将植入了针对9/10小叶的套管的斯普拉格-道利大鼠微量注射多巴胺受体配体,并立即放入活动箱中,记录其短期(0至20分钟)和延迟(20至40分钟)的自发运动活动。DA D2/D3受体激动剂喹吡罗(0.1至2.5微克)和7-羟基-DPAT(0.1至10微克)在微量注射后的前20分钟内降低了运动活动。相比之下,DAD1受体激动剂6-溴-APB(0.1至10微克)在此时间段内不影响运动活动,但在测试的最高剂量下,在20至40分钟之间显著增加了运动。还发现多巴胺受体拮抗剂氟哌啶醇和雷氯必利(1至10微克)可降低运动活动。此外,当将喹吡罗和7-羟基-DPAT微量注射到1/2或6/7小叶(未检测到DA D3受体)时,运动评分降低,但氟哌啶醇没有这种作用。这些结果表明,多巴胺受体激动剂和拮抗剂微量注射到小脑9/10小叶时均会降低运动活动。此外,多巴胺受体激动剂微量注射到9/10小叶之外时可降低自发运动。这表明,至少对于喹吡罗和7-羟基-DPAT,微量注射到小脑9/10小叶后运动减少的作用可能不是由DA D3受体的活性介导的,并且这种行为测定不太可能提供一种研究DA D3受体体内药理学的方法。

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