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多巴胺 D-1 受体激动剂与选择性 D-2 激动剂喹吡罗联合使用可促进大鼠口腔刻板行为的表达。

Dopamine D-1 receptor agonists combined with the selective D-2 agonist quinpirole facilitate the expression of oral stereotyped behaviour in rats.

作者信息

Arnt J, Hyttel J, Perregaard J

出版信息

Eur J Pharmacol. 1987 Jan 13;133(2):137-45. doi: 10.1016/0014-2999(87)90144-0.

Abstract

The behaviour of rats was studied after combined treatment with the selective DA D-2 agonist quinpirole and three selective D-1 agonists (SK & F 38393, SK & F 75670 and Lu 24-040). The effects on behaviour were compared with those on receptor binding and adenylate cyclase (AC). While the D-1 agonists alone did not induce stereotyped behaviour, quinpirole induced dose-dependent hyperactivity (locomotion, sniffing, head movements and rearing), whereas licking/biting was absent or seen only occasionally. Combined treatment with quinpirole and a D-1 agonist was followed by dose-dependent licking and occasional biting behaviour. The D-1 agonists had similar efficacies, but SK & F 75670 and Lu 24-040 were more potent than SK & F 38393. The maximal effects of SK & F 38393 plus quinpirole were effectively blocked by either a D-1 antagonist (SCH 23390) or a D-2 antagonist (YM 09151-2) confirming the close relation between D-1 and D-2 receptor sites in the brain. Good correspondence was found between affinities to D-1 receptors [( 3H]SCH 23390 binding) in vitro and the EC50 values for stimulation of AC activity. However, the maximal effects on DA-sensitive AC activity were less for SK & F 75670 and Lu 24-040 than for SK & F 38393. Thus, the results indicate that efficacies in the adenylate cyclase assay are dissociated from those on behaviour. Furthermore, the data indicate that in normal rats D-1 receptors are functionally relevant since D-1 agonists facilitate the expression of oral stereotyped behaviour after combination with a D-2 agonist.

摘要

研究了大鼠在选择性多巴胺D-2激动剂喹吡罗与三种选择性D-1激动剂(SK & F 38393、SK & F 75670和Lu 24-040)联合治疗后的行为。将其对行为的影响与对受体结合和腺苷酸环化酶(AC)的影响进行了比较。虽然单独使用D-1激动剂不会诱发刻板行为,但喹吡罗会诱发剂量依赖性多动(运动、嗅探、头部运动和竖毛),而舔舐/咬啮行为不存在或仅偶尔出现。喹吡罗与D-1激动剂联合治疗后会出现剂量依赖性舔舐和偶尔的咬啮行为。D-1激动剂具有相似的效力,但SK & F 75670和Lu 24-040比SK & F 38393更有效。SK & F 38393加喹吡罗的最大效应可被D-1拮抗剂(SCH 23390)或D-2拮抗剂(YM 09151-2)有效阻断,这证实了大脑中D-1和D-2受体位点之间的密切关系。在体外对D-1受体的亲和力[(3H]SCH 23390结合)与刺激AC活性的EC50值之间发现了良好的对应关系。然而,SK & F 75670和Lu 24-040对多巴胺敏感的AC活性的最大效应低于SK & F 38393。因此,结果表明腺苷酸环化酶测定中的效力与对行为的效力不同。此外,数据表明在正常大鼠中D-1受体在功能上是相关的,因为D-1激动剂与D-2激动剂联合后促进了口腔刻板行为的表达。

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