Arnt J, Bøgesø K P, Hyttel J, Meier E
Research Laboratories, H. Lundbeck A/S, Valby, Denmark.
Pharmacol Toxicol. 1988 Mar;62(3):121-30. doi: 10.1111/j.1600-0773.1988.tb01859.x.
The effects of a range of dopamine (DA) agonists on stereotyped behaviour in rats were analysed and compared both with the affinity of the compounds for D1 and D2 receptor binding sites in vitro and their ability to stimulate the adenylate cyclase activity in rat striatal homogenates. Full and partial agonists at the D1 receptor coupled to adenylate cyclase do not induce sterotypies when given alone, whereas full D2 agonists (e.g. quinpirole) induce hyperactivity but not oral sterotypies. Partial D2 agonists (e.g. (-)-3-PPP) only induce sedation. Mixed D1/D2 agonists (e.g. apomorphine) induce both hyperactivity and oral stereotypies. Maximum stereotypies were induced by combination of SK & F 38393 and a series of D2 agonists, including full agonists and the partial D2 agonist B-HT 920, whereas partial agonists with low intrinsic activity (e.g. (-)-3-PPP, EMD 23448) did not induce stereotypies when given together with SK & F 38393. However, these partial agonists reduced the maximum effect of apomorphine, whereas the full agonists (e.g. quinpirole, (-)-NPA) and B-HT 920 had no apomorphine antagonistic activity. The mixed D1/D2 agonists apomorphine and N,N-dipropyl-5,6-ADTN were only weakly influenced by SK & F 38393, or not at all. D1 agonists with central effects, including SK & F 38393, SK & F 81297 (with relatively high efficacies), and the partial agonist SK & F 75670 with low efficacy, changed the hyperactivity induced by quinpirole into maximum oral stereotypy, whereas the peripheral D1 agonist fenoldopam had no such effect. Inhibition of DA and NA synthesis with alpha-methyl-p-tyrosine depleted striatal DA levels by 72 per cent and antagonized the hyperactivity induced by the D2 agonists quinpirole and (-)-NPA, but not that of apomorphine. Combination of SK & F 38393 and quinpirole induced maximum stereotypy in DA-depleted animals. These results suggest that D1 receptor tonus is a necessary prerequisite for the expression of a DA agonist's effect. The hyperactivity induced by full D2 agonists appears to be mediated by D1 tonus provided by endogenous DA activity, but stronger D1 stimulation is necessary to induce oral stereotypy. A high degree of D1 receptor activation increases the ability of partial D2 agonists to induce hyperactivity or oral stereotypies since treatment with both SK & F 38393 and B-HT 920 had marked effects while B-HT 920 was ineffective.(ABSTRACT TRUNCATED AT 400 WORDS)
分析并比较了一系列多巴胺(DA)激动剂对大鼠刻板行为的影响,同时将这些化合物在体外对D1和D2受体结合位点的亲和力以及它们刺激大鼠纹状体匀浆中腺苷酸环化酶活性的能力进行了比较。与腺苷酸环化酶偶联的D1受体的完全激动剂和部分激动剂单独给药时不会诱导刻板行为,而D2完全激动剂(如喹吡罗)会诱导多动但不会诱导口部刻板行为。D2部分激动剂(如(-)-3-PPP)仅诱导镇静作用。D1/D2混合激动剂(如阿扑吗啡)会诱导多动和口部刻板行为。SK&F 38393与一系列D2激动剂(包括完全激动剂和D2部分激动剂B-HT 920)联合使用可诱导最大程度的刻板行为,而内在活性低的部分激动剂(如(-)-3-PPP、EMD 23448)与SK&F 38393一起给药时不会诱导刻板行为。然而,这些部分激动剂会降低阿扑吗啡的最大效应,而完全激动剂(如喹吡罗、(-)-NPA)和B-HT 920没有阿扑吗啡拮抗活性。D1/D2混合激动剂阿扑吗啡和N,N-二丙基-5,6-ADTN仅受到SK&F 38393的微弱影响,或根本不受影响。具有中枢作用的D1激动剂,包括SK&F 38393、SK&F 81297(具有相对较高的效能)和效能低的部分激动剂SK&F 75670,可将喹吡罗诱导的多动转变为最大程度的口部刻板行为,而外周D1激动剂非诺多泮则没有这种作用。用α-甲基-p-酪氨酸抑制多巴胺和去甲肾上腺素合成可使纹状体多巴胺水平降低72%,并拮抗D2激动剂喹吡罗和(-)-NPA诱导的多动,但不能拮抗阿扑吗啡诱导的多动。SK&F 38393和喹吡罗联合使用可在多巴胺耗竭的动物中诱导最大程度的刻板行为。这些结果表明,D1受体张力是多巴胺激动剂效应表达的必要前提。D2完全激动剂诱导的多动似乎是由内源性多巴胺活性提供的D1张力介导的,但诱导口部刻板行为需要更强的D1刺激。高度的D1受体激活会增加D2部分激动剂诱导多动或口部刻板行为的能力,因为同时用SK&F 38393和B-HT 920治疗有显著效果,而B-HT 920单独使用无效。(摘要截选至400字)
