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新型 D1 受体拮抗剂 NNC 756 或 D2 受体拮抗剂氯丙嗪对未经药物处理的恒河猴的影响:肌张力障碍、运动障碍和 D1/D2 超敏反应。

Effect of chronic treatment with NNC 756, a new D-1 receptor antagonist, or raclopride, a D-2 receptor antagonist, in drug-naive Cebus monkeys: dystonia, dyskinesia and D-1/D-2 supersensitivity.

机构信息

St Hans Hospital, Dept. P, Research Institute of Biological Psychiatry, Roskilde, Denmark.

出版信息

J Psychopharmacol. 1993 Jan;7(4):355-64. doi: 10.1177/026988119300700407.

DOI:10.1177/026988119300700407
PMID:22290999
Abstract

When given subcutaneously in gradually increasing doses, up to 1 mg/kg, NNC 756, a dopamine (DA) D-1 antagonist, failed to produce dystonia in eight drug-naive Cebus monkeys. In contrast, raclopride, a DA D-2 antagonist, produced dystonia at low doses (0.010-0.015 mg/kg). Following pre-treatment with raclopride, NNC 756 also induced dystonia at low doses (0.015-0.025 mg/kg), but continued treatment caused tolerance, and increasing doses of NNC 756 could be administered without induction of dystonia. NNC 756 induced a dose-dependent parkinsonism (slow, stiff movements and tremor), and more sedation than raclopride. After treatment for 14 weeks, withdrawal of raclopride (0.01 mg/kg) led to mild oral dyskinesia (tardive dyskinesia), while withdrawal of NNC 756 (1.0 mg/kg) led to a special grooming syndrome, but no dyskinesia. Withdrawal of raclopride as well as NNC 756 led to behavioural D-1 and D-2 dopamine supersensitivity in the form of increased dyskinesia (including grooming after NNC 756) induced by D-1 agonist (SKF 81297) and increased arousal induced by D-2 agonist (quinpirole). These results indicate that D-1 antagonists such as NNC 756 elicit fewer extrapyramidal symptoms (both acute and tardive) than D-2 antagonists such as raclopride, although extremely high doses may cause a special grooming withdrawal syndrome.

摘要

当以逐渐增加的剂量皮下给予时,高达 1mg/kg,NNC 756,一种多巴胺(DA)D-1 拮抗剂,未能在 8 只未经药物治疗的食蟹猴中产生张力障碍。相比之下,一种 DA D-2 拮抗剂,氯普噻吨,在低剂量(0.010-0.015mg/kg)下产生张力障碍。在用氯普噻吨预处理后,NNC 756 也在低剂量(0.015-0.025mg/kg)下引起张力障碍,但持续治疗引起耐受,并且可以给予增加剂量的 NNC 756 而不会引起张力障碍。NNC 756 诱导剂量依赖性帕金森病(缓慢、僵硬的运动和震颤),并且比氯普噻吨更镇静。治疗 14 周后,撤回氯普噻吨(0.01mg/kg)导致轻度口腔运动障碍(迟发性运动障碍),而撤回 NNC 756(1.0mg/kg)导致特殊梳理综合征,但没有运动障碍。撤回氯普噻吨和 NNC 756 导致 D-1 和 D-2 多巴胺受体超敏,表现为 D-1 激动剂(SKF 81297)诱导的运动障碍(包括 NNC 756 后梳理)增加和 D-2 激动剂(喹吡罗)诱导的觉醒增加。这些结果表明,D-1 拮抗剂,如 NNC 756,引起的锥体外系症状(急性和迟发性)比 D-2 拮抗剂,如氯普噻吨,少,尽管极高剂量可能导致特殊梳理综合征。

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