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长期使用抗精神病药物治疗后对多巴胺能药物的敏感性增加。

Increased sensitivity to dopaminergic agents after chronic neuroleptic treatment.

作者信息

Vonvoigtlander P F, Losey E G, Triezenberg H J

出版信息

J Pharmacol Exp Ther. 1975 Apr;193(1):88-94.

PMID:166158
Abstract

Male CF-1 mice were treated for 14 days with diets containing haloperidol, thioridazine HCl and 4'-fluoro-4[[4-(p-fluorophenyl)-4-methoxycyclohexyl]-amino]-butyrophenone HCl (U35,777A). At various times during and after neuroleptic treatment, spontaneous and d-amphetamine-stimulated motor activity were measured. Two days after cessation of treatment, the mice displayed enhanced spontaneous and d-amphetamine-stimulated motor activity. This effect was no longer apparent 9 days after neuroleptic intake was terminated. With a quantal test based on the climbing activity induced by apomorphine, it was determined that mice were also supersensitive to apomorphine at 2 days but not 9 days after withdrawal from chronic haloperidol. In an attempt to correlate this supersensitivity to a biochemical parameter related to receptor function, dopamine-stimulated adenyl cyclase activity was assayed in striatal homogenates of mice 2 days after haloperidol withdrawal. No alteration in this parameter was observed. Likewise, the ability of apomorphine to elevate striatal cyclic adenosine monophosphate concentrations in vivo was unaltered by withdrawal from chronic haloperidol. Chronic treatment with neuroleptics results in a brief supersensitivity to dopaminergic agents. This effect does not appear to be accompanied by increases in dopamine-stimulated adenyl cyclase activity in the corpus striatum.

摘要

雄性CF-1小鼠用含有氟哌啶醇、盐酸硫利达嗪和4'-氟-4[[4-(对氟苯基)-4-甲氧基环己基]-氨基]-丁酰苯盐酸盐(U35,777A)的饮食治疗14天。在抗精神病药物治疗期间和之后的不同时间,测量自发和右旋苯丙胺刺激的运动活动。治疗停止两天后,小鼠表现出自发和右旋苯丙胺刺激的运动活动增强。在抗精神病药物摄入终止9天后,这种效应不再明显。通过基于阿扑吗啡诱导的攀爬活动的定量试验,确定小鼠在从慢性氟哌啶醇撤药后2天对阿扑吗啡也超敏感,但9天后不超敏感。为了将这种超敏感性与与受体功能相关的生化参数相关联,在氟哌啶醇撤药2天后,测定小鼠纹状体匀浆中多巴胺刺激的腺苷酸环化酶活性。未观察到该参数的改变。同样,慢性氟哌啶醇撤药并未改变阿扑吗啡在体内升高纹状体环磷酸腺苷浓度的能力。慢性使用抗精神病药物会导致对多巴胺能药物出现短暂的超敏感性。这种效应似乎并未伴随纹状体中多巴胺刺激的腺苷酸环化酶活性增加。

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