间歇性使用短效抗精神病药哌啶醇治疗,可增加行为多巴胺受体的敏感性。

R H Belmaker, A Elami, J Bannet
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引用次数: 7

摘要

药物假期被认为是一种预防迟发性运动障碍的策略。在三项动物研究中,慢性抗精神病药物治疗后多巴胺受体超敏反应被用作迟发性运动障碍的模型,但没有发现间歇治疗与连续治疗相比,多巴胺受体超敏反应有任何减少。由于大多数神经阻滞剂在体内有很长的半衰期,我们假设在以前的研究中可能没有实现真正的无药期。超短效丁苯酮类镇定剂氟哌啶醇给药22天,每日2次或每48小时1次。在最后一次给药后60小时,阿吗啡诱导的刻板印象在连续给药和间歇给药的动物之间没有差异。因此,即使完全不吸毒也不能减少多巴胺受体超敏反应的发生。
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Intermittent treatment with droperidol, a short-acting neuroleptic, increases behavioral dopamine receptor sensitivity.

Drug holidays have been proposed as a preventive strategy against the development of tardive dyskinesia. Three animal studies in which dopamine receptor hypersensitivity after chronic neuroleptic treatment was used as a model for tardive dyskinesia failed to find any reduction in dopamine receptor hypersensitivity with intermittent, as opposed to continuous, treatment. Since most neuroleptics have a long half-life in vivo, we hypothesized that truly drug-free periods may not have been achieved in previous studies. Droperidol, an ultrashort-acting butyrophenone neuroleptic, was administered to rats for 22 days in twice-daily injections or one injection every 48 hours. At 60 hours after the last dose there was no difference in apomorphine-induced stereotypy between continuously treated and intermittently treated animals. Thus, even totally drug-free periods do not reduce the development of dopamine receptor hypersensitivity.

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Tardive dyskinesia: reversible and irreversible. Receptor-binding profiles of neuroleptics. Pathophysiological mechanisms underlying tardive dyskinesia. Chemical and structural changes in the brain in patients with movement disorder. Medical treatment of dystonia.
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