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精神分裂症中的异常不自主运动:它们与疾病进程还是治疗有关?它们与多巴胺受体的变化有关吗?

Abnormal involuntary movements in schizophrenia: are they related to the disease process or its treatment? Are they associated with changes in dopamine receptors?

作者信息

Crow T J, Cross A J, Johnstone E C, Owen F, Owens D G, Waddington J L

出版信息

J Clin Psychopharmacol. 1982 Oct;2(5):336-40.

PMID:7130435
Abstract

Abnormal involuntary movements indistinguishable from those now described as tardive dyskinesia were reported in schizophrenic patients by Kraepelin long before the introduction of neuroleptic drugs. Two large surveys of mental hospital patients including patients who had never received neuroleptics also revealed involuntary movements; indeed, the incidence was not substantially different from that in drug-treated patients. This fact casts doubt on the widely held assumption that these movements are persistent and irreversible effects of neuroleptic drugs. In an animal model of dyskinesia, abnormal movements were seen after administration of a phenothiazine and a thioxanthene but not after haloperidol. The syndrome appeared to be unrelated to dopamine receptor blockade or to changes in dopamine receptors. In postmortem striatal tissue from patients with schizophrenia, ligand binding to D-1 and D-2 dopamine receptors was not increased in patients who had been found to have abnormal involuntary movements in comparison with those who did not have such movements; as previously reported, binding to D-2 receptors was increased in patients with schizophrenia in comparison with controls. It is concluded that dyskinetic changes occur as a consequence of the process of schizophrenia and perhaps other diseases. Whether or not persistent and irreversible changes can be caused either in animals or humans by neuroleptic administration has yet to be clearly established. Whether they occur as a manifestation of the disease process or a consequence of drug administration, such dyskinesias are unassociated with changes in D-1 or D-2 receptors.

摘要

早在抗精神病药物问世之前,克雷佩林就报告过精神分裂症患者出现了与现在所描述的迟发性运动障碍难以区分的异常不自主运动。两项针对精神病院患者的大型调查,其中包括从未接受过抗精神病药物治疗的患者,也发现了不自主运动;事实上,其发生率与接受药物治疗的患者并无显著差异。这一事实对广泛持有的观点提出了质疑,即这些运动是抗精神病药物的持续性和不可逆性作用。在一种运动障碍的动物模型中,给予吩噻嗪和硫杂蒽后出现了异常运动,但给予氟哌啶醇后未出现。该综合征似乎与多巴胺受体阻断或多巴胺受体的变化无关。在精神分裂症患者的死后纹状体组织中,与没有异常不自主运动的患者相比,被发现有异常不自主运动的患者中,D-1和D-2多巴胺受体的配体结合并未增加;如先前报道,与对照组相比,精神分裂症患者中D-2受体的结合增加。得出的结论是,运动障碍性变化是精神分裂症以及可能其他疾病过程的结果。抗精神病药物给药是否能在动物或人类中引起持续性和不可逆的变化,尚未明确确定。无论这些运动障碍是作为疾病过程的表现还是药物给药的结果出现,它们都与D-1或D-2受体的变化无关。

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