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精神分裂症的药物治疗——过去、现在和未来。

Drug treatments for schizophrenia - past, present and future.

机构信息

Leacroft Medical Practice, Crawley, West Sussex, UK.

出版信息

Int J Psychiatry Clin Pract. 1997;1(4):227-30. doi: 10.3109/13651509709024733.

Abstract

The typical antipsychotic drugs, which have been the mainstay of treatment for schizophrenia for many years, are potent antagonists of D2 receptors. However, their lack of selectivity for D2 receptors in the mesolimbic areas compared with the nigrostriatal areas of the brain has resulted in an association at therapeutic doses with extrapyramidal side-effects, an increased risk for tardive dyskinesia and increased prolactin levels. Together with other significant side-effects, this profile has limited their acceptability for antipsychotic treatment, resulting in poor compliance, increased risk of relapse and increased severity of disease. A new generation of antipsychotics, the 'atypicals', which show greater selectivity for mesolimbic D2 receptors combined with effects on 5-HT2 receptors, have demonstrated antipsychotic efficacy, with a significantly lower incidence of extrapyramidal effects than seen with haloperidol, and often at placebo level. The first atypical antipsychotic, clozapine, has been restricted to use in treatment-resistant schizophrenia because of an association with agranwlocytosis. Two other drugs are now available, olanzapine and sertindole, and two others, quetiapine and ziprasidone, are in late-stage development. The profile of these drugs is reviewed, together with future treatment possibilities.

摘要

典型的抗精神病药物多年来一直是精神分裂症治疗的主要方法,它们是 D2 受体的有效拮抗剂。然而,与大脑黑质纹状体区域相比,它们在中脑边缘区域对 D2 受体的选择性缺乏,导致在治疗剂量下与锥体外系副作用、迟发性运动障碍风险增加和催乳素水平升高相关。加上其他显著的副作用,这一特点限制了它们作为抗精神病药物治疗的可接受性,导致依从性差、复发风险增加和疾病严重程度增加。新一代的抗精神病药物,即“非典型药物”,它们对中脑边缘 D2 受体具有更高的选择性,同时对 5-HT2 受体也有作用,已经证明了它们的抗精神病疗效,与氟哌啶醇相比,锥体外系副作用的发生率明显降低,且通常与安慰剂水平相当。第一代非典型抗精神病药物氯氮平由于与粒细胞缺乏症有关,只能用于治疗抵抗性精神分裂症。现在还有两种药物可供使用,奥氮平和齐拉西酮,另外两种药物,喹硫平和扎来普隆,正在进行后期开发。本文综述了这些药物的特点,并探讨了未来的治疗可能性。

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