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氨磺必利对精神分裂症患者体内纹状体以外和纹状体D2多巴胺受体的阻断作用

In vivo extrastriatal and striatal D2 dopamine receptor blockade by amisulpride in schizophrenia.

作者信息

Xiberas X, Martinot J L, Mallet L, Artiges E, Canal M, Loc'h C, Mazière B, Paillère-Martinot M L

机构信息

INSERM U334, Service Hospitalier Frédéric Joliot, DSV-DRM-CEA, Orsay, France.

出版信息

J Clin Psychopharmacol. 2001 Apr;21(2):207-14. doi: 10.1097/00004714-200104000-00013.

DOI:10.1097/00004714-200104000-00013
PMID:11270918
Abstract

Amisulpride, a substituted benzamide with high affinity for dopamine D2 and D3 receptors only, has been reported to have therapeutic effects on both negative and positive schizophrenic symptoms, although at distinct dose ranges (50-300 mg/day vs. 400-1,200 mg/day). The purpose of this study was to investigate the binding of amisulpride to extrastriatal (i.e., thalamus and temporal cortex) and striatal D2 dopamine receptors with respect to plasma amisulpride determinations. Ten patients with schizophrenia treated with amisulpride over a wide range of doses (25-1,200 mg/day) were studied. Positron emission tomography images were acquired by using 76Br-FLB-457, a highly specific antagonist of the D2 and D3 dopamine receptors. Binding indexes (BI) in the regions studied were estimated with reference to values from six healthy subjects. A curvilinear relationship was demonstrated between plasma concentration of amisulpride and the BI in extrastriatal regions. The BI also varied as a function of plasma concentration in striatum. Furthermore, the data provide evidence for different binding profiles: low plasma concentrations (28-92 ng/mL) induced marked extrastriatal binding and low striatal binding, whereas higher plasma concentrations (>153 ng/mL) induced marked binding both in extrastriatal and striatal regions. Dose-dependent differential binding profiles of amisulpride to D2 receptors in extrastriatal and striatal regions were demonstrated, and two therapeutic ranges of plasma concentrations for negative and positive schizophrenic symptoms, respectively, are suggested.

摘要

氨磺必利是一种仅对多巴胺D2和D3受体具有高亲和力的取代苯甲酰胺,据报道,它对精神分裂症的阴性和阳性症状均有治疗作用,尽管作用于不同的剂量范围(50 - 300毫克/天与400 - 1200毫克/天)。本研究的目的是结合血浆氨磺必利测定,研究氨磺必利与纹状体以外区域(即丘脑和颞叶皮质)以及纹状体D2多巴胺受体的结合情况。研究了10例接受广泛剂量(25 - 1200毫克/天)氨磺必利治疗的精神分裂症患者。使用D2和D3多巴胺受体的高特异性拮抗剂76Br - FLB - 457采集正电子发射断层扫描图像。参照6名健康受试者的值估算所研究区域的结合指数(BI)。氨磺必利的血浆浓度与纹状体以外区域的BI之间呈曲线关系。BI在纹状体中也随血浆浓度而变化。此外,数据提供了不同结合模式的证据:低血浆浓度(28 - 92纳克/毫升)导致明显的纹状体以外区域结合和低纹状体结合,而较高血浆浓度(>153纳克/毫升)导致纹状体以外区域和纹状体均有明显结合。证明了氨磺必利在纹状体以外区域和纹状体中对D2受体的剂量依赖性差异结合模式,并分别提出了针对精神分裂症阴性和阳性症状的两个血浆浓度治疗范围。

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