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抗精神病药物的不良主观体验及其与纹状体和纹状体外D2受体的关系:一项针对精神分裂症的正电子发射断层扫描研究

Adverse subjective experience with antipsychotics and its relationship to striatal and extrastriatal D2 receptors: a PET study in schizophrenia.

作者信息

Mizrahi Romina, Rusjan Pablo, Agid Ofer, Graff Ariel, Mamo David C, Zipursky Robert B, Kapur Shitij

机构信息

Centre for Addiction and Mental Health, Toronto, Ontario, Canada M5S 2S1.

出版信息

Am J Psychiatry. 2007 Apr;164(4):630-7. doi: 10.1176/ajp.2007.164.4.630.

Abstract

OBJECTIVES

Antipsychotic medications improve psychosis but often induce a state of dysphoria in patients. Blockade of the dopamine D(2) receptors, which is thought to mediate their efficacy, has also been implicated in producing this adverse subjective experience. The authors present the first double-blind controlled study to examine the relationship between striatal and extrastriatal dopamine D(2) receptor binding potential and occupancy values and adverse subjective experience.

METHOD

Patients with recent-onset psychosis (N=12) were randomly assigned to low or high doses of olanzapine or risperidone. Subjective experiences, motor side effects, and striatal and extrastriatal dopamine D(2) receptors (determined with [(11)C]raclopride and [(11)C]FLB 457 PET scans, respectively) were evaluated after 2 weeks of continuous antipsychotic treatment.

RESULTS

Higher dopamine D(2) receptor occupancy and binding potentials in the striatal (dorsal and ventral), temporal, and insular regions were associated with subjective experience. The finding was confirmed with two convergent methods of analysis (region-of-interest and voxel-based statistics), and the same relationship was observed using two different dopamine receptor measures (observed binding potential values and age- and sex-corrected occupancy values).

CONCLUSIONS

Higher D(2) receptor occupancy is associated with negative subjective experience in patients taking risperidone or olanzapine. These negative subjective effects may be related to the high discontinuation rates seen in usual practice. Understanding the neurobiological mechanism of these negative subjective experiences and developing antipsychotics with novel (i.e., non D(2)) mechanisms may be critical in improving the treatment of psychosis.

摘要

目的

抗精神病药物可改善精神病症状,但常使患者产生烦躁不安的状态。多巴胺D(2)受体的阻断被认为介导了其疗效,同时也与这种不良主观体验的产生有关。作者开展了第一项双盲对照研究,以检验纹状体和纹状体以外区域多巴胺D(2)受体结合潜能及占有率值与不良主观体验之间的关系。

方法

近期发病的精神病患者(N = 12)被随机分配至低剂量或高剂量奥氮平或利培酮组。在连续进行2周抗精神病药物治疗后,评估主观体验、运动副作用以及纹状体和纹状体以外区域的多巴胺D(2)受体(分别通过[11C]雷氯必利和[11C]FLB 457正电子发射断层扫描确定)。

结果

纹状体(背侧和腹侧)、颞叶和岛叶区域较高的多巴胺D(2)受体占有率和结合潜能与主观体验相关。这一发现通过两种相互验证的分析方法(感兴趣区分析和基于体素的统计学分析)得到证实,并且使用两种不同的多巴胺受体测量方法(观察到的结合潜能值以及经年龄和性别校正的占有率值)观察到了相同的关系。

结论

服用利培酮或奥氮平的患者中,较高的D(2)受体占有率与负面主观体验相关。这些负面主观效应可能与实际临床中较高的停药率有关。了解这些负面主观体验的神经生物学机制并研发具有新型(即非D(2))作用机制的抗精神病药物,对于改善精神病治疗可能至关重要。

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