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氯氮平治疗患者中D2多巴胺受体占有率的个体差异。

Individual variation in D2 dopamine receptor occupancy in clozapine-treated patients.

作者信息

Pickar D, Su T P, Weinberger D R, Coppola R, Malhotra A K, Knable M B, Lee K S, Gorey J, Bartko J J, Breier A, Hsiao J

机构信息

Experimental Therapeutics Branch, NIMH, Bethesda, MD 20892-1380, USA.

出版信息

Am J Psychiatry. 1996 Dec;153(12):1571-8. doi: 10.1176/ajp.153.12.1571.

DOI:10.1176/ajp.153.12.1571
PMID:8942453
Abstract

OBJECTIVE

The objectives of this study were 1) to pursue the question of clozapine's striatal D2 occupancy in relation to its clinical effectiveness; 2) to investigate the relation between schizophrenic symptoms, clozapine blood levels, and estimated D2 occupancy during clinically stable and unstable conditions; and 3) to examine long-term stability in D2 occupancy.

METHOD

Specific binding of the D2 radioligand [123I]benzamide ([123I]IBZM) was studied with single photon emission computed tomography in 13 patients with schizophrenia when they were clinically stable during chronic clozapine treatment, after clozapine dose reduction of > or = 50%, and in a subgroup (N = 7) after restabilization on clozapine regimens. Clozapine's estimated D2 occupancy was based on comparison with values from drug-free normal subjects.

RESULTS

A wide range of estimated D2 occupancies (18% to > or = 80%) were associated with sustained, favorable response to clozapine without correlation with residual symptoms. Clozapine blood levels were negatively related to [123I]IBZM specific binding. Acute dose reduction was associated with predicted worsening in positive and negative symptoms and increases in [123I]IBZM specific binding. Independent of clozapine blood level, patients with more symptoms showed lower [123I]IBZM specific binding, consistent with competition of endogenous dopamine for D2 binding sites in patients with greater symptoms. Restabilization on clozapine regimens produced D2 occupancies closely correlated with baseline values.

CONCLUSIONS

There was no evidence for a critical degree of D2 occupancy required to sustain clozapine's therapeutic effects across subjects. Simple linear regression was the best-fit model for clozapine's D2 occupancy. Longitudinal follow-up suggests stability over time of D2 occupancy in relation to dose and clinical response within individual patients.

摘要

目的

本研究的目的是:1)探讨氯氮平纹状体D2占有率与其临床疗效之间的关系;2)研究在临床稳定和不稳定状态下,精神分裂症症状、氯氮平血药浓度及估计的D2占有率之间的关系;3)检测D2占有率的长期稳定性。

方法

采用单光子发射计算机断层扫描技术,研究13例精神分裂症患者在氯氮平长期治疗临床稳定期、氯氮平剂量降低≥50%后以及在氯氮平治疗方案重新稳定后的亚组(N = 7)中D2放射性配体[123I]苯甲酰胺([123I]IBZM)的特异性结合情况。氯氮平的估计D2占有率是通过与未用药正常受试者的值进行比较得出的。

结果

氯氮平的估计D2占有率范围很广(18%至≥80%),与对氯氮平的持续良好反应相关,与残留症状无关。氯氮平血药浓度与[123I]IBZM特异性结合呈负相关。急性剂量降低与阳性和阴性症状的预期恶化以及[123I]IBZM特异性结合增加有关。与氯氮平血药浓度无关,症状较多的患者[123I]IBZM特异性结合较低,这与症状较重患者内源性多巴胺对D2结合位点的竞争一致。氯氮平治疗方案重新稳定后产生的D2占有率与基线值密切相关。

结论

没有证据表明在所有受试者中维持氯氮平治疗效果需要临界程度的D2占有率。简单线性回归是氯氮平D2占有率的最佳拟合模型。纵向随访表明,个体患者中D2占有率相对于剂量和临床反应随时间具有稳定性。

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