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氯氮平和去甲氯氮平的血清浓度对精神分裂症患者复发的预测作用

Serum concentrations of clozapine and norclozapine in the prediction of relapse of patients with schizophrenia.

作者信息

Xiang Ying-Qiang, Zhang Zhang-Jin, Weng Yong-Zhen, Zhai Yi-Min, Li Wen-Biao, Cai Zhuo-Ji, Tan Qing-Rong, Wang Chuan-Yue

机构信息

Laboratory of Clinical Psychopharmacology, Beijing Anding Hospital, Capital University of Medical Sciences, 5 Ankang Lane, Deshengmenwai Avenue, Xicheng District, Beijing 100088, China.

出版信息

Schizophr Res. 2006 Apr;83(2-3):201-10. doi: 10.1016/j.schres.2006.01.011. Epub 2006 Mar 9.

DOI:10.1016/j.schres.2006.01.011
PMID:16524698
Abstract

Schizophrenic outpatients (n=102) whose condition had stabilized with clozapine (CLZ) therapy and were being maintained on CLZ were followed for 1 year. Clinical status and concentrations of serum clozapine (CLZ) and its metabolite norclozapine (NCLZ) were evaluated periodically or when relapse occurred. Relapse was defined as a significant exacerbation of psychotic symptoms or hospitalization. Thirty-three patients relapsed and 69 did not. Relapse patients displayed significantly lower serum concentrations of CLZ and a sum of CLZ and NCLZ at endpoint than non-relapses (CLZ: 162 ng/ml vs. 237 ng/ml, p<0.001; CLZ+NCLZ: 225 ng/ml vs. 301 ng/ml, p<0.001). When all subjects were pooled together, a significant inverse correlation was observed between percent increase in the total score on the Brief Psychiatric Rating Scale (BPRS) from baseline and serum levels of CLZ alone (r=0.404, p<0.001) and the sum of CLZ and NCLZ (r=0.364, p<0.001). Relapses and non-relapses were well separated by a threshold CLZ serum concentration of 200 ng/ml with a sensitivity of 73% and a specificity of 80%. The threshold value represented about a 40% lower serum CLZ level than concentration achieved in acute treatment. Survival analysis showed a similarity of the relapse risk over time defined by the CLZ serum threshold and by symptomatic criteria. These results suggest that effective relapse prevention may require maintenance of patients at CLZ serum concentrations above 200 ng/ml and above 60% of the acute-phase level during long-term maintenance treatment of schizophrenia.

摘要

对102例使用氯氮平(CLZ)治疗病情已稳定且持续接受氯氮平维持治疗的精神分裂症门诊患者进行了为期1年的随访。定期或在病情复发时评估临床状态以及血清氯氮平(CLZ)及其代谢产物去甲氯氮平(NCLZ)的浓度。复发定义为精神病症状显著加重或住院治疗。33例患者复发,69例未复发。复发患者在研究终点时血清CLZ浓度以及CLZ与NCLZ浓度之和显著低于未复发患者(CLZ:162 ng/ml对237 ng/ml,p<0.001;CLZ+NCLZ:225 ng/ml对301 ng/ml,p<0.001)。当将所有受试者合并在一起时,简明精神病评定量表(BPRS)总分较基线水平的百分比增加与单独的血清CLZ水平(r=0.404,p<0.001)以及CLZ与NCLZ之和(r=0.364,p<0.001)之间存在显著的负相关。血清CLZ浓度阈值为200 ng/ml时,复发组和未复发组能得到较好区分,敏感性为73%,特异性为80%。该阈值所代表的血清CLZ水平比急性治疗时达到的浓度低约40%。生存分析表明,由CLZ血清阈值和症状标准所定义的复发风险在时间上具有相似性。这些结果表明,在精神分裂症的长期维持治疗中,有效的预防复发可能需要将患者的CLZ血清浓度维持在200 ng/ml以上以及急性期水平的60%以上。

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