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精神分裂症患者的氯丙嗪剂量。

Chlorpromazine dose for people with schizophrenia.

作者信息

Liu Xiaomeng, De Haan Saskia

机构信息

Utrecht University, Postbus 85500, Utrecht, Netherlands, 3508 GA.

出版信息

Cochrane Database Syst Rev. 2009 Apr 15(2):CD007778. doi: 10.1002/14651858.CD007778.

DOI:10.1002/14651858.CD007778
PMID:19370692
Abstract

BACKGROUND

Chlorpromazine is one of the three antipsychotic drugs on the WHO Essential Drug List. It is used worldwide. The optimal dose has been the subject of evaluative research but summaries of this work are rare.

OBJECTIVES

To determine chlorpromazine dose response and dose adverse effect relationships for schizophrenia and schizophrenia-like psychoses.

SEARCH STRATEGY

We searched the Cochrane Schizophrenia Group Trials Register (December 2008). References of all included studies were examined for further trials.

SELECTION CRITERIA

All relevant randomised controlled trials (RCTs) comparing fixed doses of chlorpromazine for people with schizophrenia and reporting clinical outcomes.

DATA COLLECTION AND ANALYSIS

We extracted data independently. For dichotomous data we calculated fixed-effect relative risk (RR) and their 95% confidence intervals (CI). For continuous data, we calculated weighted mean differences (WMD) based on a fixed-effect model.

MAIN RESULTS

We included four relevant studies (1012 participants) in this review. They are all hospital-based trials, have a duration of less than six months and are at moderate risk of bias. When low dose (</=400mg/day) was compared with medium dose (401-800 mg/day) mental state data were very few and difficult to interpret (n=22, 1 RCT, WMD 'withdrawal retardation' -2.00 CI -3.76 to -0.24). More people left for inefficacy of treatment in the low dose group (n=48, 1 RCT, RR 4.24 CI 0.24 to 74.01). In the short term, all measured extrapyramidal adverse effects tended to be lower in the low dose group (n=70, 2 RCTs, RR dystonia 0.20 CI 0.04 to 0.97). When low dose was compared with high (>800mg/day) data were taken from only one study (2gms chlorpromazine/day). Global state outcomes tended to favour the high dose group (n=416, 1 RCT, RR 'No clinically important improvement 1.12 CI 1.01 to 1.23). One case of death was reported in the high dose group (n=416, RR 0.33 CI 0.01 to 8.14) and a significantly greater number of people in the high dose group left early due to disabling adverse effects (n=416, RR 0.10 CI 0.04 to 0.27). Significantly less dystonia and unspecified extrapyramidal adverse effects were reported in the low dose group (n=416, dystonia RR 0.11 CI 0.02 to 0.45, unspecified extrapyramidal adverse effects RR 0.43 CI 0.32 to 0.59). People in both groups experienced akathisia (n=416, RR1.00 CI 0.55 to 1.83).

AUTHORS' CONCLUSIONS: The average dose of chlorpromazine given to people with schizophrenia has declined across time, but this has come about by long - and sometimes hard - experience rather than from direction from high-grade trial-based evidence. This progression towards gentler levels of dosing has taken six decades. We hope that, for modern compounds, data from relevant high-grade evaluative studies will be much more swiftly available to guide informed practice.

摘要

背景

氯丙嗪是世界卫生组织基本药物清单上的三种抗精神病药物之一。它在全球范围内使用。最佳剂量一直是评估研究的主题,但此类研究的综述很少见。

目的

确定氯丙嗪对精神分裂症和精神分裂症样精神病的剂量反应及剂量与不良反应的关系。

检索策略

我们检索了Cochrane精神分裂症研究组试验注册库(2008年12月)。对所有纳入研究的参考文献进行检查以查找更多试验。

选择标准

所有比较固定剂量氯丙嗪治疗精神分裂症患者并报告临床结局的相关随机对照试验(RCT)。

数据收集与分析

我们独立提取数据。对于二分数据,我们计算固定效应相对危险度(RR)及其95%置信区间(CI)。对于连续数据,我们基于固定效应模型计算加权均数差(WMD)。

主要结果

本综述纳入了四项相关研究(1012名参与者)。它们均为基于医院的试验,持续时间少于六个月,且存在中度偏倚风险。当将低剂量(≤400mg/天)与中等剂量(401 - 800mg/天)进行比较时,精神状态数据非常少且难以解释(n = 22,1项RCT,WMD“撤药延迟” -2.00,CI -3.76至 -0.24)。低剂量组因治疗无效而退出的人数更多(n = 48,1项RCT,RR 4.24,CI 0.24至74.01)。短期内,低剂量组所有测量的锥体外系不良反应往往较低(n = 70,2项RCT,肌张力障碍RR 0.20,CI 0.04至0.97)。当将低剂量与高剂量(>800mg/天)进行比较时,数据仅来自一项研究(氯丙嗪2g/天)。总体状态结局倾向于支持高剂量组(n = 416,1项RCT,RR“无临床重要改善”1.12,CI 1.01至1.23)。高剂量组报告了1例死亡(n = 416,RR 0.33,CI 0.01至8.14),且高剂量组因致残性不良反应而提前退出的人数明显更多(n = 416,RR 0.10,CI 0.04至0.27)。低剂量组报告的肌张力障碍和未指定的锥体外系不良反应明显较少(n = 416,肌张力障碍RR 0.11,CI 0.02至0.45,未指定的锥体外系不良反应RR 0.43,CI 0.32至0.59)。两组患者均出现静坐不能(n = 416,RR1.00,CI 0.55至1.83)。

作者结论

随着时间推移,给予精神分裂症患者的氯丙嗪平均剂量有所下降,但这是通过长期且有时艰难的经验积累实现的,而非基于高级别试验证据的指导。这种向更温和剂量水平的进展历时六十年。我们希望,对于现代化合物,相关高级别评估研究的数据能更快可得,以指导明智的临床实践。

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