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Dropout Rates in Randomized Clinical Trials of Antipsychotics: A Meta-analysis Comparing First- and Second-Generation Drugs and an Examination of the Role of Trial Design Features

机译:抗精神病药的随机临床试验中的辍学率:比较第一代和第二代药物的Meta分析和试验设计功能的作用的检查。

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Dropout is often used as an outcome measure in clinical trials of antipsychotic medication. Previous research is inconclusive regarding (a) differences in dropout rates between first- and second-generation antipsychotic medications and (b) how trial design features reduce dropout. Meta-analysis of randomized controlled trials (RCTs) of antipsychotic medication was conducted to compare dropout rates for first- and second-generation antipsychotic drugs and to examine how a broad range of design features effect dropout. Ninety-three RCTs that met inclusion criteria were located (n = 26 686). Meta-analytic random effects models showed that dropout was higher for first- than second-generation drugs (odds ratio = 1.49, 95% confidence interval: 1.31–1.66). This advantage persisted after removing study arms with excessively high dosages, in flexible dose studies, studies of patients with symptom exacerbation, nonresponder patients, inpatients, and outpatients. Mixed effects models for meta-analysis were used to identify design features that effected dropout and develop formulae to derive expected dropout rates based on trial design features, and these assigned a pivotal role to duration. Collectively, dropout rates are lower for second- than first-generation antipsychotic drugs and appear to be partly explained by trial design features thus providing direction for future trial design.
机译:在抗精神病药物的临床试验中,辍学经常被用作结果指标。关于(a)第一代和第二代抗精神病药物之间的辍学率差异以及(b)试验设计功能如何减少辍学的研究尚无定论。进行了抗精神病药物随机对照试验(RCT)的荟萃分析,以比较第一代和第二代抗精神病药物的辍学率,并研究各种设计特征如何影响辍学。找到了符合入选标准的93个RCT(n = 26686)。荟萃分析随机效应模型显示,第一代药物的辍学率高于第二代药物(赔率= 1.49,95%置信区间:1.31-1.66)。在灵活剂量研究,症状加重患者,无反应患者,住院患者和门诊患者的研究中,以高剂量移走研究组后,这种优势仍然存在。用于荟萃分析的混合效应模型用于确定影响辍学的设计特征,并根据试验设计特征开发公式以得出预期的辍学率,这些对持续时间具有关键作用。总的来说,第二代抗精神病药物的辍学率较低,并且似乎部分由试验设计特征解释,从而为将来的试验设计提供了方向。

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