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Allowing for non-adherence to treatment in a randomized controlled trial of two antidepressants (citalopram versus reboxetine): an example from the GENPOD trial.

机译:在两种抗抑郁药(西酞普兰与瑞波西汀)的随机对照试验中允许不坚持治疗:来自GENPOD试验的一个例子。

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摘要

BACKGROUND: Meta-analyses suggest that reboxetine may be less effective than other antidepressants. Such comparisons may be biased by lower adherence to reboxetine and subsequent handling of missing outcome data. This study illustrates how to adjust for differential non-adherence and hence derive an unbiased estimate of the efficacy of reboxetine compared with citalopram in primary care patients with depression. METHOD: A structural mean modelling (SMM) approach was used to generate adherence-adjusted estimates of the efficacy of reboxetine compared with citalopram using GENetic and clinical Predictors Of treatment response in Depression (GENPOD) trial data. Intention-to-treat (ITT) analyses were performed to compare estimates of effectiveness with results from previous meta-analyses. RESULTS: At 6 weeks, 92% of those randomized to citalopram were still taking their medication, compared with 72% of those randomized to reboxetine. In ITT analysis, there was only weak evidence that those on reboxetine had a slightly worse outcome than those on citalopram [adjusted difference in mean Beck Depression Inventory (BDI) scores: 1.19, 95% confidence interval (CI) -0.52 to 2.90, p = 0.17]. There was no evidence of a difference in efficacy when differential non-adherence was accounted for using the SMM approach for mean BDI (-0.29, 95% CI -3.04 to 2.46, p = 0.84) or the other mental health outcomes. CONCLUSIONS: There was no evidence of a difference in the efficacy of reboxetine and citalopram when these drugs are taken and tolerated by depressed patients. The SMM approach can be implemented in standard statistical software to adjust for differential non-adherence and generate unbiased estimates of treatment efficacy for comparisons of two (or more) active interventions.
机译:背景:荟萃分析表明瑞波西汀可能不如其他抗抑郁药有效。此类比较可能因对瑞波西汀的依从性较低以及后续缺少结果数据的处理而产生偏差。这项研究说明了如何针对差异性非依从性进行调整,从而得出在抑郁症初级保健患者中瑞波西汀与西酞普兰相比疗效的无偏估计。方法:使用结构平均模型(SMM)方法,使用基因治疗和临床抑郁症预测指标(GENPOD)的试验数据,对依波普汀与西酞普兰的疗效进行依托调整后的估计值。进行意向性治疗(ITT)分析,以比较有效性评估与先前荟萃分析的结果。结果:在第6周时,随机分配给西酞普兰的患者中92%仍在服药,而随机分配给瑞波西汀的患者中有72%。在ITT分析中,仅有微弱的证据表明瑞波西汀组比西酞普兰组的结局稍差[校正后的平均贝克抑郁量表(BDI)评分差异:1.19,95%置信区间(CI)-0.52至2.90,p = 0.17]。当使用SMM方法计算平均BDI(-0.29,95%CI -3.04至2.46,p = 0.84)或其他精神健康结果时,没有证据表明疗效差异。结论:当抑郁症患者服用和耐受这些药物时,没有证据表明瑞波西汀和西酞普兰的疗效存在差异。可以在标准统计软件中实施SMM方法,以针对差异性非依从性进行调整并生成治疗效果的无偏估计,以比较两个(或多个)有效干预措施。

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