Le Noury Joanna, Nardo John M, Healy David, Jureidini Jon, Raven Melissa, Tufanaru Catalin, Abi-Jaoude Elia
School of Medical Sciences, Bangor University, Bangor, Wales, UK.
Emory University, Atlanta, Georgia, USA.
BMJ. 2015 Sep 16;351:h4320. doi: 10.1136/bmj.h4320.
To reanalyse SmithKline Beecham's Study 329 (published by Keller and colleagues in 2001), the primary objective of which was to compare the efficacy and safety of paroxetine and imipramine with placebo in the treatment of adolescents with unipolar major depression. The reanalysis under the restoring invisible and abandoned trials (RIAT) initiative was done to see whether access to and reanalysis of a full dataset from a randomised controlled trial would have clinically relevant implications for evidence based medicine.
Double blind randomised placebo controlled trial.
12 North American academic psychiatry centres, from 20 April 1994 to 15 February 1998.
275 adolescents with major depression of at least eight weeks in duration. Exclusion criteria included a range of comorbid psychiatric and medical disorders and suicidality.
Participants were randomised to eight weeks double blind treatment with paroxetine (20-40 mg), imipramine (200-300 mg), or placebo.
The prespecified primary efficacy variables were change from baseline to the end of the eight week acute treatment phase in total Hamilton depression scale (HAM-D) score and the proportion of responders (HAM-D score ≤8 or ≥50% reduction in baseline HAM-D) at acute endpoint. Prespecified secondary outcomes were changes from baseline to endpoint in depression items in K-SADS-L, clinical global impression, autonomous functioning checklist, self-perception profile, and sickness impact scale; predictors of response; and number of patients who relapse during the maintenance phase. Adverse experiences were to be compared primarily by using descriptive statistics. No coding dictionary was prespecified.
The efficacy of paroxetine and imipramine was not statistically or clinically significantly different from placebo for any prespecified primary or secondary efficacy outcome. HAM-D scores decreased by 10.7 (least squares mean) (95% confidence interval 9.1 to 12.3), 9.0 (7.4 to 10.5), and 9.1 (7.5 to 10.7) points, respectively, for the paroxetine, imipramine and placebo groups (P=0.20). There were clinically significant increases in harms, including suicidal ideation and behaviour and other serious adverse events in the paroxetine group and cardiovascular problems in the imipramine group.
Neither paroxetine nor high dose imipramine showed efficacy for major depression in adolescents, and there was an increase in harms with both drugs. Access to primary data from trials has important implications for both clinical practice and research, including that published conclusions about efficacy and safety should not be read as authoritative. The reanalysis of Study 329 illustrates the necessity of making primary trial data and protocols available to increase the rigour of the evidence base.
重新分析史克必成公司的329号研究(由凯勒及其同事于2001年发表),其主要目的是比较帕罗西汀、丙咪嗪与安慰剂治疗单相重度抑郁症青少年的疗效和安全性。在恢复隐形和废弃试验(RIAT)倡议下进行重新分析,以探讨获取随机对照试验的完整数据集并进行重新分析是否会对循证医学产生临床相关影响。
双盲随机安慰剂对照试验。
12个北美学术性精神病学中心,时间为1994年4月20日至1998年2月15日。
275名患有至少持续8周重度抑郁症的青少年。排除标准包括一系列共病的精神和医学疾病以及自杀倾向。
参与者被随机分配接受为期8周的双盲治疗,分别使用帕罗西汀(20 - 40毫克)、丙咪嗪(200 - 300毫克)或安慰剂。
预先设定的主要疗效变量为从基线到8周急性治疗期结束时汉密尔顿抑郁量表(HAM - D)总分的变化,以及急性终点时反应者的比例(HAM - D评分≤8或基线HAM - D评分降低≥50%)。预先设定的次要结局包括从基线到终点时在儿童及青少年情感障碍和精神分裂症问卷(K - SADS - L)中的抑郁项目、临床总体印象、自主功能检查表、自我认知概况和疾病影响量表的变化;反应的预测因素;以及维持期复发的患者数量。主要通过描述性统计比较不良经历。未预先设定编码字典。
对于任何预先设定的主要或次要疗效结局,帕罗西汀和丙咪嗪的疗效与安慰剂相比,在统计学或临床上均无显著差异。帕罗西汀、丙咪嗪和安慰剂组的HAM - D评分分别降低了10.7(最小二乘均值)(95%置信区间9.1至12.3)、9.0(7.4至10.5)和9.1(7.5至10.7)分(P = 0.20)。危害有临床显著增加,包括帕罗西汀组的自杀意念和行为以及其他严重不良事件,丙咪嗪组的心血管问题。
帕罗西汀和高剂量丙咪嗪对青少年重度抑郁症均未显示出疗效,且两种药物的危害均有所增加。获取试验的原始数据对临床实践和研究都具有重要意义,包括已发表的关于疗效和安全性的结论不应被视为权威性的。329号研究的重新分析说明了提供试验原始数据和方案以提高证据基础严谨性的必要性。
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