Selective publication of antidepressant trials and its influence on apparent efficacy: Updated comparisons and meta-analyses of newer versus older trials.

IF 10.5 1区医学 Q1 MEDICINE, GENERAL & INTERNAL

PLoS Medicine Pub Date : 2022-01-19 eCollection Date: 2022-01-01 DOI:10.1371/journal.pmed.1003886

Erick H Turner, Andrea Cipriani, Toshi A Furukawa, Georgia Salanti, Ymkje Anna de Vries

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引用次数: 23

Abstract

Background: Valid assessment of drug efficacy and safety requires an evidence base free of reporting bias. Using trial reports in Food and Drug Administration (FDA) drug approval packages as a gold standard, we previously found that the published literature inflated the apparent efficacy of antidepressant drugs. The objective of the current study was to determine whether this has improved with recently approved drugs.

Methods and findings: Using medical and statistical reviews in FDA drug approval packages, we identified 30 Phase II/III double-blind placebo-controlled acute monotherapy trials, involving 13,747 patients, of desvenlafaxine, vilazodone, levomilnacipran, and vortioxetine; we then identified corresponding published reports. We compared the data from this newer cohort of antidepressants (approved February 2008 to September 2013) with the previously published dataset on 74 trials of 12 older antidepressants (approved December 1987 to August 2002). Using logistic regression, we examined the effects of trial outcome and trial cohort (newer versus older) on transparent reporting (whether published and FDA conclusions agreed). Among newer antidepressants, transparent publication occurred more with positive (15/15 = 100%) than negative (7/15 = 47%) trials (OR 35.1, CI95% 1.8 to 693). Controlling for trial outcome, transparent publication occurred more with newer than older trials (OR 6.6, CI95% 1.6 to 26.4). Within negative trials, transparent reporting increased from 11% to 47%. We also conducted and contrasted FDA- and journal-based meta-analyses. For newer antidepressants, FDA-based effect size (ESFDA) was 0.24 (CI95% 0.18 to 0.30), while journal-based effect size (ESJournals) was 0.29 (CI95% 0.23 to 0.36). Thus, effect size inflation, presumably due to reporting bias, was 0.05, less than for older antidepressants (0.10). Limitations of this study include a small number of trials and drugs-belonging to a single class-and a focus on efficacy (versus safety).

Conclusions: Reporting bias persists but appears to have diminished for newer, compared to older, antidepressants. Continued efforts are needed to further improve transparency in the scientific literature.

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选择性发表抗抑郁药试验及其对表观疗效的影响:更新的比较和新试验与旧试验的荟萃分析。

背景:有效的药物疗效和安全性评估需要无报告偏倚的证据基础。使用美国食品和药物管理局(FDA)药物批准包中的试验报告作为金标准，我们先前发现已发表的文献夸大了抗抑郁药物的明显疗效。当前研究的目的是确定最近批准的药物是否改善了这种情况。方法和研究结果:通过FDA药物批准包中的医学和统计回顾，我们确定了30项II/III期双盲安慰剂对照急性单药治疗试验，涉及13,747例患者，使用地文拉法辛、维拉唑酮、左旋美拉西普兰和沃替西汀;然后，我们确定了相应的已发表报告。我们将这一新的抗抑郁药队列(2008年2月至2013年9月批准)的数据与之前发表的12种较早的抗抑郁药74项试验的数据集(1987年12月至2002年8月批准)进行了比较。使用逻辑回归，我们检查了试验结果和试验队列(较新与较老)对透明报告(是否已发表和FDA结论是否同意)的影响。在较新的抗抑郁药中，阳性试验(15/15 = 100%)比阴性试验(7/15 = 47%)(OR为35.1,CI95%为1.8至693)更容易公开发表。在控制试验结果的情况下，新试验的公开发表比老试验更多(OR 6.6, CI95% 1.6 - 26.4)。在负面试验中，透明报告从11%增加到47%。我们还进行了基于FDA和期刊的meta分析，并进行了对比。对于较新的抗抑郁药，基于fda的效应量(ESFDA)为0.24 (CI95% 0.18至0.30)，而基于期刊的效应量(ESJournals)为0.29 (CI95% 0.23至0.36)。因此，效应大小膨胀(可能是由于报告偏倚)为0.05，低于较老的抗抑郁药(0.10)。这项研究的局限性包括试验和药物数量较少，属于单一类别，并且关注疗效(与安全性相比)。结论:报告偏倚仍然存在，但与较旧的抗抑郁药相比，新抗抑郁药的报告偏倚似乎有所减少。需要继续努力进一步提高科学文献的透明度。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

PLoS Medicine 医学-医学：内科

CiteScore

21.60

自引率

0.60%

发文量

227

审稿时长

3 months

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