临床试验中的适应性设计:系统综述--第一部分。

IF 3.9 3区 医学 Q1 HEALTH CARE SCIENCES & SERVICES
Mohamed Ben-Eltriki, Aisha Rafiq, Arun Paul, Devashree Prabhu, Michael O S Afolabi, Robert Baslhaw, Christine J Neilson, Michelle Driedger, Salaheddin M Mahmud, Thierry Lacaze-Masmonteil, Susan Marlin, Martin Offringa, Nancy Butcher, Anna Heath, Lauren E Kelly
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引用次数: 0

摘要

背景:适应性设计(ADs)旨在使临床试验更加灵活,提高效率并节约潜在成本。尽管文献中有大量关于不同适应性试验的统计方法,但大部分临床和研究界人士对这类设计的特点、优势和局限性仍不熟悉。本系统综述概述了 ADs 在已发表临床试验中的应用(第一部分)。后续部分(第二部分)将比较成人和儿科研究中AD在试验中的应用,为儿童健康界提供实际案例和建议:方法:在以下数据库中搜索 2010 年至 2020 年 4 月发表的研究:MEDLINE(Ovid)、Embase(Ovid)和International Pharmaceutical Abstracts(Ovid)。其中包括临床试验方案、报告以及使用 AD 进行的二次分析。为了与监管指南保持一致,我们排除了药物或疫苗以外的试验登记和干预措施。我们从已发表的文献中提取了有关研究特点、改编类型、统计分析、停止界限、后勤挑战、操作考虑因素和伦理考虑因素的数据,并在此进行了总结:在检索到的 23886 项研究中,有 317 篇关于适应性试验的出版物(其中 267 篇(84.2%)为试验报告,50 篇(15.8%)为研究方案)被纳入其中。最常见的疾病是肿瘤(168/317,53%)。大多数试验只包括成人参与者(265 项,83.9%),16 项试验(5.4%)只限于儿童,28 项试验(8.9%)既包括儿童也包括成人,8 项试验未报告纳入人群的年龄。一些研究报告称使用了一种以上的适应症(317 份临床试验报告中报告了 390 种适应症)。大多数试验处于药物开发的早期阶段(I期、II期(276/317,87%))。在纳入的试验中,采用剂量探索设计的比例最高(121/317,38.2%)。自适应随机化(53/317,16.7%),其中有29项试验(9.1%)采用了 "落选者"(或 "优胜者")设计,27项试验(8.5%)采用了无缝2-3期设计。此外,还报告了连续再评估方法(60/317,18.9%)和分组顺序设计(47/317,14.8%)。约三分之二的试验使用了频数统计方法(203/309,64%),而贝叶斯方法在24%(75/309)的纳入试验中有所报道:本综述全面报告了2010年至2020年间报告的适应性临床试验的方法学特征。适应性细节的报告并不统一,因此在解释和推广方面存在局限性。尽管如此,实施现有的适应性临床试验报告指南,并针对科学、操作挑战和伦理考虑因素制定新颖的教育策略,有助于临床试验界决定何时以及如何在临床试验中实施适应性临床试验。研究方案注册: https://doi.org/10.1186/s13063-018-2934-7 。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Adaptive designs in clinical trials: a systematic review-part I.

Background: Adaptive designs (ADs) are intended to make clinical trials more flexible, offering efficiency and potentially cost-saving benefits. Despite a large number of statistical methods in the literature on different adaptations to trials, the characteristics, advantages and limitations of such designs remain unfamiliar to large parts of the clinical and research community. This systematic review provides an overview of the use of ADs in published clinical trials (Part I). A follow-up (Part II) will compare the application of AD in trials in adult and pediatric studies, to provide real-world examples and recommendations for the child health community.

Methods: Published studies from 2010 to April 2020 were searched in the following databases: MEDLINE (Ovid), Embase (Ovid), and International Pharmaceutical Abstracts (Ovid). Clinical trial protocols, reports, and a secondary analyses using AD were included. We excluded trial registrations and interventions other than drugs or vaccines to align with regulatory guidance. Data from the published literature on study characteristics, types of adaptations, statistical analysis, stopping boundaries, logistical challenges, operational considerations and ethical considerations were extracted and summarized herein.

Results: Out of 23,886 retrieved studies, 317 publications of adaptive trials, 267 (84.2%) trial reports, and 50 (15.8%) study protocols), were included. The most frequent disease was oncology (168/317, 53%). Most trials included only adult participants (265, 83.9%),16 trials (5.4%) were limited to only children and 28 (8.9%) were for both children and adults, 8 trials did not report the ages of the included populations. Some studies reported using more than one adaptation (there were 390 reported adaptations in 317 clinical trial reports). Most trials were early in drug development (phase I, II (276/317, 87%). Dose-finding designs were used in the highest proportion of the included trials (121/317, 38.2 %). Adaptive randomization (53/317, 16.7%), with drop-the-losers (or pick-the-winner) designs specifically reported in 29 trials (9.1%) and seamless phase 2-3 design was reported in 27 trials (8.5%). Continual reassessment methods (60/317, 18.9%) and group sequential design (47/317, 14.8%) were also reported. Approximately two-thirds of trials used frequentist statistical methods (203/309, 64%), while Bayesian methods were reported in 24% (75/309) of included trials.

Conclusion: This review provides a comprehensive report of methodological features in adaptive clinical trials reported between 2010 and 2020. Adaptation details were not uniformly reported, creating limitations in interpretation and generalizability. Nevertheless, implementation of existing reporting guidelines on ADs and the development of novel educational strategies that address the scientific, operational challenges and ethical considerations can help in the clinical trial community to decide on when and how to implement ADs in clinical trials. STUDY PROTOCOL REGISTRATION: https://doi.org/10.1186/s13063-018-2934-7 .

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来源期刊
BMC Medical Research Methodology
BMC Medical Research Methodology 医学-卫生保健
CiteScore
6.50
自引率
2.50%
发文量
298
审稿时长
3-8 weeks
期刊介绍: BMC Medical Research Methodology is an open access journal publishing original peer-reviewed research articles in methodological approaches to healthcare research. Articles on the methodology of epidemiological research, clinical trials and meta-analysis/systematic review are particularly encouraged, as are empirical studies of the associations between choice of methodology and study outcomes. BMC Medical Research Methodology does not aim to publish articles describing scientific methods or techniques: these should be directed to the BMC journal covering the relevant biomedical subject area.
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