Are estimands being correctly used? A review of UK research protocols.

IF 2 4区医学 Q3 MEDICINE, RESEARCH & EXPERIMENTAL

Trials Pub Date : 2025-08-26 DOI:10.1186/s13063-025-08991-8

Timothy P Clark, Richard H Wicentowski, Suzie Cro, Matthew R Sydes, Brennan C Kahan

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引用次数: 0

Abstract

Background: The use of estimands in clinical trials was formalised with the adoption of the final International Conference on Harmonisation E9 Addendum on Estimands and Sensitivity Analysis in Clinical Trials (ICH E9(R1) Addendum) in November 2019. The declared objective of the ICH E9(R1) Addendum is to bring clarity and transparency to the research question of interest. For this to be achieved, the estimand must be described in accordance with the requirements of the ICH E9(R1) Addendum so that the target treatment effect is clear to all stakeholders. Previous reviews of publications and published protocols have found that few trials explicitly defined the primary estimand. To obtain a more complete picture of how the use of estimands has changed over time, whether trials are using estimands correctly (i.e. correctly defining the five attributes of an estimand), and which strategies are being used to handle intercurrent events, we obtained access to an extensive database of original research protocols (n = 29,212) submitted to the United Kingdom's Health Research Authority, which oversees ethical review of clinical trials.

Methods: Protocols were eligible for review if they included the term 'estimand' and attempted to define at least one attribute of the primary estimand. For eligible protocols, we extracted information on trial characteristics such as whether the trial was randomized and the therapeutic area, as well as whether the estimand attributes used for the primary outcome were correctly defined, and which strategies were used to handle intercurrent events.

Results: We found that the number of protocols defining a primary estimand increased starkly with publication of the ICH E9(R1) Addendum (approximately 3 protocols/year pre-ICH E9(R1) Addendum vs. 18 protocols / year during the consultation period vs. 23 protocols in the year following the adoption of the ICH E9(R1) Addendum). However, the description of the primary estimand was suboptimal; many protocols failed to mention specific attributes (such as population or treatment conditions) in the estimand description, and many protocols incorrectly defined estimand attributes (e.g. by describing the estimand population based on their analysis population).

Conclusions: Although release of the ICH E9(R1) Addendum has dramatically increased the use of estimands in clinical trials, their reporting is suboptimal. There is still work to be done to ensure estimands reach their full potential in bringing clarity and focus to research questions.

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评估是否被正确使用？英国研究方案综述。

背景：随着2019年11月通过最终的国际协调会议E9临床试验估计和敏感性分析附录（ICH E9（R1）附录），临床试验中估计的使用正式确定。ICH E9（R1）增编声明的目标是为感兴趣的研究问题带来清晰度和透明度。为了实现这一点，评估必须按照ICH E9（R1）附录的要求进行描述，以便所有利益相关者都能清楚地看到目标处理效果。先前对出版物和已发表的方案的回顾发现，很少有试验明确定义了主要估计。为了更全面地了解估计的使用是如何随着时间的推移而变化的，试验是否正确地使用了估计（即正确定义了估计的五个属性），以及正在使用哪些策略来处理并发事件，我们获得了提交给英国卫生研究管理局的原始研究方案的广泛数据库（n = 29,212），该机构负责监督临床试验的伦理审查。方法：如果方案包含术语“估计”并试图定义至少一个主要估计的属性，那么方案就有资格进行审查。对于符合条件的方案，我们提取了有关试验特征的信息，如试验是否随机化和治疗区域，以及用于主要结局的估计属性是否被正确定义，以及使用哪些策略来处理并发事件。结果：我们发现，随着ICH E9（R1）附录的发布，定义主要评估的协议数量明显增加（ICH E9（R1）附录发布前约3个协议/年，而咨询期间约18个协议/年，而采用ICH E9（R1）附录后一年为23个协议）。然而，原始估计的描述是次优的；许多方案没有在估计描述中提到特定的属性（如总体或治疗条件），并且许多方案错误地定义了估计属性（例如，通过基于其分析总体来描述估计总体）。结论：尽管ICH E9（R1）附录的发布大大增加了临床试验中评估的使用，但其报告并不理想。仍有工作要做，以确保估算充分发挥其潜力，为研究问题带来清晰度和重点。

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

Trials 医学-医学：研究与实验

CiteScore

3.80

自引率

4.00%

发文量

966

审稿时长

6 months

期刊介绍： Trials is an open access, peer-reviewed, online journal that will encompass all aspects of the performance and findings of randomized controlled trials. Trials will experiment with, and then refine, innovative approaches to improving communication about trials. We are keen to move beyond publishing traditional trial results articles (although these will be included). We believe this represents an exciting opportunity to advance the science and reporting of trials. Prior to 2006, Trials was published as Current Controlled Trials in Cardiovascular Medicine (CCTCVM). All published CCTCVM articles are available via the Trials website and citations to CCTCVM article URLs will continue to be supported.