Pfizer Inc., New York, NY, USA.
Cleveland Clinic, Cleveland, OH, USA.
Clin Trials. 2020 Oct;17(5):535-544. doi: 10.1177/1740774520934747. Epub 2020 Jul 9.
The ICH E9(R1) addendum states that the strategy to account for intercurrent events should be included when defining an estimand, the treatment effect to be estimated based on the study objective. The estimator used to assess the treatment effect needs to be aligned with the estimand that accounted for intercurrent events. Regardless of the strategy, missing data resulting from patient premature withdrawal could undermine the robustness of the study results. Informative censoring due to dropouts in an events-based study is one such example. Sensitivity analyses using imputation methods are useful to examine the uncertainty due to informative censoring and address the robustness and strength of the study results.
We assessed the effect of premature patient withdrawal in the PRECISION study, a randomized non-inferiority clinical trial of patients with chronic arthritic pain that compared the cardiovascular safety of three nonsteroidal anti-inflammatory drugs-based treatment policies or paradigms. The protocol-defined use of concomitant or rescue medications was permitted since changes in pain medications due to insufficient analgesia were expected in patients in this long-term study. Anticipating that premature study discontinuations could potentially lead to informative censoring, a supplementary analysis was pre-specified in which censored outcomes due to the premature study discontinuation were imputed based on adverse events that were clinically associated with the primary endpoint (cardiovascular outcome based on the Antiplatelet Trialists Collaboration composite endpoint). Furthermore, tipping point analyses were conducted to test the robustness of the primary analysis results by assuming data censored not at random. The level of increase at which the primary study conclusion would change was estimated.
For the analysis of time to first primary endpoint event through 30 months, 4065 out of the 24,081 enrolled patients were lost to follow-up, withdrew consent, or were no longer willing to participate in the study. These withdrawals occurred gradually and resulted in a cumulative total of 5893 censored patient-years of observation (10.2%). The rate of discontinuation and the baseline characteristics of the discontinued patients were similar across the three treatment groups. The non-inferiority conclusion from the primary analysis was confirmed in the supplementary analysis incorporating relevant adverse events. Furthermore, tipping point analyses demonstrated that in order to lose non-inferiority in the primary analysis, the risk of primary endpoint events during the censored observation time would have to increase by more than 2.7-fold in the celecoxib group while remaining constant in the other nonsteroidal anti-inflammatory drugs groups, demonstrating that the scenarios where the study results are invalid appear not plausible.
Supplementary and sensitivity analyses presented to address informative censoring in PRECISION helped to further interpret and strengthen the study results.
ICH E9(R1)附录指出,在定义估计量时应纳入对并发事件的处理策略,该估计量是基于研究目的来估计的治疗效果。用于评估治疗效果的估计器需要与考虑并发事件的估计量保持一致。无论采用何种策略,由于患者过早退出而导致的数据缺失都可能破坏研究结果的稳健性。基于事件的研究中因脱落而导致的信息性删失就是一个这样的例子。使用插补方法进行敏感性分析有助于检查信息性删失引起的不确定性,并解决研究结果的稳健性和强度。
我们评估了 PRECISION 研究中患者过早退出的影响,这是一项比较三种非甾体抗炎药治疗方案或模式的慢性关节炎疼痛患者心血管安全性的随机非劣效性临床试验。由于预计在这项长期研究中,由于镇痛不足而改变疼痛药物的情况,因此允许使用方案定义的伴随或解救药物。预计提前停止研究可能会导致信息性删失,因此预先指定了一项补充分析,根据与主要终点(基于抗血小板试验者协作综合终点的心血管结局)临床相关的不良事件,对因提前停止研究而导致的删失结局进行插补。此外,还进行了转折点分析,通过假设数据不是随机删失来检验主要分析结果的稳健性。估计了主要研究结论发生变化的增量水平。
在分析到 30 个月的首次主要终点事件时间时,在 24081 名入组患者中,有 4065 名患者失访、撤回同意或不再愿意参与研究。这些退出是逐渐发生的,导致观察的累计删失患者人数为 5893 人年(10.2%)。在三个治疗组中,退出率和退出患者的基线特征相似。在纳入相关不良事件的补充分析中,确认了主要分析的非劣效性结论。此外,转折点分析表明,为了在主要分析中失去非劣效性,在其他非甾体抗炎药组中保持不变的情况下,塞来昔布组在删失观察期间的主要终点事件风险必须增加两倍以上,这表明研究结果无效的情况似乎不太可能出现。
为解决 PRECISION 中的信息性删失问题而呈现的补充和敏感性分析有助于进一步解释和加强研究结果。
