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在自控风险区间设计中量化随时间变化的基线风险调整的影响。

Quantifying the impact of time-varying baseline risk adjustment in the self-controlled risk interval design.

作者信息

Li Lingling, Kulldorff Martin, Russek-Cohen Estelle, Kawai Alison Tse, Hua Wei

机构信息

Department of Population Medicine, Harvard Pilgrim Health Care Institute and Harvard Medical School, Boston, MA, USA.

Office of Biostatistics and Epidemiology, Center for Biologics Evaluation and Research, Food and Drug Administration, Silver Spring, MD, USA.

出版信息

Pharmacoepidemiol Drug Saf. 2015 Dec;24(12):1304-12. doi: 10.1002/pds.3885. Epub 2015 Oct 13.

Abstract

PURPOSE

The self-controlled risk interval design is commonly used to assess the association between an acute exposure and an adverse event of interest, implicitly adjusting for fixed, non-time-varying covariates. Explicit adjustment needs to be made for time-varying covariates, for example, age in young children. It can be performed via either a fixed or random adjustment. The random-adjustment approach can provide valid point and interval estimates but requires access to individual-level data for an unexposed baseline sample. The fixed-adjustment approach does not have this requirement and will provide a valid point estimate but may underestimate the variance. We conducted a comprehensive simulation study to evaluate their performance.

METHODS

We designed the simulation study using empirical data from the Food and Drug Administration-sponsored Mini-Sentinel Post-licensure Rapid Immunization Safety Monitoring Rotavirus Vaccines and Intussusception study in children 5-36.9 weeks of age. The time-varying confounder is age. We considered a variety of design parameters including sample size, relative risk, time-varying baseline risks, and risk interval length.

RESULTS

The random-adjustment approach has very good performance in almost all considered settings. The fixed-adjustment approach can be used as a good alternative when the number of events used to estimate the time-varying baseline risks is at least the number of events used to estimate the relative risk, which is almost always the case.

CONCLUSIONS

We successfully identified settings in which the fixed-adjustment approach can be used as a good alternative and provided guidelines on the selection and implementation of appropriate analyses for the self-controlled risk interval design.

摘要

目的

自控风险区间设计通常用于评估急性暴露与感兴趣的不良事件之间的关联,隐含地对固定的、非随时间变化的协变量进行调整。对于随时间变化的协变量,例如幼儿的年龄,则需要进行明确调整。可以通过固定调整或随机调整来进行。随机调整方法可以提供有效的点估计和区间估计,但需要获取未暴露基线样本的个体水平数据。固定调整方法则没有这一要求,并且将提供有效的点估计,但可能会低估方差。我们进行了一项全面的模拟研究以评估它们的性能。

方法

我们使用来自美国食品药品监督管理局资助的针对5 - 36.9周龄儿童的轮状病毒疫苗和肠套叠的迷你哨兵上市后快速免疫安全监测研究的经验数据来设计模拟研究。随时间变化的混杂因素是年龄。我们考虑了各种设计参数,包括样本量、相对风险、随时间变化的基线风险和风险区间长度。

结果

随机调整方法在几乎所有考虑的设置中都具有非常好的性能。当用于估计随时间变化的基线风险的事件数量至少与用于估计相对风险的事件数量相当时(几乎总是这种情况),固定调整方法可以作为一个很好的替代方法。

结论

我们成功地确定了可以将固定调整方法作为良好替代方法的设置,并为自控风险区间设计的适当分析的选择和实施提供了指导方针。

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