Meta-analysis of continuous outcomes combining individual patient data and aggregate data

被引:197
|
作者
Riley, Richard D. [1 ]
Lambert, Paul C. [2 ]
Staessen, Jan A. [3 ]
Wang, Jiguang [4 ]
Gueyffier, Francois [5 ]
Thijs, Lutgarde [3 ]
Boutitie, Florent [6 ]
机构
[1] Univ Liverpool, Ctr Med Stat & Hlth Evaluat, Fac Med, Liverpool L69 3GS, Merseyside, England
[2] Univ Leicester, Ctr Biostat & Genet Epidemiol, Dept Hlth Sci, Leicester LE1 7RH, Leics, England
[3] Univ Leuven, Studies Coordinating Ctr, Div Hypertens & Cardiovasc Rehabil, Dept Cardiovasc Dis, B-3000 Louvain, Belgium
[4] Shanghai Jiao Tong Univ, Ctr Epidemiol Studies & Clin Trials, Ruijin Hosp, Sch Med, Shanghai 200025, Peoples R China
[5] INSERM, CIC201, F-69000 Lyon, France
[6] Lab Biostat Sante, UMR 5558, F-69495 Pierre Benite, France
关键词
meta-analysis; individual patient data; aggregate data; treatment-covariate interaction; ecological bias;
D O I
10.1002/sim.3165
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
Meta-analysis of individual patient data (IPD) is the gold-standard for synthesizing evidence across clinical studies. However, for some studies IPD may not be available and only aggregate data (AD), such as a treatment effect estimate and its standard error, may be obtained. In this situation, methods for combining IPD and AD are important to utilize all the available evidence. In this paper, we develop and assess a range of statistical methods for combining IPD and AD in meta-analysis of continuous outcomes from randomized controlled trials. The methods take either a one-step or a two-step approach. The latter is simple, with IPD reduced to AD so that standard AD meta-analysis techniques can be employed. The one-step approach is more complex but offers a flexible framework to include both patient-level and trial-level parameters. It uses a dummy variable to distinguish IPD trials from AD trials and to constrain which parameters the AD trials estimate. We show that this is important when assessing how patient-level covariates modify treatment effect, as aggregate-level relationships across trials are subject to ecological bias and confounding. We thus develop models to separate within-trial and across-trials treatment-covariate interactions; this ensures that only IPD trials estimate the former, whilst both IPD and AD trials estimate the latter in addition to the pooled treatment effect and any between-study heterogeneity. Extension to multiple correlated outcomes is also considered. Ten IPD trials in hypertension, with blood pressure the continuous outcome of interest, are used to assess the models and identify the benefits of utilizing AD alongside IPD. Copyright (c) 2007 John Wiley & Sons, Ltd.
引用
收藏
页码:1870 / 1893
页数:24
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