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Future Cases as Present Controls to Adjust for Exposure Trend Bias in Case-only Studies
Author(s) -
Shirley Wang,
Crystal D. Linkletter,
Malcolm Maclure,
David D. Dore,
Vincent Mor,
Stephen L. Buka,
Gregory A. Wellenius
Publication year - 2011
Publication title -
epidemiology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.901
H-Index - 173
eISSN - 1531-5487
pISSN - 1044-3983
DOI - 10.1097/ede.0b013e31821d09cd
Subject(s) - odds ratio , confounding , crossover study , confidence interval , pharmacoepidemiology , crossover , case control study , medicine , odds , statistics , computer science , mathematics , logistic regression , alternative medicine , pathology , artificial intelligence , medical prescription , pharmacology , placebo
Self-matched case-only studies (such as the case-crossover or self-controlled case-series method) control by design for time-invariant confounders (measured or unmeasured), but they do not control for confounders that vary with time. A bidirectional case-crossover design can be used to adjust for exposure-time trends. In pharmacoepidemiology, however, illness often influences future use of medications, making a bidirectional design problematic. Suissa's case-time-control design combines a case-crossover and case-control design, and adjusts for exposure-trend bias in the cases' self-controlled odds ratio by dividing that ratio by the corresponding self-controlled odds ratio in a concurrent matched control group. However, if not well matched, the control group may reintroduce selection bias. We propose a "case-case-time-control" that involves crossover analyses in cases and future-case controls. This person-time sampling strategy improves matching by restricting controls to future cases. We evaluate the proposed study design through simulations and analysis of a theoretically null relationship using Veterans Administration (VA) data. Simulation studies show that the case-case-time-control can adjust for exposure trends while controlling for time-invariant confounders. Use of an inappropriate control group left case-time-control analyses biased by exposure-time trends. When analyzing the relationship between vitamin exposure and stroke, using data on 3192 patients in the VA system, a case-crossover odds ratio of 1.5 (95% confidence interval = 1.3-1.7) was reduced to 1.1 (0.9-1.3) when divided by the concurrent exposure trend odds ratio (1.4) in matched future cases. This applied example demonstrates how our approach can adjust for exposure trends observed across time axes.

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