Reasons for disparity in statin adherence rates between clinical trials and real-world observations: a review
Vonbank, Alexander; Drexel, Heinz; Agewall, Stefan; Lewis, Basil S.; Dopheide, Joern F.; Kjeldsen, Keld; Ceconi, Claudio; Savarese, Gianluigi; Rosano, Giuseppe; Wassmann, Sven; Niessner, Alexander; Schmidt, Thomas Andersen; Saely, Christoph H.; Baumgartner
EUROPEAN HEART JOURNAL-CARDIOVASCULAR PHARMACOTHERAPY
2018
VL / 4 - BP / 230 - EP / 236
abstract
With statins, the reported rate of adverse events differs widely between randomized clinical trials (RCTs) and observations in clinical practice, the rates being 1-2% in RCTs vs. 10-20% in the so-called real world. One possible explanation is the claim that RCTs mostly use a run-in period with a statin. This would exclude intolerant patients from remaining in the trial and therefore favour a bias towards lower rates of intolerance. We here review data from RCTs with more than 1000 participants with and without a run-in period, which were included in the Cholesterol Treatment Trialists Collaboration. Two major conclusions arise: (i) the majority of RCTs did not have a test dose of a statin in the run-in phase. (ii) A test dose in the run-in phase was not associated with a significantly improved adherence rate within that trial when compared to trials without a test dose. Taken together, the RCTs of statins reviewed here do not suggest a bias towards an artificially higher adherence rate because of a run-in period with a test dose of the statin. Other possible explanations for the apparent disparity between RCTs and real-world observations are also included in this review albeit mostly not supported by scientific data.
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