A comprehensive assessment of statin discontinuation among patients who concurrently initiate statins and CYP3A4-inhibitor drugs; a multistate transition model

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Donneyong2023Comprehensive-CCBYNCND.pdf (1.24 MB)
Date
2023
Authors
Donneyong, Macarius M.
Zhu, Yuxi
Zhang, Pengyue
Li, Yiting
Hunold, Katherine M.
Chiang, ChienWei
Unroe, Kathleen
Caterino, Jeffrey M.
Li, Lang
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American English
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Medicine, School of Medicine
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Wiley
Abstract

Aims: The aim of this study was to describe the 1-year direct and indirect transition probabilities to premature discontinuation of statin therapy after concurrently initiating statins and CYP3A4-inhibitor drugs.

Methods: A retrospective new-user cohort study design was used to identify (N = 160 828) patients who concurrently initiated CYP3A4 inhibitors (diltiazem, ketoconazole, clarithromycin, others) and CYP3A4-metabolized statins (statin DDI exposed, n = 104 774) vs. other statins (unexposed to statin DDI, n = 56 054) from the MarketScan commercial claims database (2012-2017). The statin DDI exposed and unexposed groups were matched (2:1) through propensity score matching techniques. We applied a multistate transition model to compare the 1-year transition probabilities involving four distinct states (start, adverse drug events [ADEs], discontinuation of CYP3A4-inhibitor drugs, and discontinuation of statin therapy) between those exposed to statin DDIs vs. those unexposed. Statistically significant differences were assessed by comparing the 95% confidence intervals (CIs) of probabilities.

Results: After concurrently starting stains and CYP3A, patients exposed to statin DDIs, vs. unexposed, were significantly less likely to discontinue statin therapy (71.4% [95% CI: 71.1, 71.6] vs. 73.3% [95% CI: 72.9, 73.6]) but more likely to experience an ADE (3.4% [95% CI: 3.3, 3.5] vs. 3.2% [95% CI: 3.1, 3.3]) and discontinue with CYP3A4-inhibitor therapy (21.0% [95% CI: 20.8, 21.3] vs. 19.5% [95% CI: 19.2, 19.8]). ADEs did not change these associations because those exposed to statin DDIs, vs. unexposed, were still less likely to discontinue statin therapy but more likely to discontinue CYP3A4-inhibitor therapy after experiencing an ADE.

Conclusion: We did not observe any meaningful clinical differences in the probability of premature statin discontinuation between statin users exposed to statin DDIs and those unexposed.

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Keywords
Adherence, Adverse drug events, Discontinuation, Drug-drug interactions, Multistate transition model, Statins
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Donneyong MM, Zhu Y, Zhang P, et al. A comprehensive assessment of statin discontinuation among patients who concurrently initiate statins and CYP3A4-inhibitor drugs; a multistate transition model. Br J Clin Pharmacol. 2023;89(7):2076-2087. doi:10.1111/bcp.15373
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British Journal of Clinical Pharmacology
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Attribution-NonCommercial-NoDerivatives 4.0 International Creative Commons licenses
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https://hdl.handle.net/1805/43639
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https://doi.org/10.1111/bcp.15373
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