Adverse drug events caused by three high-risk drug-drug interactions in patients admitted to intensive care units: a multicentre retrospective observational study

Publication date

2024-01

Authors

Klopotowska, Joanna E
Leopold, Jan-Hendrik
Bakker, Tinka
Yasrebi-de Kom, Izak
Engelaer, Frouke M
de Jonge, Evert
Haspels-Hogervorst, Esther K
van den Bergh, Walter M
Renes, Maurits H
Jong, Bas T

Editors

Advisors

Supervisors

Document Type

Article

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License

cc_by_nc

Abstract

Aims: Knowledge about adverse drug events caused by drug–drug interactions (DDI-ADEs) is limited. We aimed to provide detailed insights about DDI-ADEs related to three frequent, high-risk potential DDIs (pDDIs) in the critical care setting: pDDIs with international normalized ratio increase (INR+) potential, pDDIs with acute kidney injury (AKI) potential, and pDDIs with QTc prolongation potential. Methods: We extracted routinely collected retrospective data from electronic health records of intensive care units (ICUs) patients (≥18 years), admitted to ten hospitals in the Netherlands between January 2010 and September 2019. We used computerized triggers (e-triggers) to preselect patients with potential DDI-ADEs. Between September 2020 and October 2021, clinical experts conducted a retrospective manual patient chart review on a subset of preselected patients, and assessed causality, severity, preventability, and contribution to ICU length of stay of DDI-ADEs using internationally prevailing standards. Results: In total 85 422 patients with ≥1 pDDI were included. Of these patients, 32 820 (38.4%) have been exposed to one of the three pDDIs. In the exposed group, 1141 (3.5%) patients were preselected using e-triggers. Of 237 patients (21%) assessed, 155 (65.4%) experienced an actual DDI-ADE; 52.9% had severity level of serious or higher, 75.5% were preventable, and 19.3% contributed to a longer ICU length of stay. The positive predictive value was the highest for DDI-INR+ e-trigger (0.76), followed by DDI-AKI e-trigger (0.57). Conclusion: The highly preventable nature and severity of DDI-ADEs, calls for action to optimize ICU patient safety. Use of e-triggers proved to be a promising preselection strategy.

Keywords

adverse drug events, drug–drug interactions, intensive care, patient safety, triggers, Pharmacology (medical), Pharmacology, Journal Article

Citation

Klopotowska, J E, Leopold, J-H, Bakker, T, Yasrebi-de Kom, I, Engelaer, F M, de Jonge, E, Haspels-Hogervorst, E K, van den Bergh, W M, Renes, M H, Jong, B T, Kieft, H, Wieringa, A, Hendriks, S, Lau, C, van Bree, S H W, Lammers, H J W, Wierenga, P C, Bosman, R J, de Jong, V M, Slijkhuis, M, Franssen, E J F, Vermeijden, W J, Masselink, J, Purmer, I M, Bosma, L E, Hoeksema, M, Wesselink, E, de Lange, D W, de Keizer, N F, Dongelmans, D A & Abu-Hanna, A 2024, 'Adverse drug events caused by three high-risk drug-drug interactions in patients admitted to intensive care units : a multicentre retrospective observational study', British Journal of Clinical Pharmacology, vol. 90, no. 1, pp. 164-175. https://doi.org/10.1111/bcp.15882