Drug–Drug Interactions Involving Dexamethasone in Clinical Practice: Myth or Reality?

Author:

Bourdin Venceslas1,Bigot William1,Vanjak Anthony1ORCID,Burlacu Ruxandra1,Lopes Amanda1,Champion Karine1,Depond Audrey1,Amador-Borrero Blanca1ORCID,Sene Damien12,Comarmond Chloe12,Mouly Stéphane13

Affiliation:

1. Internal Medicine Department, Département Médico-Universitaire INVICTUS, Lariboisière Hospital, Assistance Publique-Hôpitaux de Paris (APHP).Nord—Université Paris-Cité, 75010 Paris, France

2. INSERM U976, Hôpital Saint-Louis, 75010 Paris, France

3. INSERM UMR-S1144, Hôpital Fernand Widal, 75010 Paris, France

Abstract

Concomitant administration of multiple drugs frequently causes severe pharmacokinetic or pharmacodynamic drug–drug interactions (DDIs) resulting in the possibility of enhanced toxicity and/or treatment failure. The activity of cytochrome P450 (CYP) 3A4 and P-glycoprotein (P-gp), a drug efflux pump sharing localization and substrate affinities with CYP3A4, is a critical determinant of drug clearance, interindividual variability in drug disposition and clinical efficacy, and appears to be involved in the mechanism of numerous clinically relevant DDIs, including those involving dexamethasone. The recent increase in the use of high doses of dexamethasone during the COVID-19 pandemic have emphasized the need for better knowledge of the clinical significance of drug–drug interactions involving dexamethasone in the clinical setting. We therefore aimed to review the already published evidence for various DDIs involving dexamethasone in vitro in cell culture systems and in vivo in animal models and humans.

Publisher

MDPI AG

Subject

General Medicine

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