Characteristics of CYP3A4-related potential drug-drug interactions in outpatients receiving prescriptions from multiple clinical departments

Rina Matsuoka; Shinsuke Akagi; Tomohiro Konishi; Masashi Kondo; Hideki Matsubara; Shohei Yamamoto; Keiji Izushi; Yuichi Tasaka

doi:10.1186/s40780-024-00368-4

Journal of Pharmaceutical Health Care and Sciences (Aug 2024)

Characteristics of CYP3A4-related potential drug-drug interactions in outpatients receiving prescriptions from multiple clinical departments

Rina Matsuoka,
Shinsuke Akagi,
Tomohiro Konishi,
Masashi Kondo,
Hideki Matsubara,
Shohei Yamamoto,
Keiji Izushi,
Yuichi Tasaka

Affiliations

Rina Matsuoka: Laboratory of Clinical Pharmacy, School of Pharmacy, Shujitsu University
Shinsuke Akagi: Laboratory of Clinical Pharmacy, School of Pharmacy, Shujitsu University
Tomohiro Konishi: Kojima Ai Pharmacy
Masashi Kondo: Uizu Pharmacy
Hideki Matsubara: Fuji Pharmacy
Shohei Yamamoto: Koukando Pharmacy
Keiji Izushi: Izushi Pharmacy
Yuichi Tasaka: Laboratory of Clinical Pharmacy, School of Pharmacy, Shujitsu University

DOI: https://doi.org/10.1186/s40780-024-00368-4
Journal volume & issue: Vol. 10, no. 1
pp. 1 – 8

Abstract

Read online

Abstract Background Drug-drug interactions (DDIs) increase the incidence of adverse drug reactions (ADRs). In a previous report, we revealed that the incidence of potential DDIs due to the same CYP molecular species in one prescription exceeds 90% among patients taking six or more drugs and that CYP3A4 markedly influences the increase in the number of potential DDIs in clinical practice. However, the factors contributing to an increased number of potential DDIs in prescriptions from multiple clinical departments remain poorly clarified. Methods This observational study was performed at five pharmacies in Okayama Prefecture, Japan. Patients who visited these pharmacies from 11 April 2022 to 24 April 2022 were included, except those who had prescriptions only from a single clinical department. A stratified analysis was performed to determine the incidence of CYP3A4-related potential DDIs according to the number of drugs taken. Additionally, factors associated with an increase in the number of drugs involved in CYP3A4-related potential DDIs were identified using multiple linear regression analysis. In this study, potential DDIs for the prescription data subdivided by clinical department, containing two or more drugs, were used as control data. Results Overall, 372 outpatients who received prescriptions from multiple clinical departments were included in the current study. The number of drugs contributing to CYP3A4-related potential DDIs increased with an increase in the number of clinical departments. Notably, in cases taking fewer than six drugs, prescriptions from multiple clinical departments had a higher frequency of CYP3A4-related potential DDIs than those in prescriptions subdivided by clinical department. Multiple regression analysis identified "Cardiovascular agents", "Agents affecting central nervous system", and "Urogenital and anal organ agents" as the top three drug classes that increase CYP3A4-related potential DDIs. Conclusion Collectively, these results highlight the importance of a unified management strategy for prescribed drugs and continuous monitoring of ADRs in outpatients receiving prescriptions from multiple clinical departments even if the number of drugs taken is less than six.

Published in Journal of Pharmaceutical Health Care and Sciences

ISSN: 2055-0294 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Therapeutics. Pharmacology; Medicine: Pharmacy and materia medica
Website: https://jphcs.biomedcentral.com/

About the journal

Abstract

Keywords