Drug-Associated Delirium Identified in The Food and Drug Administration Adverse Events Reporting System
Drug-Associated Delirium Identified in The Food and Drug Administration Adverse Events Reporting System
Author Info
Adrian Wong Angela Li Kane- Gill Matthew P. Gray Pamela L. Smithburger Seohyun (Claudia) Choi
Corresponding Author
Kane- GillUniversity of Pittsburgh Medical Center Presbyterian-Shadyside, Pittsburgh, Pennsylvania
A B S T R A C T
Introduction: Drug toxicity and polypharmacy are major risk factors for delirium, especially in older adult patients with underlying comorbidities. However, numerous case reports have described drugs with a lower suspicion of being deliriogenic. The objective of this study was to identify deliriogenic drugs in the Food and Drug Administration Adverse Events Reporting System (FAERS) to broaden the public knowledge and understanding. Study Design: Retrospective pharmacovigilance evaluation. Methods: FAERS reports from 2004 through 2015 were reviewed for delirium-associated terms, which were utilized to identify drugs most frequently reported to cause delirium. Drugs were categorized as: 1) known to be deliriogenic; 2) potentially deliriogenic; or 3) new potential to be deliriogenic. The 100 most frequently reported drugs were analyzed in reporting odds ratios (ROR). Results: Of the known deliriogenic drugs (n=32), paroxetine (ROR 4.1, CI 4.0-4.3), olanzapine (ROR 3.3, CI 3.2-3.4), and clozapine (ROR 2.9, CI 2.8-3.0) were most reported. Of the potentially deliriogenic drugs (n=54), duloxetine (ROR 3.2, CI 3.1-3.3), varenicline (ROR 3.1, CI 3.0-3.2), and gabapentin (ROR 2.9, CI 2.7-3.0) were most reported. Three drugs were considered to have new potential to be deliriogenic: heparin (ROR 1.5, CI 1.4-1.6), metformin (ROR 1.3, CI 1.3-1.4), and dalfampridine (ROR 1.1, CI 1.1-1.2). Conclusion: The majority of drugs were considered potentially deliriogenic. FAERS can provide postmarketing surveillance data to guide future studies on potentially deliriogenic drugs to guide management of causal agents.
Article Info
Article Type
Research ArticlePublication history
Received: Mon 08, Jul 2019Accepted: Tue 30, Jul 2019
Published: Mon 12, Aug 2019
Copyright
© 2023 Kane- Gill. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Hosting by Science Repository.DOI: 10.31487/j.PDR.2019.03.01