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Drug-induced herpes zoster: a pharmacovigilance analysis of FDA adverse event reports from 2004 to 2024

Affiliation
Department of Dermatology ,The Affiliated Xuzhou Municipal Hospital of Xuzhou Medical University ,Xuzhou ,China
Xia, Jiali;
Affiliation
Department of Critical Care Medicine ,The Affiliated Xuzhou Municipal Hospital of Xuzhou Medical University ,Xuzhou ,China
Zhang, Jing;
Affiliation
Central Laboratory ,The Affiliated Xuzhou Municipal Hospital of Xuzhou Medical University ,Xuzhou ,China
Zhu, Hongyu;
Affiliation
Department of Dermatology ,The Affiliated Xuzhou Municipal Hospital of Xuzhou Medical University ,Xuzhou ,China
Ding, Li

Background Herpes zoster severely impacts patients’ quality of life and therapeutic results. This research utilized data from the FDA Adverse Event Reporting System (FAERS) to examine the prevalence and attributes of drug-induced herpes zoster. Methods We analyzed FAERS reports about zoster from Q1 2004 to Q3 2024 and developed a list of possible pathogenic agents. Ranked the 30 medicines with the greatest incidence of reported herpes zoster cases. Statistical disproportionality analysis was employed to identify an elevated reporting frequency of herpes zoster linked to a particular medication. Results Herpes zoster was referenced in 50,164 FAERS reports from 2004 to 2024. The majority of the implicated drugs were immunosuppressants. Anifrolumab exhibited the greatest ROR and PRR ratings among the drugs evaluated. Furthermore, rozanolixizumab, tozinameran, elapegademase, and other medications not indicated for inducing herpes zoster were recognized, underscoring the necessity for increased clinical vigilance and awareness. Nonetheless, these correlations should be regarded with caution, as they do not establish a direct causative relationship. Conclusion This study underscores the need of pharmacovigilance in recognizing and comprehending drug-induced herpes zoster. Additional research is required to validate these findings and to design strategies for risk management and reduction to enhance treatment outcomes in patients.

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License Holder: Copyright © 2025 Xia, Zhang, Zhu and Ding.

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