Drug-Related Glomerular Phenotypes: A Global Pharmacovigilance Perspective

Author:

Baptista Alexandre12,Macedo Ana M.12,Marreiros Ana12ORCID,Coelho André3ORCID,Perazella Mark A.4ORCID

Affiliation:

1. School of Medicine and Biomedical Sciences, Algarve University (UAlg), 8005-139 Faro, Portugal

2. Algarve Biomedical Centre (ABC), 8005-139 Faro, Portugal

3. Escola Superior Saúde e Tecnologia de Lisboa (ESTEsL), 1990-096 Lisboa, Portugal

4. School of Medicine, Yale University, New Haven, CT 06520, USA

Abstract

Introduction: Adverse drug reactions are a significant problem in modern society, stemming from the increase in prescribed medications, over-the-counter drugs, and overall polypharmacy. Glomerular disorders are one of the frequently reported renal conditions associated with medication use. VigiBase is a significant tool for evaluating events associated with drug use, and, to the authors’ knowledge, no study has yet assessed this database to identify the primary medications associated with glomerular disorders. Materials and Methods: We collected data from VigiBase for 54 years and evaluated data based on global frequencies, disproportionality (IC025 values), nephrotoxic potential, and physiopathological mechanisms. Results: Over the evaluation period, 33.932.051 spontaneous notifications of adverse drug reactions reported in VigiBase were assessed, from which 106.775 notifications of drug-associated glomerular disorders were extracted. The isolated medications were classified as ‘potential nephrotoxins’ (47.0%), with 40% of the medications lacking scientific references to report any association with the development of glomerular disorders. Among the evaluated medications, Inotersen (IC025 of 8.3), Penicillamine (IC025 6.8), Bevacizumab (IC025 5.9) and Lenvatinib (IC025 5.4) were identified as having the strongest association with these glomerular disorders. For medications classified as ‘non-nephrotoxic’, a high disproportionality index was observed, suggesting drugs that might be considered as new potential nephrotoxins. Conclusions: Drug-induced glomerular disorders were significantly associated with medications that had no established nephrotoxic role but demonstrated a high disproportionality index in VigiBase. These newly alleged nephrotoxic drugs warrant further evaluation in dedicated studies to assess their true nephrotoxic potential.

Funder

Algarve Biomedical Centre/University of Algarve

Publisher

MDPI AG

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