Background: Although there are reports of adverse events (AEs) of cyclin-dependent kinase 4 and 6 (CDK4/6) inhibitors, the safety of ribociclib alone has not yet been comprehensively evaluated in real-world clinical practice.
Objectives: To investigate the overall real-world safety profile of ribociclib by mining data from the FDA Adverse Event Reporting System (FAERS).
Design: A retrospective disproportionality analysis was conducted based on the FAERS database.
Methods: We processed reports from the first quarter of 2017 to the second quarter of 2023 and applied disproportionality analysis using four different methods: reporting odds ratio, Medicines and Healthcare Products Regulatory Agency, Bayesian confidence propagation neural network, and multi-item gamma Poisson shrinker.
Results: A total of 12,885 AE reports of ribociclib as the primary suspect were enrolled. 48.81% of AEs occur within 60 days of ribociclib administration. Blood and lymphatic system disorders and abnormalities in investigation at the system organ class level showed statistically significant signals in all four methods. Nausea (n = 1426), neutropenia (n = 940), vomiting (n = 863), white blood cell count decreased (n = 812), and alopecia (n = 536) turned out to be the five most frequent AEs at the preferred term level. Twenty-eight AEs undiscovered in the label were newly identified. Neutropenia, as a widely recognized AE, was observed to potentially result in more serious outcomes than previously anticipated (p < 0.001).
Conclusion: This study utilized the FAERS database to analyze real-world AE signals associated with ribociclib following its market approval. We characterized the clinical profiles of reported AEs and found some significant signals consistent with previous clinical trials. In addition, several AEs not included in the drug label or exhibiting unexpected severity were detected. These findings provide valuable insights for clinicians and highlight directions for further causality-focused research to validate the observed results.
Keywords: FAERS; breast cancer; disproportionality analysis; ribociclib.
An analysis of the safety of ribociclib after its marketing based on the FDA Adverse Event Reporting System Why was the study done? Ribociclib, as an anti-cancer drug mainly applied to breast cancer patients, is now widely used. However, its comprehensive safety profile remains unrevealed. The researchers aim to use the adverse event reports registered in the FDA Adverse Event Reporting System to give a general view of adverse events of ribociclib in the real-world clinical practice after its marketing. What did the researchers do? The researchers collected reports from the first quarter of 2017 to the second quarter of 2023, analyzed the data and detected the signals of adverse events associated with ribociclib at different levels utilizing four different statistical methods. How is the study designed? This study is a disproportionality analysis, which analyzed the past data from the FAERS database. What did the researchers find? The researchers analyzed 12,885 reports in which ribociclib was suspected as the primary cause of the adverse event. Here are the main findings: - Almost half of the adverse events occur in the first 60 days of ribociclib using. - “Blood and lymphatic system disorders” and abnormalities in “Investigation” showed significant signals in all four methods used. Nausea, neutropenia, vomiting, white blood cell count decreased, and alopecia were the five most common adverse events with ribociclib. These were consistent with previous clinical trials. - 28 adverse events undiscovered in the drug label were identified. - Among the widely recognized adverse events, neutropenia could result in more serious outcomes than common knowledge. What do the findings mean? This study could serve as a warning to clinicians and provide a direction for further studies. Follow-up researches based on long-term data or further prospective studies are necessary to validate the results of our study and to reveal the causality.
© The Author(s), 2025.