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Life-threatening toxicities upon Pembrolizumab intake: could pharmacokinetics be the bad guy?

Authors :
Hamimed, Mourad
Devillier, Raynier
Weiller, Pierre-Jean
Marin, Clémence
Schiano, Jean-Marc
Belmecheri, Nawel
Etienne-Grimaldi, Marie-Christine
Ciccolini, Joseph
Harbi, Samia
Source :
Cancer Chemotherapy & Pharmacology. Jun2024, Vol. 93 Issue 6, p627-632. 6p.
Publication Year :
2024

Abstract

Purpose: We report the case of an adult patient diagnosed with Hodgkin's lymphoma who was scheduled for Pembrolizumab after failure of standard therapy. After three well-tolerated courses of Pembrolizumab, a PET scan showed a favorable outcome and a fourth course of Pembrolizumab was started. Unexpectedly, extremely severe toxicities (i.e., autoimmune peripheral hypothyroidism, rhabdomyolysis and severe acute renal failure) occurred after this last course, requiring transfer to the intensive care unit. Methods: Therapeutic drug monitoring was performed to measure residual Pembrolizumab levels at intervals from the last dose (i.e., 120 and then 170 days), as well as pharmacogenetics investigations on the FCγR gene. Results: Pembrolizumab plasma concentrations that were still pharmacologically active months after the last administration, suggesting impaired elimination of Pembrolizumab in this patient. Further pharmacokinetic modeling based on the population approach showed that both half-life (47.8 days) and clearance (0.12 L/day) values were significantly different from the standard values usually reported in patients. Further in silico simulations showed that pharmacologically active concentrations of Pembrolizumab were maintained for up to 136 days after the last dose. The search for possible polymorphisms affecting the genes coding for FCγR (i.e., rs1801274 on FCGR2A and rs396991 on FCGR3A gene) was negative. Further TDM showed that Pembrolizumab could be detected up to 263 days after the last administration. Conclusion: This case report suggests that persistent overexposure in plasma could lead to life-threatening toxicities with Pembrolizumab. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
03445704
Volume :
93
Issue :
6
Database :
Academic Search Index
Journal :
Cancer Chemotherapy & Pharmacology
Publication Type :
Academic Journal
Accession number :
177481696
Full Text :
https://doi.org/10.1007/s00280-023-04611-x