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Evidence‐based rationale for low dose nivolumab in critically ill patients with sepsis‐induced immunosuppression

Authors :
Demy A. C. van denHaak
Leila‐Sophie Otten
Hans J. P. M. Koenen
Ruben L. Smeets
Berber Piet
Peter Pickkers
Matthijs Kox
Rob ter Heine
Source :
Clinical and Translational Science, Vol 16, Iss 6, Pp 978-986 (2023)
Publication Year :
2023
Publisher :
Wiley, 2023.

Abstract

Abstract A substantial part of critically ill patients suffer from sepsis‐induced immunosuppression. Reversal of immunosuppression through PD‐1 checkpoint inhibition has been proposed as a treatment strategy to overcome immunosuppression in these patients. The PD‐1 inhibitor nivolumab, currently used in treatment of cancer, has been evaluated in phase I/II studies in patients with sepsis, demonstrating tolerability and signs of clinical efficacy. No proper dose finding was performed in these studies and, after a single high dose of 480 mg or 960 mg nivolumab, PD‐1 inhibition persisted beyond 90 days in the majority of cases. As the duration of sepsis is ~7–10 days, prolonged PD‐1 inhibition may unnecessarily induce longer‐term immune‐related side effects. Based on previously published pharmacokinetic and pharmacodynamic data of nivolumab, a thorough in silico dose finding study for nivolumab in critically ill patients was performed. We found that volume of distribution and clearance of nivolumab were not higher in patients with sepsis compared to the cancer population for which nivolumab is currently approved and showed profound variability. We found that with a single dose of 20 mg nivolumab, the PD‐1 receptor occupancy is predicted to stay above the 90% threshold for a median of 23 days (90% prediction interval of 7–78 days). We propose to investigate this dose in critically ill patients as a potential safe and cost‐effective pharmacotherapeutic intervention to treat sepsis‐induced immunosuppression.

Details

Language :
English
ISSN :
17528062 and 17528054
Volume :
16
Issue :
6
Database :
Directory of Open Access Journals
Journal :
Clinical and Translational Science
Publication Type :
Academic Journal
Accession number :
edsdoj.bb884040f1e74e3499a2afb8eaacaa74
Document Type :
article
Full Text :
https://doi.org/10.1111/cts.13503