PT  - JOURNAL ARTICLE
AU  - Pieter-Jan De Sutter
AU  - Pieter De Cock
AU  - Trevor N. Johnson
AU  - Helen Musther
AU  - Elke Gasthuys
AU  - An Vermeulen
TI  - Predictive Performance of Physiologically Based Pharmacokinetic Modelling of Beta-Lactam Antibiotic Concentrations in Adipose, Bone and Muscle Tissues
AID  - 10.1124/dmd.122.001129
DP  - 2023 Jan 01
TA  - Drug Metabolism and Disposition
PG  - DMD-AR-2022-001129
4099  - http://dmd.aspetjournals.org/content/early/2023/01/13/dmd.122.001129.short
4100  - http://dmd.aspetjournals.org/content/early/2023/01/13/dmd.122.001129.full
AB  - Physiologically based pharmacokinetic (PBPK) models consist of compartments representing different tissues. As most models are only verified based on plasma concentrations, it is unclear how reliable associated tissue profiles are. This study aimed to assess the accuracy of PBPK predicted beta-lactam antibiotic concentrations in different tissues and assess the impact of using effect site concentrations for evaluation of target attainment. Adipose, bone and muscle concentrations of five beta-lactams (piperacillin, cefazolin, cefuroxime, ceftazidime and meropenem) in healthy adults were collected from literature and compared to PBPK predictions. Model performance was evaluated with average fold errors (AFEs) and absolute AFEs (AAFEs) between predicted and observed concentrations. In total, 26 studies were included, 14 of which reported total tissue concentrations and 12 unbound interstitial fluid (uISF) concentrations. Concurrent plasma concentrations, used as baseline verification of the models, were fairly accurate (AFE: 1.14, AAFE: 1.50). Predicted total tissue concentrations were less accurate (AFE: 0.68, AAFE: 1.89). A slight trend for underprediction was observed but none of the studies had AFE or AAFE values outside threefold. Similarly, predictions of microdialysis-derived uISF concentrations were less accurate than plasma concentration predictions (AFE: 1.52, AAFE: 2.32). uISF concentrations tended to be overpredicted and two studies had AFEs and AAFEs outside threefold. Pharmacodynamic simulations in our case showed only a limited impact of using uISF concentrations instead of unbound plasma concentrations on target attainment rates. The results of this study illustrate the limitations of current PBPK models to predict tissue concentrations and the associated need for more accurate models. Significance Statement Clinical inaccessibility of local effect site concentrations precipitates a need for predictive methods for the estimation of tissue concentrations. This is the first study in which the accuracy of PBPK predicted tissue concentrations of beta-lactam antibiotics in man were assessed. Predicted tissue concentrations were found to be less accurate than concurrent predicted plasma concentrations. When using PBPK models to predict tissue concentrations this potential relative loss of accuracy should be acknowledged when clinical tissue concentrations are unavailable to verify predictions.