Abstract
Tissue:plasma partition coefficients are key parameters in physiologically based pharmacokinetic (PBPK) models, yet the coefficients are challenging to measure in vivo. Several mechanistic-based equations have been developed to predict partition coefficients using tissue composition information and the compound's physicochemical properties, but it is not clear which, if any, of the methods is most appropriate under given circumstances. Complicating the evaluation, each prediction method was developed, and is typically employed, using a different set of tissue composition information, thereby making a controlled comparison impossible. This study proposed a standardized tissue composition for humans that can be used as a common input for each of the five frequently used prediction methods. These methods were implemented in R and were used to predict partition coefficients for 11 drugs, classified as strong bases, weak bases, acids, neutrals, and zwitterions. PBPK models developed in R (mrgsolve) for each drug and each set of partition coefficient predictions were compared with respective observed plasma concentration data. Percent root mean square error and half-life percent error were used to evaluate the accuracy of the PBPK model predictions using each partition coefficient method as summarized by strong bases, weak bases, acids, neutrals, and zwitterions characterization. The analysis indicated that no partition coefficient method consistently yielded the most accurate PBPK model predictions. As such, PBPK model predictions using all partition coefficient methods should be considered during drug development. SIGNIFICANCE STATEMENT: Several mechanistic-based methods exist to predict tissue:plasma partition coefficients critical to PBPK modeling. Controlled comparisons are confounded by the use of different tissue composition values for each method; a standardized tissue composition was proposed. Resulting assessments indicated that no method was consistently superior; therefore, sensitivity of PBPK predictions to each method may be warranted prior to model optimization.
Highlights
Based pharmacokinetic (PBPK) models predict the absorption, distribution, metabolism, and excretion properties of a drug at physiologically relevant scales
Since Physiologically based pharmacokinetic (PBPK) models are based on first principles, they can be used to make pharmacokinetic (PK) predictions for the drug of interest prior to conducting clinical trials
The goal of the current study was to investigate the impact of five commonly used tissue:plasma partition coefficient prediction methods (PT, Berez, Rodgers and Rowland (RR), Schmitt prediction method (Schmitt), and default PK-Sim prediction method (PK-Sim)) on PBPK model predictions based on a standardized human physiology and the physicochemical properties of 11 distinct drugs
Summary
Based pharmacokinetic (PBPK) models predict the absorption, distribution, metabolism, and excretion properties of a drug at physiologically relevant (e.g., tissue and organ) scales. Since PBPK models are based on first principles, they can be used to make pharmacokinetic (PK) predictions for the drug of interest prior to conducting clinical trials. Common applications include first-in-human, environmental toxicology, or rare-disease populations studies (Jones and Rowland-Yeo, 2013). Portions of this work were previously presented: Utsey K, Gastonguay MS, Russell S, Freling R, Riggs MM, and Elmokadem A. Impact of partition coefficient prediction methods on PBPK model output using a unified tissue composition, in ACoP10; 2019; Orlando, FL.
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