Dynamic Mass Balance Modeling for Chemical Distribution Over Time in Systems With Repeated Dosing.

Front Toxicol

Department of Occupational and Environmental Health, School of Public Health, Université de Montréal, Montreal, QC, Canada.

Published: August 2022

As toxicologists and risk assessors move away from animal testing and more toward using models and biological modeling, it is necessary to produce tools to quantify the chemical distribution within the environment prior to extrapolating concentrations to human equivalent doses. Although models predicting chemical distribution have been developed, very little has been done for repeated dosing scenarios, which are common in prolonged experiments where the medium needs to be refreshed. Failure to account for repeated dosing may lead to inaccurate estimations of exposure and introduce bias into subsequent to extrapolations. Our objectives were to develop a dynamic mass balance model for repeated dosing in systems; to evaluate model accuracy against experimental data; and to perform illustrative simulations to assess the impact of repeated doses on predicted cellular concentrations. A novel dynamic partitioning mass balance model (IV-MBM DP v1.0) was created based on the well-established fugacity approach. We parameterized and applied the dynamic mass balance model to single dose and repeat dosing scenarios, and evaluated the predicted medium and cellular concentrations against available empirical data. We also simulated repeated dosing scenarios for organic chemicals with a range of partitioning properties and compared the distributions over time. In single dose scenarios, for which only medium concentrations were available, simulated concentrations predicted measured concentrations with coefficients of determination ( ) of 0.85-0.89, mean absolute error within a factor of two and model bias of nearly one. Repeat dose scenario simulations displayed model bias <2 within the cell lysate, and ∼1.5-3 in the medium. The concordance between simulated and available experimental data supports the predictive capacity of the IV-MBM DP v1.0 tool, but further evaluation as empirical data becomes available is warranted, especially for cellular concentrations.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9441784PMC
http://dx.doi.org/10.3389/ftox.2022.911128DOI Listing

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