4.5 Article

Are Non-animal Systemic Safety Assessments Protective? A Toolbox and Workflow

Journal

TOXICOLOGICAL SCIENCES
Volume 189, Issue 1, Pages 124-147

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/toxsci/kfac068

Keywords

Bayesian modelling; new approach methodologies; point of departure; physiologically based pharmacokinetics; probabilistic risk assessment

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This study proposes a core NAM toolbox and workflow for conducting systemic safety assessments for adult consumers. The toolbox includes physiologically based kinetic models and bioactivity platforms, and a Bayesian model is developed for quantifying uncertainty. The evaluation approach shows that the toolbox can make robust safety decisions without using animal data.
An important question in toxicological risk assessment is whether non-animal new approach methodologies (NAMs) can be used to make safety decisions that are protective of human health, without being overly conservative. In this work, we propose a core NAM toolbox and workflow for conducting systemic safety assessments for adult consumers. We also present an approach for evaluating how protective and useful the toolbox and workflow are by benchmarking against historical safety decisions. The toolbox includes physiologically based kinetic (PBK) models to estimate systemic C-max levels in humans, and 3 bioactivity platforms, comprising high-throughput transcriptomics, a cell stress panel, and in vitro pharmacological profiling, from which points of departure are estimated. A Bayesian model was developed to quantify the uncertainty in the C-max estimates depending on how the PBK models were parameterized. The feasibility of the evaluation approach was tested using 24 exposure scenarios from 10 chemicals, some of which would be considered high risk from a consumer goods perspective (eg, drugs that are systemically bioactive) and some low risk (eg, existing food or cosmetic ingredients). Using novel protectiveness and utility metrics, it was shown that up to 69% (9/13) of the low risk scenarios could be identified as such using the toolbox, whilst being protective against all (5/5) the high-risk ones. The results demonstrated how robust safety decisions could be made without using animal data. This work will enable a full evaluation to assess how protective and useful the toolbox and workflow are across a broader range of chemical-exposure scenarios.

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