Frontiers in Toxicology (Apr 2022)

Considerations for Improving Metabolism Predictions for In Vitro to In Vivo Extrapolation

  • Marjory Moreau,
  • Pankajini Mallick,
  • Marci Smeltz,
  • Saad Haider,
  • Chantel I. Nicolas,
  • Salil N. Pendse,
  • Jeremy A. Leonard,
  • Matthew W. Linakis,
  • Patrick D. McMullen,
  • Rebecca A. Clewell,
  • Harvey J. Clewell,
  • Miyoung Yoon

DOI
https://doi.org/10.3389/ftox.2022.894569
Journal volume & issue
Vol. 4

Abstract

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High-throughput (HT) in vitro to in vivo extrapolation (IVIVE) is an integral component in new approach method (NAM)-based risk assessment paradigms, for rapidly translating in vitro toxicity assay results into the context of in vivo exposure. When coupled with rapid exposure predictions, HT-IVIVE supports the use of HT in vitro assays for risk-based chemical prioritization. However, the reliability of prioritization based on HT bioactivity data and HT-IVIVE can be limited as the domain of applicability of current HT-IVIVE is generally restricted to intrinsic clearance measured primarily in pharmaceutical compounds. Further, current approaches only consider parent chemical toxicity. These limitations occur because current state-of-the-art HT prediction tools for clearance and metabolite kinetics do not provide reliable data to support HT-IVIVE. This paper discusses current challenges in implementation of IVIVE for prioritization and risk assessment and recommends a path forward for addressing the most pressing needs and expanding the utility of IVIVE.

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