Quantitative in vitro to in vivo extrapolation for developmental toxicity potency of valproic acid analogues

Xiaoqing Chang; Jessica Palmer; Annie Lumen; Un Jung Lee; Patricia Ceger; Kamel Mansouri; Catherine Sprankle; Elizabeth Donley; Shannon Bell; Thomas B Knudsen; John Wambaugh; Bethany Cook; David Allen; Nicole Kleinstreuer

doi:10.1002/bdr2.2019

Quantitative in vitro to in vivo extrapolation for developmental toxicity potency of valproic acid analogues

Birth Defects Res. 2022 Oct 1;114(16):1037-1055. doi: 10.1002/bdr2.2019. Epub 2022 May 9.

Authors

Affiliations

¹ Inotiv-RTP, Morrisville, North Carolina, USA.
² Stemina Biomarker Discovery, Inc., Madison, Wisconsin, USA.
³ National Center for Toxicological Research, U.S. Food and Drug Administration, Jefferson, Arkansas, USA.
⁴ National Toxicology Program Interagency Center for the Evaluation of Alternative Toxicological Methods, National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina, USA.
⁵ Center for Computational Toxicology and Exposure, Environmental Protection Agency, Research Triangle Park, North Carolina, USA.

Abstract

Background: The developmental toxicity potential (dTP) concentration from the devTOX quickPredict (devTOX^qP ) assay, a metabolomics-based human induced pluripotent stem cell assay, predicts a chemical's developmental toxicity potency. Here, in vitro to in vivo extrapolation (IVIVE) approaches were applied to address whether the devTOX^qP assay could quantitatively predict in vivo developmental toxicity lowest effect levels (LELs) for the prototypical teratogen valproic acid (VPA) and a group of structural analogues.

Methods: VPA and a series of structural analogues were tested with the devTOX^qP assay to determine dTP concentration and we estimated the equivalent administered doses (EADs) that would lead to plasma concentrations equivalent to the in vitro dTP concentrations. The EADs were compared to the LELs in rat developmental toxicity studies, human clinical doses, and EADs reported using other in vitro assays. To evaluate the impact of different pharmacokinetic (PK) models on IVIVE outcomes, we compared EADs predicted using various open-source and commercially available PK and physiologically based PK (PBPK) models. To evaluate the effect of in vitro kinetics, an equilibrium distribution model was applied to translate dTP concentrations to free medium concentrations before subsequent IVIVE analyses.

Results: The EAD estimates for the VPA analogues based on different PK/PBPK models were quantitatively similar to in vivo data from both rats and humans, where available, and the derived rank order of the chemicals was consistent with observed in vivo developmental toxicity. Different models were identified that provided accurate predictions for rat prenatal LELs and conservative estimates of human safe exposure. The impact of in vitro kinetics on EAD estimates is chemical-dependent. EADs from this study were within range of predicted doses from other in vitro and model organism data.

Conclusions: This study highlights the importance of pharmacokinetic considerations when using in vitro assays and demonstrates the utility of the devTOX^qP human stem cell-based platform to quantitatively assess a chemical's developmental toxicity potency.

Keywords: developmental toxicity potency; in vitro to in vivo extrapolation; pharmacokinetics; valproic acid (VPA) analogues.

Published 2022. This article is a U.S. Government work and is in the public domain in the USA. Birth Defects Research published by Wiley Periodicals LLC.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Animals
Female
Humans
Induced Pluripotent Stem Cells*
Pregnancy
Rats
Teratogens / toxicity
Valproic Acid* / toxicity

Substances

Teratogens
Valproic Acid

Grants and funding

HHSN273201500010C/ES/NIEHS NIH HHS/United States