Reproducibility of organ-level effects in repeat dose animal studies

Katie Paul Friedman; Miran J Foster; Ly Ly Pham; Madison Feshuk; Sean M Watford; John F Wambaugh; Richard S Judson; R Woodrow Setzer; Russell S Thomas

doi:10.1016/j.comtox.2023.100287

Reproducibility of organ-level effects in repeat dose animal studies

Comput Toxicol. 2023 Nov:28:1-17. doi: 10.1016/j.comtox.2023.100287.

Authors

Affiliations

¹ Center for Computational Toxicology and Exposure, Office of Research and Development, U.S. Environmental Protection Agency, Research Triangle Park, North Carolina, 27711, USA.
² Oak Ridge Associated Universities, Oak Ridge, TN.
³ Currently at Janssen Research & Development, LLC, San Diego, CA, USA; previously with Oak Ridge Institute for Science and Education, ORAU Way, Oak Ridge, TN 37380.
⁴ Center for Public Health and Environmental Assessment, Office of Research and Development, U.S. Environmental Protection Agency, Research Triangle Park, North Carolina, 27711, USA.
⁵ Emeritus contributor.

PMID: 37990691
PMCID: PMC10659077 (available on 2024-11-01)
DOI: 10.1016/j.comtox.2023.100287

Abstract

This work estimates benchmarks for new approach method (NAM) performance in predicting organ-level effects in repeat dose studies of adult animals based on variability in replicate animal studies. Treatment-related effect values from the Toxicity Reference database (v2.1) for weight, gross, or histopathological changes in the adrenal gland, liver, kidney, spleen, stomach, and thyroid were used. Rates of chemical concordance among organ-level findings in replicate studies, defined by repeated chemical only, chemical and species, or chemical and study type, were calculated. Concordance was 39 - 88%, depending on organ, and was highest within species. Variance in treatment-related effect values, including lowest effect level (LEL) values and benchmark dose (BMD) values when available, was calculated by organ. Multilinear regression modeling, using study descriptors of organ-level effect values as covariates, was used to estimate total variance, mean square error (MSE), and root residual mean square error (RMSE). MSE values, interpreted as estimates of unexplained variance, suggest study descriptors accounted for 52-69% of total variance in organ-level LELs. RMSE ranged from 0.41 - 0.68 log₁₀-mg/kg/day. Differences between organ-level effects from chronic (CHR) and subchronic (SUB) dosing regimens were also quantified. Odds ratios indicated CHR organ effects were unlikely if the SUB study was negative. Mean differences of CHR - SUB organ-level LELs ranged from -0.38 to -0.19 log₁₀ mg/kg/day; the magnitudes of these mean differences were less than RMSE for replicate studies. Finally, in vitro to in vivo extrapolation (IVIVE) was employed to compare bioactive concentrations from in vitro NAMs for kidney and liver to LELs. The observed mean difference between LELs and mean IVIVE dose predictions approached 0.5 log₁₀-mg/kg/day, but differences by chemical ranged widely. Overall, variability in repeat dose organ-level effects suggests expectations for quantitative accuracy of NAM prediction of LELs should be at least ± 1 log₁₀-mg/kg/day, with qualitative accuracy not exceeding 70%.

Keywords: ToxRefDB; Variability; organ; repeat dose.

Grants and funding

EPA999999/ImEPA/Intramural EPA/United States