In vivo genotoxicity testing strategies: Report from the 8th International Workshop on Genotoxicity Testing (IWGT)

Carol Beevers; Yoshifumi Uno; Krista Meurer; Shuichi Hamada; Kiyohiro Hashimoto; David Kirkland; Matthew J LeBaron; Frank Le Curieux; Ludovic Le Hegarat; Hans-Joerg Martus; Kenichi Masumura; Wakako Ohyama; Daniel J Roberts; Marie Vasquez; James Whitwell; Kristine L Witt

doi:10.1002/em.22578

In vivo genotoxicity testing strategies: Report from the 8th International Workshop on Genotoxicity Testing (IWGT)

Environ Mol Mutagen. 2023 Nov 9. doi: 10.1002/em.22578. Online ahead of print.

Authors

Carol Beevers¹, Yoshifumi Uno², Krista Meurer³, Shuichi Hamada⁴, Kiyohiro Hashimoto⁵, David Kirkland⁶, Matthew J LeBaron⁷, Frank Le Curieux⁸, Ludovic Le Hegarat⁹, Hans-Joerg Martus¹⁰, Kenichi Masumura¹¹, Wakako Ohyama¹², Daniel J Roberts¹³, Marie Vasquez¹⁴, James Whitwell¹⁵, Kristine L Witt¹⁶

Affiliations

¹ Corteva Agriscience, Oxford, UK.
² LSI Medience Co., Tokyo, Japan.
³ BASF SE, Limburgerhof, Germany.
⁴ BoZo Research Center Inc., Tokyo, Japan.
⁵ Takeda Pharmaceutical Co., Ltd., Tokyo, Japan.
⁶ Kirkland Consulting, Tadcaster, UK.
⁷ The Dow Chemical Company, Midland, Michigan, USA.
⁸ European Chemicals Agency, Helsinki, Finland.
⁹ ANSES, French Agency for Food, Environmental and Occupational Health and Safety, Fougères Laboratory, Toxicology of Contaminants Unit, Fougères, France.
¹⁰ Preclinical Safety, Novartis Institutes for BioMedical Research, Basel, Switzerland.
¹¹ National Institute of Health Sciences, Kawasaki, Kanagawa, Japan.
¹² Yakult Central Institute, Yakult Honsha Co., Ltd., Tokyo, Japan.
¹³ Charles River Labs, Genetic & In Vitro Toxicology, Cook County, Illinois, USA.
¹⁴ Helix3 Inc., Morrisville, North Carolina, USA.
¹⁵ Labcorp Drug Development, Harrogate, UK.
¹⁶ Division of Translational Toxicology, National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina, USA.

PMID: 37942839
DOI: 10.1002/em.22578

Abstract

The in vivo working group (WG) considered three topics: acceptable maximum doses for negative erythrocyte micronucleus (MN) tests, validation status of MN assays in non-hematopoietic tissues, and nuisance factors in the comet assay. The WG reached agreement on many issues, including: negative erythrocyte MN studies should be acceptable if dosing is conducted to Organisation for Economic Co-operation and Development (OECD) test guideline (TG) 474 recommendations and if sufficient bone marrow exposure is demonstrated; consensus on the evidence required to demonstrate "sufficient" exposure was not reached. The liver MN test using six-week-old rats is sufficiently validated to develop an OECD TG, but the impact of animal age warrants additional study. Ki-67 is a reliable marker for cellular proliferation in hepatocytes. The gastrointestinal tract MN test is useful for detecting poorly absorbed or rapidly degraded aneugens, and for genotoxic metabolites formed in the colon. Although current validation data are insufficient to support the development of an OECD TG, the methodologies are sufficient to consider as an appendix to OECD TG474. Comparison of comet assay results to laboratory historical control data (HCD) should not be used in data evaluation, unless the HCD distribution is demonstrated to be stable and the predominant source of HCD variation is due to animal, not study, factors. No universally acceptable negative control limit for any tissue was identified. Methodological differences in comet studies can result in variable data interpretations; more data are required before best practice recommendations can be made. Hedgehogs alone are unreliable indicators of cytotoxicity and additional investigations into cytotoxicity markers are required.

Keywords: GI tract micronucleus; International Workshop on Genotoxicity Testing (IWGT); comet assay; genetic toxicology; in vivo; liver micronucleus.

Publication types

Review