A comparison of transgenic rodent mutation and in vivo comet assay responses for 91 chemicals

David Kirkland; Dan D Levy; Matthew J LeBaron; Marilyn J Aardema; Carol Beevers; Javed Bhalli; George R Douglas; Patricia A Escobar; Christopher S Farabaugh; Melanie Guerard; George E Johnson; Rohan Kulkarni; Frank Le Curieux; Alexandra S Long; Jasmin Lott; David P Lovell; Mirjam Luijten; Francesco Marchetti; John J Nicolette; Stefan Pfuhler; Daniel J Roberts; Leon F Stankowski Jr; Veronique Thybaud; Sandy K Weiner; Andrew Williams; Kristine L Witt; Robert Young

doi:10.1016/j.mrgentox.2019.01.007

A comparison of transgenic rodent mutation and in vivo comet assay responses for 91 chemicals

Mutat Res Genet Toxicol Environ Mutagen. 2019 Mar:839:21-35. doi: 10.1016/j.mrgentox.2019.01.007. Epub 2019 Jan 18.

Authors

David Kirkland¹, Dan D Levy², Matthew J LeBaron³, Marilyn J Aardema⁴, Carol Beevers⁵, Javed Bhalli⁶, George R Douglas⁷, Patricia A Escobar⁸, Christopher S Farabaugh⁹, Melanie Guerard¹⁰, George E Johnson¹¹, Rohan Kulkarni⁶, Frank Le Curieux¹², Alexandra S Long⁷, Jasmin Lott¹³, David P Lovell¹⁴, Mirjam Luijten¹⁵, Francesco Marchetti⁷, John J Nicolette¹⁶, Stefan Pfuhler¹⁷, Daniel J Roberts⁹, Leon F Stankowski Jr⁹, Veronique Thybaud¹⁸, Sandy K Weiner¹⁹, Andrew Williams⁷, Kristine L Witt²⁰, Robert Young⁶

Affiliations

¹ Kirkland Consulting, PO Box 79, Tadcaster LS24 0AS, UK.
² US Food and Drug Administration Center for Food Safety and Applied Nutrition, College Park, MD, USA.
³ The Dow Chemical Company, Toxicology & Environmental Research & Consulting, Midland, MI, USA.
⁴ Marilyn Aardema Consulting LLC, 5315 Oakbrook Dr., Fairfield, OH 45014, USA.
⁵ Exponent International Ltd, Harrogate, UK.
⁶ MilliporeSigma, BioReliance Toxicology Testing Services, Rockville, MD, USA.
⁷ Environmental Health Science and Research Bureau, Health Canada, Ottawa, K1A 0K9, Canada.
⁸ Merck & Co. Inc., West Point, PA 19486, USA.
⁹ Charles River Laboratories, Skokie, IL, USA.
¹⁰ Roche Innovation Center Basel, pRed, F. Hoffmann-La Roche Ltd., Basel, Switzerland.
¹¹ Swansea University Medical School, Swansea, UK.
¹² European Chemicals Agency, Helsinki, Finland.
¹³ Boehringer Ingelheim Pharma GmbH & Co. KG, Biberach an der Riß, Germany.
¹⁴ St George's Medical School, University of London, London, UK.
¹⁵ Centre for Health Protection, National Institute for Public Health and the Environment (RIVM), Bilthoven, the Netherlands.
¹⁶ AbbVie, Inc., Pre-clinical Safety, North Chicago, Illinois, USA.
¹⁷ Procter & Gamble, Global Product Stewardship, Mason, OH 45040, USA.
¹⁸ Sanofi, Vitry-sur-Seine, France.
¹⁹ Janssen Research & Development, Spring House, PA 19477, USA.
²⁰ National Institute of Environmental Health Sciences/Division of the National Toxicology Program, Research Triangle Park, NC, USA.

Abstract

A database of 91 chemicals with published data from both transgenic rodent mutation (TGR) and rodent comet assays has been compiled. The objective was to compare the sensitivity of the two assays for detecting genotoxicity. Critical aspects of study design and results were tabulated for each dataset. There were fewer datasets from rats than mice, particularly for the TGR assay, and therefore, results from both species were combined for further analysis. TGR and comet responses were compared in liver and bone marrow (the most commonly studied tissues), and in stomach and colon evaluated either separately or in combination with other GI tract segments. Overall positive, negative, or equivocal test results were assessed for each chemical across the tissues examined in the TGR and comet assays using two approaches: 1) overall calls based on weight of evidence (WoE) and expert judgement, and 2) curation of the data based on a priori acceptability criteria prior to deriving final tissue specific calls. Since the database contains a high prevalence of positive results, overall agreement between the assays was determined using statistics adjusted for prevalence (using AC1 and PABAK). These coefficients showed fair or moderate to good agreement for liver and the GI tract (predominantly stomach and colon data) using WoE, reduced agreement for stomach and colon evaluated separately using data curation, and poor or no agreement for bone marrow using both the WoE and data curation approaches. Confidence in these results is higher for liver than for the other tissues, for which there were less data. Our analysis finds that comet and TGR generally identify the same compounds (mainly potent mutagens) as genotoxic in liver, stomach and colon, but not in bone marrow. However, the current database content precluded drawing assay concordance conclusions for weak mutagens and non-DNA reactive chemicals.

Keywords: DNA damage; Genotoxicity in vivo; Mutagens; Risk assessment; Transgenic rodents.

Publication types

Comparative Study

MeSH terms

Animals
Animals, Genetically Modified
Bone Marrow / drug effects*
Colon / drug effects*
Comet Assay / methods*
DNA Damage
Female
Liver / drug effects*
Male
Mice
Micronucleus Tests
Mutagens / toxicity*
Mutation*
Rats
Stomach / drug effects*

Substances

Mutagens

Grants and funding

Z99 ES999999/Intramural NIH HHS/United States