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A Collaborative Initiative to Establish Genomic Biomarkers for Assessing Tumorigenic Potential to Reduce Reliance on Conventional Rodent Carcinogenicity Studies

Authors :
J Christopher Corton
Constance A Mitchell
Scott Auerbach
Pierre Bushel
Heidrun Ellinger-Ziegelbauer
Patricia A Escobar
Roland Froetschl
Alison H Harrill
Kamin Johnson
James E Klaunig
Arun R Pandiri
Alexei A Podtelezhnikov
Julia E Rager
Keith Q Tanis
Jan Willem van der Laan
Alisa Vespa
Carole L Yauk
Syril D Pettit
Frank D Sistare
Source :
Toxicological Sciences. 188:4-16
Publication Year :
2022
Publisher :
Oxford University Press (OUP), 2022.

Abstract

There is growing recognition across broad sectors of the scientific community that use of genomic biomarkers has the potential to reduce the need for conventional rodent carcinogenicity studies of industrial chemicals, agrochemicals, and pharmaceuticals through a weight-of-evidence approach. These biomarkers fall into 2 major categories: (1) sets of gene transcripts that can identify distinct tumorigenic mechanisms of action; and (2) cancer driver gene mutations indicative of rapidly expanding growth-advantaged clonal cell populations. This call-to-action article describes a collaborative approach launched to develop and qualify biomarker gene expression panels that measure widely accepted molecular pathways linked to tumorigenesis and their activation levels to predict tumorigenic doses of chemicals from short-term exposures. Growing evidence suggests that application of such biomarker panels in short-term exposure rodent studies can identify both tumorigenic hazard and tumorigenic activation levels for chemical-induced carcinogenicity. In the future, this approach will be expanded to include methodologies examining mutations in key cancer driver gene mutation hotspots as biomarkers of both genotoxic and nongenotoxic chemical tumor risk. Analytical, technical, and biological validation studies of these complementary genomic tools are being undertaken by multisector and multidisciplinary collaborative teams within the Health and Environmental Sciences Institute. Success from these efforts will facilitate the transition from current heavy reliance on conventional 2-year rodent carcinogenicity studies to more rapid animal- and resource-sparing approaches for mechanism-based carcinogenicity evaluation supporting internal and regulatory decision-making.

Details

ISSN :
10960929 and 10966080
Volume :
188
Database :
OpenAIRE
Journal :
Toxicological Sciences
Accession number :
edsair.doi.dedup.....ab1ea167ef959d91cb05ee2aeb0e6fc9
Full Text :
https://doi.org/10.1093/toxsci/kfac041