Application of a new approach methodology (NAM)-based strategy for genotoxicity assessment of data-poor compounds

The conventional battery for genotoxicity testing is not well suited to assessing the large number of chemicals needing evaluation. Traditional in vitro tests lack throughput, provide little mechanistic information, and have poor specificity in predicting in vivo genotoxicity. New Approach Methodolo...

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Autores principales: Fortin, Anne-Marie V., Long, Alexandra S., Williams, Andrew, Meier, Matthew J., Cox, Julie, Pinsonnault, Claire, Yauk, Carole L., White, Paul A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Toxicology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9899896/
https://www.ncbi.nlm.nih.gov/pubmed/36756349
http://dx.doi.org/10.3389/ftox.2023.1098432
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author Fortin, Anne-Marie V.
Long, Alexandra S.
Williams, Andrew
Meier, Matthew J.
Cox, Julie
Pinsonnault, Claire
Yauk, Carole L.
White, Paul A.
author_facet Fortin, Anne-Marie V.
Long, Alexandra S.
Williams, Andrew
Meier, Matthew J.
Cox, Julie
Pinsonnault, Claire
Yauk, Carole L.
White, Paul A.
author_sort Fortin, Anne-Marie V.
collection PubMed
description The conventional battery for genotoxicity testing is not well suited to assessing the large number of chemicals needing evaluation. Traditional in vitro tests lack throughput, provide little mechanistic information, and have poor specificity in predicting in vivo genotoxicity. New Approach Methodologies (NAMs) aim to accelerate the pace of hazard assessment and reduce reliance on in vivo tests that are time-consuming and resource-intensive. As such, high-throughput transcriptomic and flow cytometry-based assays have been developed for modernized in vitro genotoxicity assessment. This includes: the TGx-DDI transcriptomic biomarker (i.e., 64-gene expression signature to identify DNA damage-inducing (DDI) substances), the MicroFlow(®) assay (i.e., a flow cytometry-based micronucleus (MN) test), and the MultiFlow(®) assay (i.e., a multiplexed flow cytometry-based reporter assay that yields mode of action (MoA) information). The objective of this study was to investigate the utility of the TGx-DDI transcriptomic biomarker, multiplexed with the MicroFlow(®) and MultiFlow(®) assays, as an integrated NAM-based testing strategy for screening data-poor compounds prioritized by Health Canada’s New Substances Assessment and Control Bureau. Human lymphoblastoid TK6 cells were exposed to 3 control and 10 data-poor substances, using a 6-point concentration range. Gene expression profiling was conducted using the targeted TempO-Seq™ assay, and the TGx-DDI classifier was applied to the dataset. Classifications were compared with those based on the MicroFlow(®) and MultiFlow(®) assays. Benchmark Concentration (BMC) modeling was used for potency ranking. The results of the integrated hazard calls indicate that five of the data-poor compounds were genotoxic in vitro, causing DNA damage via a clastogenic MoA, and one via a pan-genotoxic MoA. Two compounds were likely irrelevant positives in the MN test; two are considered possibly genotoxic causing DNA damage via an ambiguous MoA. BMC modeling revealed nearly identical potency rankings for each assay. This ranking was maintained when all endpoint BMCs were converted into a single score using the Toxicological Prioritization (ToxPi) approach. Overall, this study contributes to the establishment of a modernized approach for effective genotoxicity assessment and chemical prioritization for further regulatory scrutiny. We conclude that the integration of TGx-DDI, MicroFlow(®), and MultiFlow(®) endpoints is an effective NAM-based strategy for genotoxicity assessment of data-poor compounds.
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spelling pubmed-98998962023-02-07 Application of a new approach methodology (NAM)-based strategy for genotoxicity assessment of data-poor compounds Fortin, Anne-Marie V. Long, Alexandra S. Williams, Andrew Meier, Matthew J. Cox, Julie Pinsonnault, Claire Yauk, Carole L. White, Paul A. Front Toxicol Toxicology The conventional battery for genotoxicity testing is not well suited to assessing the large number of chemicals needing evaluation. Traditional in vitro tests lack throughput, provide little mechanistic information, and have poor specificity in predicting in vivo genotoxicity. New Approach Methodologies (NAMs) aim to accelerate the pace of hazard assessment and reduce reliance on in vivo tests that are time-consuming and resource-intensive. As such, high-throughput transcriptomic and flow cytometry-based assays have been developed for modernized in vitro genotoxicity assessment. This includes: the TGx-DDI transcriptomic biomarker (i.e., 64-gene expression signature to identify DNA damage-inducing (DDI) substances), the MicroFlow(®) assay (i.e., a flow cytometry-based micronucleus (MN) test), and the MultiFlow(®) assay (i.e., a multiplexed flow cytometry-based reporter assay that yields mode of action (MoA) information). The objective of this study was to investigate the utility of the TGx-DDI transcriptomic biomarker, multiplexed with the MicroFlow(®) and MultiFlow(®) assays, as an integrated NAM-based testing strategy for screening data-poor compounds prioritized by Health Canada’s New Substances Assessment and Control Bureau. Human lymphoblastoid TK6 cells were exposed to 3 control and 10 data-poor substances, using a 6-point concentration range. Gene expression profiling was conducted using the targeted TempO-Seq™ assay, and the TGx-DDI classifier was applied to the dataset. Classifications were compared with those based on the MicroFlow(®) and MultiFlow(®) assays. Benchmark Concentration (BMC) modeling was used for potency ranking. The results of the integrated hazard calls indicate that five of the data-poor compounds were genotoxic in vitro, causing DNA damage via a clastogenic MoA, and one via a pan-genotoxic MoA. Two compounds were likely irrelevant positives in the MN test; two are considered possibly genotoxic causing DNA damage via an ambiguous MoA. BMC modeling revealed nearly identical potency rankings for each assay. This ranking was maintained when all endpoint BMCs were converted into a single score using the Toxicological Prioritization (ToxPi) approach. Overall, this study contributes to the establishment of a modernized approach for effective genotoxicity assessment and chemical prioritization for further regulatory scrutiny. We conclude that the integration of TGx-DDI, MicroFlow(®), and MultiFlow(®) endpoints is an effective NAM-based strategy for genotoxicity assessment of data-poor compounds. Frontiers Media S.A. 2023-01-23 /pmc/articles/PMC9899896/ /pubmed/36756349 http://dx.doi.org/10.3389/ftox.2023.1098432 Text en Copyright © 2023 His Majesty the King in Right of Canada. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Toxicology
Fortin, Anne-Marie V.
Long, Alexandra S.
Williams, Andrew
Meier, Matthew J.
Cox, Julie
Pinsonnault, Claire
Yauk, Carole L.
White, Paul A.
Application of a new approach methodology (NAM)-based strategy for genotoxicity assessment of data-poor compounds
title Application of a new approach methodology (NAM)-based strategy for genotoxicity assessment of data-poor compounds
title_full Application of a new approach methodology (NAM)-based strategy for genotoxicity assessment of data-poor compounds
title_fullStr Application of a new approach methodology (NAM)-based strategy for genotoxicity assessment of data-poor compounds
title_full_unstemmed Application of a new approach methodology (NAM)-based strategy for genotoxicity assessment of data-poor compounds
title_short Application of a new approach methodology (NAM)-based strategy for genotoxicity assessment of data-poor compounds
title_sort application of a new approach methodology (nam)-based strategy for genotoxicity assessment of data-poor compounds
topic Toxicology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9899896/
https://www.ncbi.nlm.nih.gov/pubmed/36756349
http://dx.doi.org/10.3389/ftox.2023.1098432
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