From vision toward best practices: Evaluating in vitro transcriptomic points of departure for application in risk assessment using a uniform workflow

The growing number of chemicals in the current consumer and industrial markets presents a major challenge for regulatory programs faced with the need to assess the potential risks they pose to human and ecological health. The increasing demand for hazard and risk assessment of chemicals currently ex...

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Autores principales: Reardon, Anthony J. F., Farmahin, Reza, Williams, Andrew, Meier, Matthew J., Addicks, Gregory C., Yauk, Carole L., Matteo, Geronimo, Atlas, Ella, Harrill, Joshua, Everett, Logan J., Shah, Imran, Judson, Richard, Ramaiahgari, Sreenivasa, Ferguson, Stephen S., Barton-Maclaren, Tara S.
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/PMC10242042/
https://www.ncbi.nlm.nih.gov/pubmed/37288009
http://dx.doi.org/10.3389/ftox.2023.1194895
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author Reardon, Anthony J. F.
Farmahin, Reza
Williams, Andrew
Meier, Matthew J.
Addicks, Gregory C.
Yauk, Carole L.
Matteo, Geronimo
Atlas, Ella
Harrill, Joshua
Everett, Logan J.
Shah, Imran
Judson, Richard
Ramaiahgari, Sreenivasa
Ferguson, Stephen S.
Barton-Maclaren, Tara S.
author_facet Reardon, Anthony J. F.
Farmahin, Reza
Williams, Andrew
Meier, Matthew J.
Addicks, Gregory C.
Yauk, Carole L.
Matteo, Geronimo
Atlas, Ella
Harrill, Joshua
Everett, Logan J.
Shah, Imran
Judson, Richard
Ramaiahgari, Sreenivasa
Ferguson, Stephen S.
Barton-Maclaren, Tara S.
author_sort Reardon, Anthony J. F.
collection PubMed
description The growing number of chemicals in the current consumer and industrial markets presents a major challenge for regulatory programs faced with the need to assess the potential risks they pose to human and ecological health. The increasing demand for hazard and risk assessment of chemicals currently exceeds the capacity to produce the toxicity data necessary for regulatory decision making, and the applied data is commonly generated using traditional approaches with animal models that have limited context in terms of human relevance. This scenario provides the opportunity to implement novel, more efficient strategies for risk assessment purposes. This study aims to increase confidence in the implementation of new approach methods in a risk assessment context by using a parallel analysis to identify data gaps in current experimental designs, reveal the limitations of common approaches deriving transcriptomic points of departure, and demonstrate the strengths in using high-throughput transcriptomics (HTTr) to derive practical endpoints. A uniform workflow was applied across six curated gene expression datasets from concentration-response studies containing 117 diverse chemicals, three cell types, and a range of exposure durations, to determine tPODs based on gene expression profiles. After benchmark concentration modeling, a range of approaches was used to determine consistent and reliable tPODs. High-throughput toxicokinetics were employed to translate in vitro tPODs (µM) to human-relevant administered equivalent doses (AEDs, mg/kg-bw/day). The tPODs from most chemicals had AEDs that were lower (i.e., more conservative) than apical PODs in the US EPA CompTox chemical dashboard, suggesting in vitro tPODs would be protective of potential effects on human health. An assessment of multiple data points for single chemicals revealed that longer exposure duration and varied cell culture systems (e.g., 3D vs. 2D) lead to a decreased tPOD value that indicated increased chemical potency. Seven chemicals were flagged as outliers when comparing the ratio of tPOD to traditional POD, thus indicating they require further assessment to better understand their hazard potential. Our findings build confidence in the use of tPODs but also reveal data gaps that must be addressed prior to their adoption to support risk assessment applications.
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spelling pubmed-102420422023-06-07 From vision toward best practices: Evaluating in vitro transcriptomic points of departure for application in risk assessment using a uniform workflow Reardon, Anthony J. F. Farmahin, Reza Williams, Andrew Meier, Matthew J. Addicks, Gregory C. Yauk, Carole L. Matteo, Geronimo Atlas, Ella Harrill, Joshua Everett, Logan J. Shah, Imran Judson, Richard Ramaiahgari, Sreenivasa Ferguson, Stephen S. Barton-Maclaren, Tara S. Front Toxicol Toxicology The growing number of chemicals in the current consumer and industrial markets presents a major challenge for regulatory programs faced with the need to assess the potential risks they pose to human and ecological health. The increasing demand for hazard and risk assessment of chemicals currently exceeds the capacity to produce the toxicity data necessary for regulatory decision making, and the applied data is commonly generated using traditional approaches with animal models that have limited context in terms of human relevance. This scenario provides the opportunity to implement novel, more efficient strategies for risk assessment purposes. This study aims to increase confidence in the implementation of new approach methods in a risk assessment context by using a parallel analysis to identify data gaps in current experimental designs, reveal the limitations of common approaches deriving transcriptomic points of departure, and demonstrate the strengths in using high-throughput transcriptomics (HTTr) to derive practical endpoints. A uniform workflow was applied across six curated gene expression datasets from concentration-response studies containing 117 diverse chemicals, three cell types, and a range of exposure durations, to determine tPODs based on gene expression profiles. After benchmark concentration modeling, a range of approaches was used to determine consistent and reliable tPODs. High-throughput toxicokinetics were employed to translate in vitro tPODs (µM) to human-relevant administered equivalent doses (AEDs, mg/kg-bw/day). The tPODs from most chemicals had AEDs that were lower (i.e., more conservative) than apical PODs in the US EPA CompTox chemical dashboard, suggesting in vitro tPODs would be protective of potential effects on human health. An assessment of multiple data points for single chemicals revealed that longer exposure duration and varied cell culture systems (e.g., 3D vs. 2D) lead to a decreased tPOD value that indicated increased chemical potency. Seven chemicals were flagged as outliers when comparing the ratio of tPOD to traditional POD, thus indicating they require further assessment to better understand their hazard potential. Our findings build confidence in the use of tPODs but also reveal data gaps that must be addressed prior to their adoption to support risk assessment applications. Frontiers Media S.A. 2023-05-23 /pmc/articles/PMC10242042/ /pubmed/37288009 http://dx.doi.org/10.3389/ftox.2023.1194895 Text en Copyright © 2023 Reardon, Farmahin, Williams, Meier, Addicks, Yauk, Matteo, Atlas, Harrill, Everett, Shah, Judson, Ramaiahgari, Ferguson and Barton-Maclaren. 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
Reardon, Anthony J. F.
Farmahin, Reza
Williams, Andrew
Meier, Matthew J.
Addicks, Gregory C.
Yauk, Carole L.
Matteo, Geronimo
Atlas, Ella
Harrill, Joshua
Everett, Logan J.
Shah, Imran
Judson, Richard
Ramaiahgari, Sreenivasa
Ferguson, Stephen S.
Barton-Maclaren, Tara S.
From vision toward best practices: Evaluating in vitro transcriptomic points of departure for application in risk assessment using a uniform workflow
title From vision toward best practices: Evaluating in vitro transcriptomic points of departure for application in risk assessment using a uniform workflow
title_full From vision toward best practices: Evaluating in vitro transcriptomic points of departure for application in risk assessment using a uniform workflow
title_fullStr From vision toward best practices: Evaluating in vitro transcriptomic points of departure for application in risk assessment using a uniform workflow
title_full_unstemmed From vision toward best practices: Evaluating in vitro transcriptomic points of departure for application in risk assessment using a uniform workflow
title_short From vision toward best practices: Evaluating in vitro transcriptomic points of departure for application in risk assessment using a uniform workflow
title_sort from vision toward best practices: evaluating in vitro transcriptomic points of departure for application in risk assessment using a uniform workflow
topic Toxicology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10242042/
https://www.ncbi.nlm.nih.gov/pubmed/37288009
http://dx.doi.org/10.3389/ftox.2023.1194895
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