Ethylene Oxide: Cancer Evidence Integration and Dose–Response Implications

The International Agency for Research on Cancer (IARC) and the United States Environmental Protection Agency (USEPA) classified ethylene oxide (EtO) as a known human carcinogen. Critically, both noted that the epidemiological evidence based on lymphoid and breast cancers was “limited,” but that the...

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Main Authors: Melissa J. Vincent, Jordan S. Kozal, William J. Thompson, Andrew Maier, G. Scott Dotson, Elizabeth A. Best, Kenneth A. Mundt
Format: Article
Language:English
Published: SAGE Publishing 2019-12-01
Series:Dose-Response
Online Access:https://doi.org/10.1177/1559325819888317
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spelling doaj-b4781d30b39f4777b72dbae4bf3f9d412020-11-25T03:38:27ZengSAGE PublishingDose-Response1559-32582019-12-011710.1177/1559325819888317Ethylene Oxide: Cancer Evidence Integration and Dose–Response ImplicationsMelissa J. Vincent0Jordan S. Kozal1William J. Thompson2Andrew Maier3G. Scott Dotson4Elizabeth A. Best5Kenneth A. Mundt6 Cardno ChemRisk, Cincinnati, OH, USA Cardno ChemRisk, San Francisco, CA, USA Cardno ChemRisk, Boston, MA, USA Cardno ChemRisk, Cincinnati, OH, USA Cardno ChemRisk, Cincinnati, OH, USA Cardno ChemRisk, Boulder, CO, USA Cardno ChemRisk, Boston, MA, USAThe International Agency for Research on Cancer (IARC) and the United States Environmental Protection Agency (USEPA) classified ethylene oxide (EtO) as a known human carcinogen. Critically, both noted that the epidemiological evidence based on lymphoid and breast cancers was “limited,” but that the evidence in animal studies was “sufficient” and “extensive” (respectively) and that EtO is genotoxic. The USEPA derived one of the highest published inhalation unit risk (IUR) values (3 × 10 −3 per [µg/m 3 EtO]), based on results from 2 epidemiological studies. We performed focused reviews of the epidemiological and toxicological evidence on the carcinogenicity of EtO and considered the USEPA’s reliance on a genotoxic mode of action to establish EtO’s carcinogenicity and to determine likely dose–response patterns. Higher quality epidemiological studies demonstrated no increased risk of breast cancers or lymphohematopoietic malignancies (LHM). Similarly, toxicological studies and studies of early effect biomarkers in animals and humans provided no strong indication that EtO causes LHM or mammary cancers. Ultimately, animal data are inadequate to define the actual dose–response shape or predict tumor response at very low doses with any confidence. We conclude that the IARC and USEPA classification of EtO as a known human carcinogen overstates the underlying evidence and that the IUR derived by USEPA grossly overestimates risk.https://doi.org/10.1177/1559325819888317
collection DOAJ
language English
format Article
sources DOAJ
author Melissa J. Vincent
Jordan S. Kozal
William J. Thompson
Andrew Maier
G. Scott Dotson
Elizabeth A. Best
Kenneth A. Mundt
spellingShingle Melissa J. Vincent
Jordan S. Kozal
William J. Thompson
Andrew Maier
G. Scott Dotson
Elizabeth A. Best
Kenneth A. Mundt
Ethylene Oxide: Cancer Evidence Integration and Dose–Response Implications
Dose-Response
author_facet Melissa J. Vincent
Jordan S. Kozal
William J. Thompson
Andrew Maier
G. Scott Dotson
Elizabeth A. Best
Kenneth A. Mundt
author_sort Melissa J. Vincent
title Ethylene Oxide: Cancer Evidence Integration and Dose–Response Implications
title_short Ethylene Oxide: Cancer Evidence Integration and Dose–Response Implications
title_full Ethylene Oxide: Cancer Evidence Integration and Dose–Response Implications
title_fullStr Ethylene Oxide: Cancer Evidence Integration and Dose–Response Implications
title_full_unstemmed Ethylene Oxide: Cancer Evidence Integration and Dose–Response Implications
title_sort ethylene oxide: cancer evidence integration and dose–response implications
publisher SAGE Publishing
series Dose-Response
issn 1559-3258
publishDate 2019-12-01
description The International Agency for Research on Cancer (IARC) and the United States Environmental Protection Agency (USEPA) classified ethylene oxide (EtO) as a known human carcinogen. Critically, both noted that the epidemiological evidence based on lymphoid and breast cancers was “limited,” but that the evidence in animal studies was “sufficient” and “extensive” (respectively) and that EtO is genotoxic. The USEPA derived one of the highest published inhalation unit risk (IUR) values (3 × 10 −3 per [µg/m 3 EtO]), based on results from 2 epidemiological studies. We performed focused reviews of the epidemiological and toxicological evidence on the carcinogenicity of EtO and considered the USEPA’s reliance on a genotoxic mode of action to establish EtO’s carcinogenicity and to determine likely dose–response patterns. Higher quality epidemiological studies demonstrated no increased risk of breast cancers or lymphohematopoietic malignancies (LHM). Similarly, toxicological studies and studies of early effect biomarkers in animals and humans provided no strong indication that EtO causes LHM or mammary cancers. Ultimately, animal data are inadequate to define the actual dose–response shape or predict tumor response at very low doses with any confidence. We conclude that the IARC and USEPA classification of EtO as a known human carcinogen overstates the underlying evidence and that the IUR derived by USEPA grossly overestimates risk.
url https://doi.org/10.1177/1559325819888317
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