Induction of Oxidative Stress Responses by Dioxin and other Ligands of the Aryl Hydrocarbon Receptor

Induction of Oxidative Stress Responses by Dioxin and other Ligands of the Aryl Hydrocarbon Receptor

TCDD and other polyhalogenated aromatic hydrocarbon ligands of the aryl hydrocarbon receptor (AHR) have been classically considered as non-genotoxic compounds because they fail to be directly mutagenic in either bacteria or most in vitro assay systems. They do so in spite of having repeatedly been l...

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Main Authors: John F. Reichard, Timothy P. Dalton, Howard G. Shertzer, Alvaro Puga
Format: Article
Language:English
Published: SAGE Publishing 2005-07-01
Series:Dose-Response
Online Access:https://doi.org/10.2203/dose-response.003.03.003
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spelling doaj-821c8d5936e7482db80a2e40cd47ab412020-11-25T02:34:07ZengSAGE PublishingDose-Response1559-32582005-07-01310.2203/dose-response.003.03.003Induction of Oxidative Stress Responses by Dioxin and other Ligands of the Aryl Hydrocarbon ReceptorJohn F. ReichardTimothy P. DaltonHoward G. ShertzerAlvaro PugaTCDD and other polyhalogenated aromatic hydrocarbon ligands of the aryl hydrocarbon receptor (AHR) have been classically considered as non-genotoxic compounds because they fail to be directly mutagenic in either bacteria or most in vitro assay systems. They do so in spite of having repeatedly been linked to oxidative stress and to mutagenic and carcinogenic outcomes. Oxidative stress, on the other hand, has been used as a marker for the toxicity of dioxin and its congeners. We have focused this review on the connection between oxidative stress induction and the toxic effects of fetal and adult dioxin exposure, with emphasis on the large species difference in sensitivity to this agent. We examine the roles that the dioxin-inducible cytochromes P450s play in the cellular and toxicological consequences of dioxin exposure with emphasis on oxidative stress involvement. Many components of the health consequences resulting from dioxin exposure may be attributable to epigenetic mechanisms arising from prolonged reactive oxygen generation.https://doi.org/10.2203/dose-response.003.03.003
collection DOAJ
language English
format Article
sources DOAJ
author John F. Reichard
Timothy P. Dalton
Howard G. Shertzer
Alvaro Puga
spellingShingle John F. Reichard
Timothy P. Dalton
Howard G. Shertzer
Alvaro Puga
Induction of Oxidative Stress Responses by Dioxin and other Ligands of the Aryl Hydrocarbon Receptor
Dose-Response
author_facet John F. Reichard
Timothy P. Dalton
Howard G. Shertzer
Alvaro Puga
author_sort John F. Reichard
title Induction of Oxidative Stress Responses by Dioxin and other Ligands of the Aryl Hydrocarbon Receptor
title_short Induction of Oxidative Stress Responses by Dioxin and other Ligands of the Aryl Hydrocarbon Receptor
title_full Induction of Oxidative Stress Responses by Dioxin and other Ligands of the Aryl Hydrocarbon Receptor
title_fullStr Induction of Oxidative Stress Responses by Dioxin and other Ligands of the Aryl Hydrocarbon Receptor
title_full_unstemmed Induction of Oxidative Stress Responses by Dioxin and other Ligands of the Aryl Hydrocarbon Receptor
title_sort induction of oxidative stress responses by dioxin and other ligands of the aryl hydrocarbon receptor
publisher SAGE Publishing
series Dose-Response
issn 1559-3258
publishDate 2005-07-01
description TCDD and other polyhalogenated aromatic hydrocarbon ligands of the aryl hydrocarbon receptor (AHR) have been classically considered as non-genotoxic compounds because they fail to be directly mutagenic in either bacteria or most in vitro assay systems. They do so in spite of having repeatedly been linked to oxidative stress and to mutagenic and carcinogenic outcomes. Oxidative stress, on the other hand, has been used as a marker for the toxicity of dioxin and its congeners. We have focused this review on the connection between oxidative stress induction and the toxic effects of fetal and adult dioxin exposure, with emphasis on the large species difference in sensitivity to this agent. We examine the roles that the dioxin-inducible cytochromes P450s play in the cellular and toxicological consequences of dioxin exposure with emphasis on oxidative stress involvement. Many components of the health consequences resulting from dioxin exposure may be attributable to epigenetic mechanisms arising from prolonged reactive oxygen generation.
url https://doi.org/10.2203/dose-response.003.03.003
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AT timothypdalton inductionofoxidativestressresponsesbydioxinandotherligandsofthearylhydrocarbonreceptor
AT howardgshertzer inductionofoxidativestressresponsesbydioxinandotherligandsofthearylhydrocarbonreceptor
AT alvaropuga inductionofoxidativestressresponsesbydioxinandotherligandsofthearylhydrocarbonreceptor
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