Facing the Challenge of Data Transfer from Animal Models to Humans: the Case of Persistent Organohalogens

<p>Abstract</p> <p>A well-documented fact for a group of persistent, bioaccumulating organohalogens contaminants, namely polychlorinated biphenyls (PCBs), is that appropriate regulation was delayed, on average, up to 50 years. Some of the delay may be attributed to the fact that th...

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Main Authors: Takser Larissa, Suvorov Alexander
Format: Article
Language:English
Published: BMC 2008-11-01
Series:Environmental Health
Online Access:http://www.ehjournal.net/content/7/1/58
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spelling doaj-d41bcd6ad534468f836121334e95b2bd2020-11-25T00:15:11ZengBMCEnvironmental Health1476-069X2008-11-01715810.1186/1476-069X-7-58Facing the Challenge of Data Transfer from Animal Models to Humans: the Case of Persistent OrganohalogensTakser LarissaSuvorov Alexander<p>Abstract</p> <p>A well-documented fact for a group of persistent, bioaccumulating organohalogens contaminants, namely polychlorinated biphenyls (PCBs), is that appropriate regulation was delayed, on average, up to 50 years. Some of the delay may be attributed to the fact that the science of toxicology was in its infancy when PCBs were introduced in 1920's. Nevertheless, even following the development of modern toxicology this story repeats itself 45 years later with polybrominated diphenyl ethers (PBDEs) another compound of concern for public health. The question is why? One possible explanation may be the low coherence between experimental studies of toxic effects in animal models and human studies. To explore this further, we reviewed a total of 807 PubMed abstracts and full texts reporting studies of toxic effects of PCB and PBDE in animal models. Our analysis documents that human epidemiological studies of PBDE stand to gain little from animal studies due to the following: 1) the significant delay between the commercialisation of a substance and studies with animal models; 2) experimental exposure levels in animals are several orders of magnitude higher than exposures in the general human population; 3) the limited set of evidence-based endocrine endpoints; 4) the traditional testing sequence (adult animals – neonates – foetuses) postpones investigation of the critical developmental stages; 5) limited number of animal species with human-like toxicokinetics, physiology of development and pregnancy; 6) lack of suitable experimental outcomes for the purpose of epidemiological studies. Our comparison of published PCB and PBDE studies underscore an important shortcoming: history has, unfortunately, repeated itself. Broadening the crosstalk between the various branches of toxicology should therefore accelerate accumulation of data to enable timely and appropriate regulatory action.</p> http://www.ehjournal.net/content/7/1/58
collection DOAJ
language English
format Article
sources DOAJ
author Takser Larissa
Suvorov Alexander
spellingShingle Takser Larissa
Suvorov Alexander
Facing the Challenge of Data Transfer from Animal Models to Humans: the Case of Persistent Organohalogens
Environmental Health
author_facet Takser Larissa
Suvorov Alexander
author_sort Takser Larissa
title Facing the Challenge of Data Transfer from Animal Models to Humans: the Case of Persistent Organohalogens
title_short Facing the Challenge of Data Transfer from Animal Models to Humans: the Case of Persistent Organohalogens
title_full Facing the Challenge of Data Transfer from Animal Models to Humans: the Case of Persistent Organohalogens
title_fullStr Facing the Challenge of Data Transfer from Animal Models to Humans: the Case of Persistent Organohalogens
title_full_unstemmed Facing the Challenge of Data Transfer from Animal Models to Humans: the Case of Persistent Organohalogens
title_sort facing the challenge of data transfer from animal models to humans: the case of persistent organohalogens
publisher BMC
series Environmental Health
issn 1476-069X
publishDate 2008-11-01
description <p>Abstract</p> <p>A well-documented fact for a group of persistent, bioaccumulating organohalogens contaminants, namely polychlorinated biphenyls (PCBs), is that appropriate regulation was delayed, on average, up to 50 years. Some of the delay may be attributed to the fact that the science of toxicology was in its infancy when PCBs were introduced in 1920's. Nevertheless, even following the development of modern toxicology this story repeats itself 45 years later with polybrominated diphenyl ethers (PBDEs) another compound of concern for public health. The question is why? One possible explanation may be the low coherence between experimental studies of toxic effects in animal models and human studies. To explore this further, we reviewed a total of 807 PubMed abstracts and full texts reporting studies of toxic effects of PCB and PBDE in animal models. Our analysis documents that human epidemiological studies of PBDE stand to gain little from animal studies due to the following: 1) the significant delay between the commercialisation of a substance and studies with animal models; 2) experimental exposure levels in animals are several orders of magnitude higher than exposures in the general human population; 3) the limited set of evidence-based endocrine endpoints; 4) the traditional testing sequence (adult animals – neonates – foetuses) postpones investigation of the critical developmental stages; 5) limited number of animal species with human-like toxicokinetics, physiology of development and pregnancy; 6) lack of suitable experimental outcomes for the purpose of epidemiological studies. Our comparison of published PCB and PBDE studies underscore an important shortcoming: history has, unfortunately, repeated itself. Broadening the crosstalk between the various branches of toxicology should therefore accelerate accumulation of data to enable timely and appropriate regulatory action.</p>
url http://www.ehjournal.net/content/7/1/58
work_keys_str_mv AT takserlarissa facingthechallengeofdatatransferfromanimalmodelstohumansthecaseofpersistentorganohalogens
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