Improving prediction of chemical carcinogenicity by considering multiple mechanisms and applying toxicogenomic approaches | Health & Environmental Research Online (HERO)

Health & Environmental Research Online (HERO)

Print Feedback Export to File

This record has one attached file:

Citation
Tags

HERO ID

412535

Reference Type

Journal Article

Subtype

Review

Title

Improving prediction of chemical carcinogenicity by considering multiple mechanisms and applying toxicogenomic approaches

Author(s)

Guyton, KZ; Kyle, AD; Aubrecht, J; Cogliano, VJ; Eastmond, DA; Jackson, M; Keshava, N; Sandy, MS; Sonawane, B; Zhang, LP; Waters, MD; Smith, MT

Year

2009

Is Peer Reviewed?

Journal

Mutation Research: Reviews in Mutation Research
ISSN: 1383-5742
EISSN: 1388-2139

Volume

681

Issue

2-3

Page Numbers

230-240

Language

English

PMID

19010444

DOI

10.1016/j.mrrev.2008.10.001

Web of Science Id

WOS:000264095000010

Abstract

While scientific knowledge of the potential health significance of chemical exposures has grown, experimental methods for predicting the carcinogenicity of environmental agents have not been substantially updated in the last two decades. Current methodologies focus first on identifying genotoxicants under the premise that agents capable of directly damaging DNA are most likely to be carcinogenic to humans. Emphasis on the distinction between genotoxic and non-genotoxic carcinogens is also motivated by assumed implications for the dose-response curve; it is purported that genotoxicants would lack a threshold in the low dose region, in contrast to non-genotoxic agents. However, for the vast majority of carcinogens, little if any empirical data exist to clarify the nature of the cancer dose-response relationship at low doses in the exposed human population. Recent advances in scientific understanding of cancer biology-and increased appreciation of the multiple impacts of carcinogens on this disease process-support the view that environmental chemicals can act through multiple toxicity pathways, modes and/or mechanisms of action to induce cancer and other adverse health outcomes. Moreover, the relationship between dose and a particular outcome in an individual could take multiple forms depending on genetic background, target tissue, internal dose and other factors besides mechanisms or modes of action: inter-individual variability and susceptibility in response are, in turn, key determinants of the population dose-response curve. New bioanalytical approaches (e.g., transcriptomics, proteomics, and metabolomics) applied in human, animal and in vitro studies could better characterize a wider array of hazard traits and improve the ability to predict the potential carcinogenicity of chemicals. Published by Elsevier B.V

Keywords

Carcinogenicity testing; Carcinogens; CHROMOSOMAL-ABERRATIONS; DISCRIMINATE RODENT CARCINOGENS; Disease; Dna; DOSE-RESPONSE RELATIONSHIPS; EXPOSED HUMAN-SUBJECTS; GENE-EXPRESSION PROFILES; Genotoxicity battery; HUMAN CANCER; Humans; In Vitro; methods; RELATIVE PREDICTIVITY; Risk Assessment; RISK-ASSESSMENT; SACCHAROMYCES-CEREVISIAE; toxicity; VITRO GENOTOXICITY TESTS