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HERO ID
628058
Reference Type
Journal Article
Subtype
Review
Title
Arsenic and cardiovascular disease
Author(s)
States, JC; Srivastava, S; Chen, Y; Barchowsky, A
Year
2009
Is Peer Reviewed?
1
Journal
Toxicological Sciences
ISSN:
1096-6080
EISSN:
1096-0929
Volume
107
Issue
2
Page Numbers
312-323
Language
English
PMID
19015167
DOI
10.1093/toxsci/kfn236
Web of Science Id
WOS:000262723000003
Abstract
Chronic arsenic exposure is a worldwide health problem. Although arsenic-induced cancer has been widely studied, comparatively little attention has been paid to arsenic-induced vascular disease. Epidemiological studies have shown that chronic arsenic exposure is associated with increased morbidity and mortality from cardiovascular disease. In addition, studies suggest that susceptibility to arsenic-induced vascular disease may be modified by nutritional factors in addition to genetic factors. Recently, animal models for arsenic-induced atherosclerosis and liver sinusoidal endothelial cell dysfunction have been developed. Initial studies in these models show that arsenic exposure accelerates and exacerbates atherosclerosis in apolipoprotein E-knockout mice. Microarray studies of liver mRNA and micro-RNA abundance in mice exposed in utero suggest that a permanent state of stress is induced by the arsenic exposure. Furthermore, the livers of the arsenic-exposed mice have activated pathways involved in immune responses suggesting a pro-hyperinflammatory state. Arsenic exposure of mice after weaning shows a clear dose-response in the extent of disease exacerbation. In addition, increased inflammation in arterial wall is evident. In response to arsenic-stimulated oxidative signaling, liver sinusoidal endothelium differentiates into a continuous endothelium that limits nutrient exchange and waste elimination. Data suggest that nicotinamide adenine dinucleotide phosphate oxidase-derived superoxide or its derivatives are essential second messengers in the signaling pathway for arsenic-stimulated vessel remodeling. The recent findings provide future directions for research into the cardiovascular effects of arsenic exposure.
Keywords
arsenic; inflammation; oxidative signaling; vascular disease; nutrition; microarray
Tags
IRIS
•
Arsenic (Inorganic)
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Arsenic MOA
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Cardiovascular disease
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Arsenic Susceptibility
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Cardiovascular disease
1. Susceptibility Literature Screening
Supplemental Search
2. Excluded
MOA/Mechanistic
3. References Identified During Review
Life Stages Citation Mapping
Top 5%
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Inorganic Arsenic (7440-38-2) [Final 2025]
1. Initial Lit Search
PubMed
WOS
ToxNet
3. Initial Filter through Oct 2015
Reviews
7. Other Studies through Oct 2015
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