Abstract
This review summarizes the literature describing the molecular mechanisms of arsenic-induced oxidative stress, its relevant biomarkers, and its relation to various diseases, including preventive and therapeutic strategies. Arsenic alters multiple cellular pathways including expression of growth factors, suppression of cell cycle checkpoint proteins, promotion of and resistance to apoptosis, inhibition of DNA repair, alterations in DNA methylation, decreased immunosurveillance, and increased oxidative stress, by disturbing the pro/antioxidant balance. These alterations play prominent roles in disease manifestation, such as carcinogenicity, genotoxicity, diabetes, cardiovascular and nervous systems disorders. The exact molecular and cellular mechanisms involved in arsenic toxicity are rather unrevealed. Arsenic alters cellular glutathione levels either by utilizing this electron donor for the conversion of pentavalent to trivalent arsenicals or directly binding with it or by oxidizing glutathione via arsenic-induced free radical generation. Arsenic forms oxygen-based radicals (OH(bullet), O2(bullet)-) under physiological conditions by directly binding with critical thiols. As a carcinogen, it acts through epigenetic mechanisms rather than as a classical mutagen. The carcinogenic potential of arsenic may be attributed to activation of redox-sensitive transcription factors and other signaling pathways involving nuclear factor (kappa)B, activator protein-1, and p53. Modulation of cellular thiols for protection against reactive oxygen species has been used as a therapeutic strategy against arsenic. N-acetylcysteine, (alpha)-lipoic acid, vitamin E, quercetin, and a few herbal extracts show prophylactic activity against the majority of arsenic-mediated injuries in both in vitro and in vivo models. This review also updates the reader on recent advances in chelation therapy and newer therapeutic strategies suggested to treat arsenic-induced oxidative damage. (copyright) 2011 Elsevier Inc.
Author supplied keywords
- Aloe vera barbadensis
- Aloe vera barbadensis extract
- Centella asiatica
- Centella asiatica extract
- DNA modification
- DNA repair
- Hippophae rhamnoides
- Hippophae rhamnoides extract
- Hydrocotyl asiatica
- Hydrocotyl asiatica extract
- Moringa oleifera
- Moringa oleifera extract
- acetylcysteine
- alpha tocopherol
- antioxidant activity
- apoptosis
- arsenic
- arsenic toxicity
- arsenic trioxide
- ascorbic acid
- atherosclerosis
- carcinogenesis
- cardiovascular disease
- catalase
- cell activity
- cell cycle phase
- cell protection
- chelating agent
- chelation therapy
- chromosome aberration
- curcumin
- endothelial dysfunction
- enzyme activity
- enzyme degradation
- enzyme release
- garlic
- garlic extract
- glutathione peroxidase
- glutathione reductase
- heavy metal poisoning
- human
- immunoglobulin enhancer binding protein
- ischemic heart disease
- kidney disease
- lipid peroxidation
- liver disease
- methylation
- mitochondrion
- neurologic disease
- non insulin dependent diabetes mellitus
- nonhuman
- oxidation reduction potential
- oxidative stress
- oxidized low density lipoprotein
- pathophysiology
- plant extract
- priority journal
- prophylaxis
- protein p53
- protein phosphorylation
- quercetin
- reactive oxygen metabolite
- reduced nicotinamide adenine dinucleotide phosphat
- review
- signal transduction
- superoxide dismutase
- taurine
- thioctic acid
- transcription factor
- transcription factor AP 1
- unclassified drug
- unindexed drug
- unithiol
Cite
CITATION STYLE
S.J.S., F. (2011). Arsenic-induced oxidative stress and its reversibility. Free Radical Biology and Medicine, 51(2), 257–281. Retrieved from http://www.embase.com/search/results?subaction=viewrecord&from=export&id=L51436746
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