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Journal ArticleDOI

A comparison of the in vitro genotoxicity of tri- and hexavalent chromium.

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TLDR
The comet assay did not indicate the involvement of oxidative mechanisms in the DNA-damaging activity of trivalent chromium and it is speculated that its binding to cellular ligands may play a role in its genotoxicity.
Abstract
Chromium can be found in the environment in two main valence states: hexavalent (Cr(VI)) and trivalent (Cr(III)). Cr(VI) salts are well known human carcinogens, but the results from in vitro studies are often conflicting. Cr(VI) primarily enters the cells and undergoes metabolic reduction; however, the ultimate product of this reduction, Cr(III) predominates within the cell. In the present work, we compared the effects of tri- and hexavalent chromium on the DNA damage and repair in human lymphocytes using the alkaline single cell gel electrophoresis (comet assay). Potassium dichromate induced DNA damage in the lymphocytes, measured as the increase in comet tail moment. The effect was dose-dependent. Treated cells were able to recover within a 120-min incubation. Cr(III) caused greater DNA migration than Cr(VI). The lymphocytes did not show measurable DNA repair. Vitamin C at 50 μM reduced the extent of DNA migration. This was either due to a decrease in DNA strand breaks and/or alkali labile sites induced by Cr(VI) or to the formation of DNA crosslinks by Cr(VI) in the presence of vitamin C. Vitamin C, however, did not modify the effects of Cr(III). Catalase, an enzyme inactivating hydrogen peroxide, decreased the extent of DNA damage induced by Cr(VI) but not the one induced by Cr(III). Lymphocytes exposed to Cr(VI) and treated with endonuclease III, which recognizes oxidized pyrimidines, displayed greater extent of DNA damage than those not treated with the enzyme. Such an effect was not observed when Cr(III) was tested. The results obtained suggest that reactive oxygen species and hydrogen peroxide may be involved in the formation of DNA lesions by hexavalent chromium. The comet assay did not indicate the involvement of oxidative mechanisms in the DNA-damaging activity of trivalent chromium and we speculate that its binding to cellular ligands may play a role in its genotoxicity.

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Citations
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Journal ArticleDOI

A new look at biomedical Ti-based shape memory alloys

TL;DR: The metals Ti, Au, Sn, Ta, Nb, Ru and Zr are identified as candidates for the production of thoroughly biocompatible SMAs - alloys that exhibit the full range of shape memory abilities yet are also free of any undesirable side effects.
Journal ArticleDOI

Genotoxicity and mutagenicity of water contaminated with tannery effluents, as evaluated by the micronucleus test and comet assay using the fish Oreochromis niloticus and chromosome aberrations in onion root-tips

TL;DR: Water samples from three sites in the Corrego dos Bagres stream in the Franca municipality of the Brazilian state of Sao Paulo were subjected to the comet assay and micronucleus test using erythrocytes from the fish Oreochromis niloticus, supporting the hypothesis that chromium residues can be genotoxic.
BookDOI

Physiology and biochemistry of metal toxicity and tolerance in plants

TL;DR: In this paper, Mysliwa-Kurdziel et al. studied the effect of heavy metal on the light phase of photosynthesis in plants and found that heavy metal influence on photosynthetic pigments was significant.
Journal ArticleDOI

Effects of chromium on the immune system

TL;DR: Chromium is of significant importance in altering the immune response by immunostimulatory or immunosuppressive processes as shown by its effects on T and B lymphocytes, macrophages, cytokine production and theimmune response that may induce hypersensitivity reactions.
Journal ArticleDOI

Trivalent Chromium: Assessing the Genotoxic Risk of an Essential Trace Element and Widely Used Human and Animal Nutritional Supplement

TL;DR: In this paper, the authors reviewed the literature on genotoxic effects of Trivalent chromium [Cr(III) compounds to determine whether recent findings provided a sufficient weight of evidence to modify the conclusions about the safety of this dietary supplement reached in the several comprehensive reviews conducted during the period 1990-2004.
References
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Journal ArticleDOI

A simple technique for quantitation of low levels of DNA damage in individual cells

TL;DR: Human lymphocytes were exposed to X-irradiation or treated with H2O2 and the extent of DNA migration was measured using a single-cell microgel electrophoresis technique under alkaline conditions and this technique appears to be sensitive and useful for detecting damage and repair in single cells.
Journal ArticleDOI

Oxidative mechanisms in the toxicity of metal ions

TL;DR: Some mechanisms associated with the toxicities of metal ions are very similar to the effects produced by many organic xenobiotics, related to differences in solubilities, absorbability, transport, chemical reactions, and the complexes that are formed within the body.
Journal ArticleDOI

Direct enzymic detection of endogenous oxidative base damage in human lymphocyte DNA

TL;DR: Using an endonuclease specific for oxidized pyrimidines, in conjunction with the highly sensitive method of single cell gel electrophoresis, significant oxidative damage is detected in untreated, freshly isolated lymphocytes from normal, healthy individuals.
Journal Article

Antioxidant Supplementation Decreases Oxidative DNA Damage in Human Lymphocytes

TL;DR: The hypothesis that fruit and vegetables exert a cancer-protective effect via a decrease in oxidative damage to DNA is supported via a reduction in endogenous oxidative base damage in the lymphocyte DNA of both smokers and nonsmokers.
Journal ArticleDOI

Genotoxicity of chromium compounds. A review.

TL;DR: This article reviews approximately 700 results reported in the literature with 32 chromium compounds assayed in 130 short-term tests, using different targets and/or genetic end-points, to provide useful information for predicting and interpreting the peculiar patterns of Cr(VI) carcinogenicity.
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