Mechanism of chromium(VI) carcinogenesis
- 1 July 1989
- journal article
- review article
- Published by Springer Nature in Biological Trace Element Research
- Vol. 21 (1) , 405-411
- https://doi.org/10.1007/bf02917282
Abstract
Since chromium(VI) is unreactive toward DNA under physiological conditions in vitro, the ability of carcinogenic chromium(VI) compounds to damage DNA depends on the presence of cellular redox components that reduce chromium(VI) to reactive species capable of interacting with DNA. We have examined the role of glutathione and hydrogen peroxide in chromium(VI)-induced DNA damage in vitro. Upon reaction with chromium(VI), glutathione produced chromium(V) and glutathione thiyl radical reactive intermediates, whereas hydrogen peroxide produced chromium(V) and hydroxyl radical. Reaction of DNA with chromium(VI) in the presence of glutathione resulted in binding of chromium and glutathione to DNA with little or no DNA strand breakage. Reaction of DNA with chromium(VI) in the presence of hydrogen peroxide produced the 8-hydroxydeoxy-guanosine adduct and extensive DNA strand breakage in the absence of significant Cr-DNA adduct formation. These results suggest that the nature of chromium(VI)-induced DNA damage will be strongly dependent on reactive intermediates such as chromium(V), glutathione thiyl radical, and hydroxyl radical, produced by cellular components active in chromium(VI) metabolism. In order to assess the ability of chromium(VI)-induced DNA damage to affect the normal template function of DNA, we investigated the effects of chromium(VI) on steady-state mRNA levels of various genes in chick embryo liver in vivo, and compared the effects to the levels of DNA damage observed. Chromium(VI) induced DNA-protein and DNA interstrand cross-links in chick embryo liver in vivo and suppressed the induction of 5-aminolevulinic acid synthase and cytochrome P-450 mRNA expression by porphyrinogenic drugs. In contrast, chromium(VI) increased the basal levels of expression of these two inducible genes, but had little or no effect on the expression of the constitutive albumin, β-actin, and conalbumin genes. Comparison of the time course of formation and repair of DNA damage with that of changes in gene expression suggests that chromium(VI) may form a mono-adduct prior to formation of DNA cross-links, and that chromium(VI)-induced DNA lesions may target certain classes of genes and lead to changes in their expression.Keywords
This publication has 17 references indexed in Scilit:
- Metabolism of the carcinogen chromate by cellular constituentsPublished by Springer Nature ,2007
- Effects of vitamin E, vitamin B2 and selenite on DNA single strand breaks induced by sodium chromate (VI)Cancer Letters, 1987
- Relatively long-lived chromium(V) species are produced by the action of glutathione on carcinogenic chromium(VI)Journal of Inorganic Biochemistry, 1986
- Inhibition of steroid-inducible tyrosine aminotransferase gene expression by N-methyl-N'-nitro-N-nitrosoguanidine in a rat hepatoma cell lineCarcinogenesis: Integrative Cancer Research, 1986
- Chromium (VI)-induced DNA damage in chick embryo liver and blood cells in vivoCarcinogenesis: Integrative Cancer Research, 1986
- Changes in hepatic levels of tyrosine aminotransferase messenger RNA during chemical hepatocarcinogenesisCancer Letters, 1984
- Effects of carcinogens on hormonal regulation of gene expression in primary cultures of adult rat hepatocytesCarcinogenesis: Integrative Cancer Research, 1983
- The carcinogen chromate causes DNA damage and inhibits drug-mediated induction of porphyrin accumulation and glucuronidation in chick embryo hepatocytesCarcinogenesis: Integrative Cancer Research, 1983
- The role of metals in carcinogenesis: biochemistry and metabolism.Environmental Health Perspectives, 1981
- Aflatoxin inhibition of glucocorticoid binding capacity of rat liver nucleiBiochimica et Biophysica Acta (BBA) - General Subjects, 1976