In vitro investigations into the interaction of β-carotene with DNA: Evidence for the role of carbon-centered free radicals

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Abstract

Supplementation by β-carotene has unexpectedly appeared to increase lung cancer risk among smokers. In order to explain this it has been suggested that at high serum levels of β-carotene, prooxidant characteristics of β-carotene may become manifest, yielding reactive oxygen species (ROS) and inducing oxidative DNA damage. It has further been hypothesized that cigarette smoke carcinogens such as benzo[a]pyrene (B[a]P) and/or B[a]P metabolites, may directly react with β -carotene. Furthermore, β-carotene oxidation products may have a role in the bioactivation of B[a]P analogous to the peroxide shunt pathway of cytochrome P450 supported by cumene hydroperoxide. The aim of this study was to assess the effects of β-carotene on the formation of B[a]P-DNA adducts and oxidative DNA damage in vitro in isolated DNA, applying as metabolizing systems rat liver and lung metabolizing fractions and lung metabolizing fractions from smoking and non-smoking humans. We established that β-carotene in the presence of various metabolizing systems was unable to induce oxidative DNA damage (8-oxo-dG , although β-carotene is capable of generating ROS spontaneously in the absence of metabolizing fractions. We also could not find an effect of β-carotene on DNA adduct formation induced by B[a]P upon metabolic activation. We could, however, provide evidence of the occurrence of a carbon-centered β-carotene radical which was found to be able to interact with B[a]P and to intercalate in DNA. © Oxford University Press 2004; all rights reserved.

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Kleinjans, J. C. S., van Herwijnen, M. H. M., van Maanen, J. M. S., Maas, L. M., de Kok, T. M. C. M., Moonen, H. J. J., & Briedé, J. J. (2004, July). In vitro investigations into the interaction of β-carotene with DNA: Evidence for the role of carbon-centered free radicals. Carcinogenesis. https://doi.org/10.1093/carcin/bgh125

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