Isoflavonoids and lignans have different potentials to modulate oxidative genetic damage in human colon cells

doi:10.1093/carcin/21.6.1247

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Carcinogenesis, Vol. 21, No. 6, 1247-1252, June 2000
© 2000 Oxford University Press

Carcinogenesis

Isoflavonoids and lignans have different potentials to modulate oxidative genetic damage in human colon cells

Beatrice L. Pool-Zobel⁵, Herman Adlercreutz¹, Michael Glei, Ute M. Liegibel, Julie Sittlingon², Ian Rowland², Kristiina Wähälä⁴ and Gerhard Rechkemmer³

Department of Nutritional Toxicology, Institute for Nutrition, Friedrich Schiller University, Dornburger Straße 25, 07743 Jena, Germany,
¹ Institute for Preventive Medicine, Nutrition and Cancer, Folkhälsan Research Center and Department of Clinical Chemistry, University of Helsinki, PO Box 60, Mannerheimintie 97, 00014 Helsinki, Finland,
² Northern Ireland Centre for Diet and Health, University of Ulster, Coleraine BT521AA, UK,
³ Institute for Nutritional Physiology, Federal Research Centre for Nutrition, Haid-und-Neu-Straße 9, 76131 Karlsruhe, Germany and
⁴ Organic Chemistry Laboratory, Department of Chemistry, University of Helsinki, PO Box 55, 00014 Helsinki, Finland

Polyphenolic compounds, including isoflavonoids and lignans,have been suggested to be chemopreventive on account of antioxidativeproperties. In this context it is of importance to have knowledgeof their ability to reduce oxidative stress within target cellsof tumorigenesis. Therefore, we investigated isoflavonoids andlignans for modulation of oxidative genetic damage in mammaliancells. H₂O₂-induced damage as well as endogenous DNA strandbreaks and oxidized bases were determined after 30 min incubationof human colon cells with polyphenols using various modificationsof the microgel electrophoresis assay (Comet assay). Enterolactone,a mammalian metabolite of plant lignans, was additionally investigatedfor modulation of intracellular oxidative stress in NIH 3T3cells using laser scanning microscopy. In vivo effects of ryecrispbread (a source of lignans) were investigated in 12 humanvolunteers by determining genetic damage in lymphocytes andantioxidant activity in plasma (FRAP assay). Genistein inducedDNA breaks in the human tumour cell line HT29 clone 19A (12.5–100µM). The polyphenols (100 µM) did not reduce damageinduced by 150 µM H₂O₂, indicating that they lacked antioxidativepotential. At this concentration enterolactone also had no effecton intracellular oxidative stress induced by 31.25 and 125 µMH₂O₂. In contrast, enterolactone, dihydrogenistein and formononetinreduced endogenous oxidative DNA damage at 100 µM. Dailyingestion of nine slices (76.5 g/day) of rye crispbread perday (containing 41.8 and 33.0 µg/100 g dry weight secoisolariciresinoland matairesinol, respectively) for 2 weeks did not significantlyreduce genetic damage in blood lymphocytes, nor was there amodulation of plasma antioxidant capacity. The moderate effectsof high concentrations of the tested compounds on endogenousoxidative DNA damage and failure to prevent H₂O₂- induced damageare indicative of only marginal protective potential by antioxidantmechanisms. The genotoxic effects of genistein deserve furtherinvestigation.

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