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    Evaluation of genotoxic potential of avarol, avarone, and its methoxy and methylamino derivatives in prokaryotic and eukaryotic test models

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    <p>In this study, mutagenic and genotoxic potential of anti-tumor compounds avarol, avarone, and its derivatives 3ā€²-methoxyavarone, 4ā€²-(methylamino)avarone and 3ā€²-(methylamino)avarone was evaluated and compared to cytostatics commonly used in chemotherapy (5-fluorouracil, etoposid, and cisplatin). Mutagenic potential of selected hydroquinone and quinones was assessed in prokaryotic model by the SOS/<i>umuC</i> assay in <i>Salmonella typhimurium</i> TA1535/pSK1002. Genotoxic potential was also assessed in eukaryotic models using comet assay in human fetal lung cell line (MRC-5), human adenocarcinoma epithelial cell line (A549), and in human peripheral blood cells (HPBC). The results indicated that avarol and avarone do not exert mutagenic/genotoxic potential. Among the studied avarone derivatives, mutagenic potential was detected by SOS/<i>umuC</i> test for 3ā€²-(methylamino)avarone, but only after metabolic activation. The results of comet assay indicated that 3ā€²-methoxyavarone and 3ā€²-(methylamino)avarone have a significant impact on the level of DNA damage in the MRC-5 cell line. Genotoxic potential was not observed in A549 cells or HPBC probably due to a different uptake rate for the compounds and lower in metabolism rate within these cells.</p
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