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Lack of genoprotective effect of phytosterols and conjugated linoleic acids on Caco-2 cells
Authors:Trevor J. Daly,S. Aisling AherneTom P. O&rsquo  Connor,Nora M. O&rsquo  Brien
Affiliation:Department of Food and Nutritional Sciences, University College Cork, Western Road, Cork, Ireland
Abstract:Much interest has focused on the cholesterol-lowering effects of phytosterols (plant sterols) but limited data suggests they may also possess anti-carcinogenic activity. Conjugated linoleic acids (CLA), sourced from meat and dairy products of ruminant animals, has also received considerable attention as a potential anti-cancer agent. Therefore, the aims of this project were to (i) examine the effects of phytosterols and CLA on the viability and growth of human intestinal Caco-2 cells and (ii) determine their potential genoprotective (comet assay), COX-2 modulatory (ELISA) and apoptotic (Hoechst staining) activities. Caco-2 cells were supplemented with the phytosterols campesterol, β-sitosterol, or β-sitostanol, or a CLA mixture, or individual CLA isomers (c10t12-CLA, t9t11-CLA) for 48 h. The three phytosterols, at the highest levels tested, were found to reduce both the viability and growth of Caco-2 cells while CLA exhibited isomer-specific effects. None of the phytosterols protected against DNA damage. At a concentration of 25 μM, both c10t12-CLA and t9t11-CLA enhanced (< 0.05) oxidant-induced, but not mutagen-induced, DNA damage. Neither the phytosterols nor CLA induced apoptosis or modulated COX-2 production. In conclusion, campesterol, β-sitosterol, β-sitostanol, c10t12-CLA, and t9t11-CLA were not toxic to Caco-2 cells, at the lower levels tested, and did not exhibit potential anti-carcinogenic activity.
Keywords:CLA, conjugated linoleic acid   COX-2, cyclooxygenase-2   H2O2, hydrogen peroxide   IL-1β, interleukin-1β   MNNG, 1-methyl,3-nitro-1-nitrosoguanidine
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