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Differential Effects of Falcarinol and Related Aliphatic C(17)-Polyacetylenes on Intestinal Cell Proliferation

Quantitative major polyacetylenes of carrots (falcarinol and falcarindiol) and American ginseng roots (falcarinol and panaxydol) were isolated and tested in human intestinal epithelial cells of normal (FHs 74 Int.) and cancer (Caco-2) origin. A hormesis effect was seen for all isolated polyacetylene...

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Autores principales: Purup, Stig, Larsen, Eric, Christensen, Lars P.
Formato: Texto
Lenguaje:English
Publicado: American Chemical Society 2009
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2745230/
https://www.ncbi.nlm.nih.gov/pubmed/19694436
http://dx.doi.org/10.1021/jf901503a
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author Purup, Stig
Larsen, Eric
Christensen, Lars P.
author_facet Purup, Stig
Larsen, Eric
Christensen, Lars P.
author_sort Purup, Stig
collection PubMed
description Quantitative major polyacetylenes of carrots (falcarinol and falcarindiol) and American ginseng roots (falcarinol and panaxydol) were isolated and tested in human intestinal epithelial cells of normal (FHs 74 Int.) and cancer (Caco-2) origin. A hormesis effect was seen for all isolated polyacetylenes when added to Caco-2 cells in concentrations ranging from 1 ng/mL to 20 μg/mL. The relative inhibitory potency was falcarinol > panaxydol > falcarindiol. No hormesis effect was observed when adding the polyacetylenes to FHs 74 Int. cells. Instead, an inhibitory growth response was observed above 1 μg/mL. The relative inhibitory potency was panaxydol > falcarinol > falcarindiol. Maximal inhibition at 20 μg/mL corresponded to approximately 95% and 80% inhibition of cell proliferation in normal and cancer cells, respectively. Combinations of falcarinol and falcarindiol added to normal and cancer cells showed a synergistic response for the inhibition of cell growth. Furthermore, the oxidized form of falcarinol, falcarinon, showed a significantly less growth inhibitory effect in intestinal cells of both normal and cancer origin; hence, a hydroxyl group at C-3 may be important for activity of falcarinol-type polyacetylenes. Extracts of carrots, containing different amounts of falcarinol, falcarindiol, and falcarindiol 3-acetate had significant inhibitory effects on both normal and cancer cell proliferation. In cancer cells, the extract containing the highest concentration of falcarinol tended to have the highest growth inhibitory effect, in accordance with a higher potency of falcarinol than falcarindiol. The present study demonstrates that aliphatic C(17)-polyacetylenes are potential anticancer principles of carrots and related vegetables and that synergistic interaction between bioactive polyacetylenes may be important for their bioactivity.
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spelling pubmed-27452302009-09-16 Differential Effects of Falcarinol and Related Aliphatic C(17)-Polyacetylenes on Intestinal Cell Proliferation Purup, Stig Larsen, Eric Christensen, Lars P. J Agric Food Chem Quantitative major polyacetylenes of carrots (falcarinol and falcarindiol) and American ginseng roots (falcarinol and panaxydol) were isolated and tested in human intestinal epithelial cells of normal (FHs 74 Int.) and cancer (Caco-2) origin. A hormesis effect was seen for all isolated polyacetylenes when added to Caco-2 cells in concentrations ranging from 1 ng/mL to 20 μg/mL. The relative inhibitory potency was falcarinol > panaxydol > falcarindiol. No hormesis effect was observed when adding the polyacetylenes to FHs 74 Int. cells. Instead, an inhibitory growth response was observed above 1 μg/mL. The relative inhibitory potency was panaxydol > falcarinol > falcarindiol. Maximal inhibition at 20 μg/mL corresponded to approximately 95% and 80% inhibition of cell proliferation in normal and cancer cells, respectively. Combinations of falcarinol and falcarindiol added to normal and cancer cells showed a synergistic response for the inhibition of cell growth. Furthermore, the oxidized form of falcarinol, falcarinon, showed a significantly less growth inhibitory effect in intestinal cells of both normal and cancer origin; hence, a hydroxyl group at C-3 may be important for activity of falcarinol-type polyacetylenes. Extracts of carrots, containing different amounts of falcarinol, falcarindiol, and falcarindiol 3-acetate had significant inhibitory effects on both normal and cancer cell proliferation. In cancer cells, the extract containing the highest concentration of falcarinol tended to have the highest growth inhibitory effect, in accordance with a higher potency of falcarinol than falcarindiol. The present study demonstrates that aliphatic C(17)-polyacetylenes are potential anticancer principles of carrots and related vegetables and that synergistic interaction between bioactive polyacetylenes may be important for their bioactivity. American Chemical Society 2009-08-20 2009-09-23 /pmc/articles/PMC2745230/ /pubmed/19694436 http://dx.doi.org/10.1021/jf901503a Text en Copyright © 2009 American Chemical Society http://pubs.acs.org This is an open-access article distributed under the ACS AuthorChoice Terms & Conditions. Any use of this article, must conform to the terms of that license which are available at http://pubs.acs.org.
spellingShingle Purup, Stig
Larsen, Eric
Christensen, Lars P.
Differential Effects of Falcarinol and Related Aliphatic C(17)-Polyacetylenes on Intestinal Cell Proliferation
title Differential Effects of Falcarinol and Related Aliphatic C(17)-Polyacetylenes on Intestinal Cell Proliferation
title_full Differential Effects of Falcarinol and Related Aliphatic C(17)-Polyacetylenes on Intestinal Cell Proliferation
title_fullStr Differential Effects of Falcarinol and Related Aliphatic C(17)-Polyacetylenes on Intestinal Cell Proliferation
title_full_unstemmed Differential Effects of Falcarinol and Related Aliphatic C(17)-Polyacetylenes on Intestinal Cell Proliferation
title_short Differential Effects of Falcarinol and Related Aliphatic C(17)-Polyacetylenes on Intestinal Cell Proliferation
title_sort differential effects of falcarinol and related aliphatic c(17)-polyacetylenes on intestinal cell proliferation
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2745230/
https://www.ncbi.nlm.nih.gov/pubmed/19694436
http://dx.doi.org/10.1021/jf901503a
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