Literature DB >> 25881551

The deleterious metabolic and genotoxic effects of the bacterial metabolite p-cresol on colonic epithelial cells.

Mireille Andriamihaja1, Annaïg Lan1, Martin Beaumont1, Marc Audebert2, Ximena Wong3, Kana Yamada1, Yulong Yin4, Daniel Tomé1, Catalina Carrasco-Pozo3, Martin Gotteland5, Xiangfeng Kong4, François Blachier6.   

Abstract

p-Cresol that is produced by the intestinal microbiota from the amino acid tyrosine is found at millimolar concentrations in the human feces. The effects of this metabolite on colonic epithelial cells were tested in this study. Using the human colonic epithelial HT-29 Glc(-/+) cell line, we found that 0.8mM p-cresol inhibits cell proliferation, an effect concomitant with an accumulation of the cells in the S phase and with a slight increase of cell detachment without necrotic effect. At this concentration, p-cresol inhibited oxygen consumption in HT-29 Glc(-/+) cells. In rat normal colonocytes, p-cresol also inhibited respiration. Pretreatment of HT-29 Glc(-/+) cells with 0.8mM p-cresol for 1 day resulted in an increase of the state 3 oxygen consumption and of the cell maximal respiratory capacity with concomitant increased anion superoxide production. At higher concentrations (1.6 and 3.2mM), p-cresol showed similar effects but additionally increased after 1 day the proton leak through the inner mitochondrial membrane, decreasing the mitochondrial bioenergetic activity. At these concentrations, p-cresol was found to be genotoxic toward HT-29 Glc(-/+) and also LS-174T intestinal cells. Lastly, a decreased ATP intracellular content was observed after 3 days treatment. p-Cresol at 0.8mM concentration inhibits colonocyte respiration and proliferation. In response, cells can mobilize their "respiratory reserve." At higher concentrations, p-cresol pretreatment uncouples cell respiration and ATP synthesis, increases DNA damage, and finally decreases the ATP cell content. Thus, we have identified p-cresol as a metabolic troublemaker and as a genotoxic agent toward colonocytes.
Copyright © 2015 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Anion superoxide production; Cell proliferation; Genotoxicity; Intestinal microbiota; Large intestine; Mitochondrial oxygen consumption

Mesh:

Substances:

Year:  2015        PMID: 25881551     DOI: 10.1016/j.freeradbiomed.2015.04.004

Source DB:  PubMed          Journal:  Free Radic Biol Med        ISSN: 0891-5849            Impact factor:   7.376


  36 in total

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Journal:  Inflamm Bowel Dis       Date:  2019-04-11       Impact factor: 5.325

Review 3.  Effects of the L-tyrosine-derived bacterial metabolite p-cresol on colonic and peripheral cells.

Authors:  F Blachier; M Andriamihaja
Journal:  Amino Acids       Date:  2021-09-01       Impact factor: 3.520

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Journal:  Nat Microbiol       Date:  2016-06-27       Impact factor: 17.745

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Review 6.  Gut microbiota-derived metabolites in CRC progression and causation.

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8.  Dual effects of the tryptophan-derived bacterial metabolite indole on colonic epithelial cell metabolism and physiology: comparison with its co-metabolite indoxyl sulfate.

Authors:  Lucie Armand; Masou Fofana; Kristell Couturier-Becavin; Mireille Andriamihaja; François Blachier
Journal:  Amino Acids       Date:  2022-02-02       Impact factor: 3.520

Review 9.  Interference of dietary polyphenols with potentially toxic amino acid metabolites derived from the colonic microbiota.

Authors:  Naschla Gasaly; Martin Gotteland
Journal:  Amino Acids       Date:  2021-07-07       Impact factor: 3.520

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Authors:  Tomas Clive Barker-Tejeda; Raphaelle Bazire; David Obeso; Leticia Mera-Berriatua; Domenico Rosace; Sonia Vazquez-Cortes; Tania Ramos; Maria Del Pilar Rico; Tomás Chivato; Coral Barbas; Alma Villaseñor; Maria M Escribese; Montserrat Fernández-Rivas; Carlos Blanco; Domingo Barber
Journal:  Allergy       Date:  2020-09-22       Impact factor: 13.146

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