The Mycotoxin Fumonisin B1 Alters the Proliferation and the Barrier Function of Porcine Intestinal Epithelial Cells

doi:10.1093/toxsci/kfh006

ToxSci Advance Access originally published online on November 4, 2003

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Toxicological Sciences 77, 165-171 (2004)
Copyright © 2004 by the Society of Toxicology

SYSTEMS TOXICOLOGY

The Mycotoxin Fumonisin B₁ Alters the Proliferation and the Barrier Function of Porcine Intestinal Epithelial Cells

Sandrine Bouhet^*, Edith Hourcade^*, Nicolas Loiseau^*, Asmaa Fikry^*, Stéphanie Martinez^*, Marianna Roselli, Pierre Galtier^*, Elena Mengheri and Isabelle P. Oswald^*^,1

^* Laboratoire de Pharmacologie-Toxicologie, Institut National de Recherche Agronomique, 31931 Toulouse, France; and Istituto Nazionale di Ricerca per gli Alimenti e la Nutrizione, 00178 Roma, Italy

Fumonisin B₁ (FB₁) is a mycotoxin produced by Fusarium verticillioides(formerly F. moniliforme), a fungus that commonly contaminatesmaize. FB₁ causes toxicological effects in laboratory and domesticanimals including pigs. Because the gastrointestinal tract representsthe first barrier met by exogenous food compounds, the purposeof this study was to investigate the effects of FB₁ on IPEC-1,a porcine intestinal epithelial cell line. We first verifiedthat low concentrations of FB₁ did not exert any cytotoxic effecton IPEC-1. Indeed, significant LDH release was only observedfor FB₁ concentrations greater than 50 and 700 µM on proliferatingand nonproliferating cells, respectively. We then demonstratedthat FB₁ inhibits proliferation of IPEC-1. Fluorescence-activatedcell sorting (FACS) analysis of the cell cycle indicated thatFB₁ blocks the proliferation of intestinal cells in the G0/G1phase. Similar results were obtained with LLC-PK1, a renal porcineepithelial cell line, which is considered to be a good modelfor studying FB₁ in vitro effects. We have also assessed theeffects of FB₁ on the integrity of the barrier formed by theintestinal epithelium. We demonstrated that FB₁ decreases thetransepithelial electrical resistance (TEER) of IPEC-1 in atime- and dose-dependent manner. This effect was only noticedafter a long exposure (8–12 days of treatment). FB₁ inducedthe TEER decrease independently of the cell differentiationstage, and this effect was partially reversible. Taken together,our data indicate that FB₁ alters the proliferation and thebarrier function of intestinal cells. These results may haveimplications for humans and animals consuming FB₁-contaminatedfood or feed.

Key Words: fumonisin B₁; intestinal epithelial cells; IPEC-1; swine; barrier function; transepithelial electrical resistance.

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