Anti-Inflammatory Effect of <i>Lactobacillus casei</i> on <i>Shigella</i> -Infected Human Intestinal Epithelial Cells

Meng-Tsung Tien(Inserm), Stephen E. Girardin(Inserm), Béatrice Regnault(Gene Therapy Laboratory), Lionel Le Bourhis(Institut Pasteur), Marie‐Agnès Dillies(Gene Therapy Laboratory), Jean-Yves Coppée(Gene Therapy Laboratory), Raphaëlle Bourdet‐Sicard(Danone (France)), Philippe Sansonetti(Inserm), Thierry Pédron(Inserm)
The Journal of Immunology
January 1, 2006
Cited by 314

Abstract

Shigella invades the human intestinal mucosa, thus causing bacillary dysentery, an acute recto-colitis responsible for lethal complications, mostly in infants and toddlers. Conversely, commensal bacteria live in a mutualistic relationship with the intestinal mucosa that is characterized by homeostatic control of innate responses, thereby contributing to tolerance to the flora. Cross-talk established between commensals and the intestinal epithelium mediate this active process, the mechanisms of which remain largely uncharacterized. Probiotics such as Lactobacillus casei belong to a subclass of these commensals that modulate mucosal innate responses and possibly display anti-inflammatory properties. We analyzed whether L. casei could attenuate the pro-inflammatory signaling induced by Shigella flexneri after invasion of the epithelial lining. Cultured epithelial cells were infected with L. casei, followed by a challenge with S. flexneri. Using macroarray DNA chips, we observed that L. casei down-regulated the transcription of a number of genes encoding pro-inflammatory effectors such as cytokines and chemokines and adherence molecules induced by invasive S. flexneri. This resulted in an anti-inflammatory effect that appeared mediated by the inhibition of the NF-kappaB pathway, particularly through stabilization of I-kappaBalpha. In a time-course experiment using GeneChip hybridization analysis, the expression of many genes involved in ubiquitination and proteasome processes were modulated during L. casei treatment. Thus, L. casei has developed a sophisticated means to maintain intestinal homeostasis through a process that involves manipulation of the ubiquitin/proteasome pathway upstream of I-kappaBalpha.


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