Tumor necrosis factor regulates intestinal epithelial cell migration by receptor-dependent mechanisms

doi:10.1152/ajpcell.00309.2002

Tumor necrosis factor regulates intestinal epithelial cell migration by receptor-dependent mechanisms

Julissa Corredor¹, Fang Yan¹, Christopher C. Shen¹, Wei Tong¹, Sutha K. John¹, Guinn Wilson¹, Robert Whitehead²^,³, and D. Brent Polk¹^,²

Departments of ¹ Pediatrics, ² Cell and Developmental Biology, and ³ Medicine, Division of Gastroenterology and Nutrition, Vanderbilt University School of Medicine, Nashville, Tennessee 37232-2576

Altered mucosal integrity and increased cytokine production, including tumor necrosis factor (TNF), are the hallmarks of inflammatorybowel disease (IBD). In this study, we addressed the role of TNFreceptors (TNFR) on intestinal epithelial cell migration in anin vitro wound closure model. With mouse TNFR1 or TNFR2 knockoutintestinal epithelial cells, gene transfection, and pharmacologicalinhibitors, we show a concentration-dependent receptor-mediatedregulation of intestinal cell migration by TNF. A physiologicalTNF level (1 ng/ml) enhances migration through TNFR2, whereasa pathological level (100 ng/ml) inhibits wound closure throughTNFR1. Increased rate of wound closure by TNFR2 or inhibitionby TNFR1 cannot be explained by either increased proliferationor apoptosis, respectively. Furthermore, inhibiting Src tyrosinekinase decreases TNF-induced focal adhesion kinase (FAK) tyrosinephosphorylation and cellular migration. We therefore concludethat TNFR2 activates a novel Src-regulated pathway involving FAKtyrosine phosphorylation that enhances migration of intestinalepithelialcells.

intestinal restitution; Src; focal adhesion kinase

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