Journal
INFLAMMATORY BOWEL DISEASES
Volume 14, Issue 10, Pages 1366-1372Publisher
OXFORD UNIV PRESS INC
DOI: 10.1002/ibd.20499
Keywords
galectins; epithelial cells; apoptosis; inflammatory bowel diseases; proliferation
Categories
Funding
- Eli and Edythe Broad Foundation
- Forechungsforderung of the Charite
- Universitatsmedizin Berlin
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Background: Inflammatory bowel diseases (IBDs) are characterized by various degrees of mucosal surface damage and subsequent impairment of the intestinal barrier function. Resealing of epithelial barrier harrier requires intestinal cell migration and proliferation. Galectins are increasingly recognized as novel regulators of inflammation. Thus, we aimed to explore the effect of galectin-2 (Gal-2) and Gal-4 on epithelial cell function and Wound healing. Methods: Binding of Gal-2 and Gal-4 was determined by flow cytometric analysis and binding sites by SDS-PAGE electrophoresis. Cell migration by Gal-1. -2. and -4 was determined by a would-healing assay. Cell cycle analysis stud detection of apoptosis were determined by flow cytometric analysis. Results: Gal-2 and Gal-4 hind to epithelial cells at the E-cadherin/beta-catenin complex. Both galectins significantly enhanced intestinal epithelial cell restitution in vitro. This enhancement of epithelial cell restitution was TGF-beta-independent. In contrast. Gal-1 decreased epithelial cell migration TGF-beta dependently. By performing cell cycle analysis. we show that Gal-2 and Gal-4 increased cyclin B1 expression and consequently cell cycle progression. while Gal-1 inhibited cell cycling. Determining the influence of Gal-2 and Gal-4 on epithelial cell apoptosis, we showed no induction of apoptosis. Whereas Gal-1 significantly induced apoptosis of epithelial cells caspase-independently. Conclusions: Gal-2 and Gal-4 bind to intestinal epithelial cells and promote their restitution. Thus. our study provides for the first time evidence that these galectins play a significant role in intestinal wound-healing processes and might exert beneficial effects in diseases characterized by epithelial harrier disruption like IBDs. (Inflamm Bowel Dis 2008; 14:1366-1372)
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