Table I.
Associations of representative diseases and disease models with intestinal barrier loss
| Inflammatory Bowel Disease | Celiac Disease | Graft vs. Host Disease | Type I Diabetes Mellitus | |
|---|---|---|---|---|
| Structural alterations | ||||
| Pore pathway | Increased claudin-2 expression45,47,60,85 | Increased claudin-2 expression119,120,162 | Increased claudin-2 expression139 | |
| Leak pathway | Reduced occludin expression47; increased MLCK expression and activity58,60,86, MLCK inactivation reduces severity60 | Reduced occludin expression104,119 | Reduced occludin expression163 | |
| Unrestricted pathway | Ulceration, epithelial apoptosis60,135,164 | Epithelial apoptosis165 | ||
| Functional alterations | ||||
| Pore and/or leak pathways | Increased lactulose:mannitol ratio and PEG-400 permeability in disease,82,83,166–168 impending relapse,87–89,169 and some healthy relatives92,93,170 | Increased lactulose:mannitol ratio in disease82,96,171 | Increased sucralose permeability137 | Increased lactulose:mannitol ratio141,142,172 |
| Leak and/or unrestricted pathways | Increased 4kD dextran and Evan’s blue flux in DSS-induced colitis135,173,174 | Pathogenic bacterial that increase intestinal permeability accelerate disease175 | Development of experimental minor mismatch disease requires intestinal damage 139, the extent of barrier loss induced by pre- transplant conditioning correlates with disease severity176 | |