| Literature DB >> 27143302 |
K Bergstrom1, J Fu1,2, M E V Johansson3, X Liu4, N Gao5, Q Wu1,6, J Song1, J M McDaniel1, S McGee1, W Chen5, J Braun7, G C Hansson3, L Xia1,2,8.
Abstract
Core 1- and 3-derived mucin-type O-glycans are primary components of the mucus layer in the colon. Reduced mucus thickness and impaired O-glycosylation are observed in human ulcerative colitis. However, how both types of O-glycans maintain mucus barrier function in the colon is unclear. We found that C1galt1 expression, which synthesizes core 1 O-glycans, was detected throughout the colon, whereas C3GnT, which controls core 3 O-glycan formation, was most highly expressed in the proximal colon. Consistent with this, mice lacking intestinal core 1-derived O-glycans (IEC C1galt1-/-) developed spontaneous colitis primarily in the distal colon, whereas mice lacking both intestinal core 1- and 3-derived O-glycans (DKO) developed spontaneous colitis in both the distal and proximal colon. DKO mice showed an early onset and more severe colitis than IEC C1galt1-/- mice. Antibiotic treatment restored the mucus layer and attenuated colitis in DKO mice. Mucins from DKO mice were more susceptible to proteolysis than wild-type mucins. This study indicates that core 1- and 3-derived O-glycans collectively contribute to the mucus barrier by protecting it from bacterial protease degradation and suggests new therapeutic targets to promote mucus barrier function in colitis patients.Entities:
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Year: 2016 PMID: 27143302 PMCID: PMC5097036 DOI: 10.1038/mi.2016.45
Source DB: PubMed Journal: Mucosal Immunol ISSN: 1933-0219 Impact factor: 8.701