Abstract

Background & AimsOne of the features of ulcerative colitis (UC) is a defect in the protective mucus layer. This has been attributed to a reduced number of goblet cells (GCs). However, it is not known whether abnormal GC mucus secretion also contributes to the reduced mucus layer. Our aims were to investigate whether GC secretion was abnormal in UC and exists as a long-term effect of chronic inflammation.MethodsColonoids were established from intestinal stem cells of healthy subjects (HS) and patients with UC. Colonoids were maintained as undifferentiated (UD) or induced to differentiate (DF) and studied as three-dimensional or monolayers on Transwell filters. Total RNA was extracted for quantitative real-time polymerase chain reaction analysis. Carbachol and prostaglandin E2 mediated mucin stimulation was examined by MUC2 IF/confocal microscopy and transmission electron microscopy.ResultsColonoids from UC patients can be propagated over many passages; however, they exhibit a reduced rate of growth and transepithelial electrical resistance compared with HS. Differentiated UC colonoid monolayers form a thin and non-continuous mucus layer. UC colonoids have increased expression of secretory lineage markers ATOH1 and SPDEF, along with MUC2 positive GCs, but failed to secrete mucin in response to the cholinergic agonist carbachol and prostaglandin E2, which caused increased secretion in HS. Exposure to tumor necrosis factor α (5 days) reduced the number of GCs, with a greater percentage decrease in UC colonoids compared with HS.ConclusionsChronic inflammation in UC causes long-term changes in GCs, leading to abnormal mucus secretion. This continued defect in GC mucus secretion may contribute to the recurrence in UC.

Highlights

  • BACKGROUND & AIMSOne of the features of ulcerative colitis (UC) is a defect in the protective mucus layer

  • Colonoids from UC patients can be propagated over many passages; they exhibit a reduced rate of growth and transepithelial electrical resistance compared with healthy subjects (HS)

  • Mucus layer defects contribute to the UC pathophysiology by triggering immune responses and/or allowing increased and more proximate exposure to luminal bacteria, both of which can lead to further reduced barrier maintenance, mucosal

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Summary

Objectives

Our aims were to investigate whether GC secretion was abnormal in UC and exists as a long-term effect of chronic inflammation

Methods
Results
Discussion
Conclusion

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