Abstract
Chronic intestinal inflammation contributes to pathologies such as inflammatory bowel disease (IBD) and colon cancer. While the precise etiology remains controversial, IBD is believed to manifest as a result of various factors. We previously reported that intestinal-specific overexpression of the transcription factor Kaiso results in an intestinal inflammatory response; however, the cause of this inflammation is unknown. To elucidate the underlying mechanism(s) of the Kaiso-mediated intestinal inflammatory phenotype, we evaluated two independent transgenic mouse lines that express varying levels of Kaiso (KaisoTg). Histological analyses of KaisoTg mice revealed intestinal damage including thickening of the mucosa, intestinal “lesions” and crypt abscesses, which are reminiscent of IBD pathology. Additionally, higher Kaiso levels induced intestinal neutrophilia as early as 12 weeks, which worsened as the mice aged. Notably, the Kaiso-induced intestinal inflammation correlated with a leaky intestinal barrier and mis-regulation of E-cadherin expression and localization. Interestingly, Kaiso overexpression resulted in reduced proliferation but enhanced migration of intestinal epithelial cells prior to the onset of inflammation. Collectively, these data suggest that Kaiso plays a role in regulating intestinal epithelial cell integrity and function, dysregulation of which contributes to a chronic inflammatory phenotype as mice age.
Highlights
inflammatory bowel disease (IBD) refers to two intestinal disorders characterized by chronic inflammation: Crohn’s disease (CD), which affects both the small and large intestine in discontinuous patches of inflamed lesions, and ulcerative colitis (UC), which is restricted to the large intestine and presents as continuous regions of inflamed tissue [1,2,3]
We detected enhanced Kaiso staining in all four CD intestinal tissues (US Biomax) compared to normal tissues (Fig 1A), supporting the notion that Kaiso may be a relevant participant in the development of chronic intestinal inflammation
Given our findings that E-cadherin expression and lateral localization are diminished in pre-symptomatic villin Kaiso line A (VKA) mice, and since E-cadherin is a Kaiso target gene [15, 17] and is an important regulator of collective cell migration during intestinal restitution [39], we investigated whether intestinal epithelial cells (IEC) migration was altered in VKA mice
Summary
IBD refers to two intestinal disorders characterized by chronic inflammation: Crohn’s disease (CD), which affects both the small and large intestine in discontinuous patches of inflamed lesions, and ulcerative colitis (UC), which is restricted to the large intestine and presents as continuous regions of inflamed tissue [1,2,3]. There is no cure for IBD, and both UC and CD are primarily managed by alleviation of the symptoms [3]. Kaiso overexpression perturbs intestinal epithelial integrity and induces intestinal inflammation design, data collection and analysis, decision to publish, or preparation of the manuscript
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