| Literature DB >> 24266926 |
Tsunekazu Mizushima1, Satoko Arakawa2, Yasuaki Sanada3, Ikuyo Yoshino2, Dai Miyazaki2, Hayato Urushima4, Yoshihide Tsujimoto5, Toshinori Ito4, Shigeomi Shimizu6.
Abstract
IL-10-deficient mice spontaneously develop intestinal inflammation, which has many similarities to Crohn's disease. Several reports suggest that epithelial cell death may increase the severity of colitis; however, decisive evidence is lacking. In the present report, we addressed whether and how epithelial cell death plays a role in the development of chronic colitis. We first examined the morphological characteristics of intestines of IL-10-deficient mice and found two forms of epithelial cell death (typical apoptosis and necrosis-like cell death) in colitis. To elucidate the pathological roles of epithelial cell death, we crossbred IL-10-deficient knockout mice with Bcl-2 transgenic mice, in which the anti-apoptosis protein Bcl-2 was overexpressed in intestinal epithelial cells, but not in immune cells. Epithelial cell-specific Bcl-2 protected IL-10 deficiency-induced colitis and markedly reduced their symptoms. Interestingly, morphological analysis revealed that Bcl-2 suppressed apoptosis and necrosis-like cell death, and better maintained mucosal barrier in IL-10-deficient mice. From the immunological aspect, Bcl-2 did not alter the activation of T-helper cell 1 but inhibited the growth of T-helper cell 17, suggesting that mucosal integrity may control the immune responses. These results provide genetic evidence demonstrating that epithelial cell death is crucial for the development of chronic colitis.Entities:
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Year: 2013 PMID: 24266926 DOI: 10.1016/j.ajpath.2013.08.012
Source DB: PubMed Journal: Am J Pathol ISSN: 0002-9440 Impact factor: 4.307