The amount of keratins matters for stress protection of the colonic epithelium

A1 Journal article (refereed)


Internal Authors/Editors


Publication Details

List of Authors: ASGHAR M.N., SILVANDER J.S.G., HELENIUS T.O., LÄHDENIEMI I.A.K., ALAM C., FORTELIUS L.E., HOLMSTEN R.O., TOIVOLA D.M.
Publisher: Public Library of Science
Publication year: 2015
Journal: PLoS ONE
Volume number: 10
Issue number: 5
Start page: 1
End page: 17
eISSN: 1932-6203


Abstract

Keratins (K) are important for epithelial stress protection as evidenced by keratin mutations predisposing to human liver diseases and possibly inflammatory bowel diseases. A role for K8 in the colon is supported by the ulcerative colitis-phenotype with epithelial hyperproliferation and abnormal ion transport in K8-knockout (K8-/-) mice. The heterozygote knockout (K8+/-) colon appears normal but displays a partial ion transport-defect. Characterizing the colonic phenotype we show that K8+/- colon expresses ~50% less keratins compared to K8 wild type (K8+/+) but de novo K7 expression is observed in the top-most cells of the K8+/- and K8-/- crypts. The K8+/- colonic crypts are significantly longer due to increased epithelial hyperproliferation, but display no defects in apoptosis or inflammation in contrast to K8-/-. When exposed to colitis using the dextran sulphate sodium-model, K8+/- mice showed higher disease sensitivity and delayed recovery compared to K8+/+ littermates. Therefore, the K8+/- mild colonic phenotype correlates with decreased keratin levels and increased sensitivity to experimental colitis, suggesting that a sufficient amount of keratin is needed for efficient stress protection in the colonic epithelia.

Last updated on 2019-20-10 at 05:04