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Publication : The ROS-generating oxidase Nox1 is required for epithelial restitution following colitis.

First Author  Kato M Year  2016
Journal  Exp Anim Volume  65
Issue  3 Pages  197-205
PubMed ID  26876598 Mgi Jnum  J:315994
Mgi Id  MGI:6832220 Doi  10.1538/expanim.15-0127
Citation  Kato M, et al. (2016) The ROS-generating oxidase Nox1 is required for epithelial restitution following colitis. Exp Anim 65(3):197-205
abstractText  Accumulating evidence suggests that reactive oxygen species (ROS) generated by endogenous metabolic enzymes are involved in a variety of intracellular mechanisms. In particular, superoxide-generating NADPH oxidase (Nox) 1 is highly expressed in the colon and has been implicated in physiological and pathophysiological states of colon tissues. However, its role in tissue repair following colitis has not been fully elucidated. Our study using experimental colitis in mice showed that repair of the mucosal layer did not occur in Nox1-deficient mice following dextran sulfate sodium-induced colitis. This was accompanied by inhibition of proliferation, cell survival, migration, and terminal differentiation (generation of goblet cells) of crypt progenitor cells, as determined by histochemical analyses. Furthermore, Nox1 expression as well as ROS production in the colon crypt was increased during the repair process, and Nox1 deficiency suppressed these events. The results suggest that Nox1 promotes colon mucosal wound repair by sustaining the bioactivity of crypt progenitor cells and plays a crucial role in the epithelial restitution in the case of damage associated with colitis.
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