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Intestinal retinol saturase is implicated in the development of obesity and epithelial homeostasis upon injury

Item Type:Article
Title:Intestinal retinol saturase is implicated in the development of obesity and epithelial homeostasis upon injury
Creators Name:Kiefer, M.F., Meng, Y., Yang, N., Vahrenbrink, M., Wulff, S., Li, C., Wowro, S.J., Petricek, K.M., Sommerfeld, M., Flores, R.E., Obermayer, B., Piepelow, K., Klaus, S., Hartl, K., Guillot, A., Tacke, F., Sigal, M. and Schupp, M.
Abstract:Retinol saturase (RetSat) is an oxidoreductase involved in lipid metabolism and the cellular sensitivity to peroxides. RetSat is highly expressed in metabolic organs like liver and adipose tissue and its global loss in mice increases body weight and adiposity. The regulation of RetSat expression and its function in the intestine are unexplored. Here, we show that RetSat is present in different segments of the digestive system, localizes to intestinal epithelial cells, and is upregulated by feeding mice high-fat diet (HFD). Intestine-specific RetSat deletion in adult mice did not affect nutrient absorption and energy homeostasis basally, but lowered body weight gain and fat mass of HFD-fed mice, potentially via increasing locomotor activity. Moreover, jejunal expression of genes related to β-oxidation and cholesterol efflux were decreased and colonic cholesterol content reduced upon RetSat deletion. In colitis, which we show to downregulate intestinal RetSat expression in humans and mice, RetSat ablation improved epithelial architecture of the murine colon. Thus, intestinal RetSat expression is regulated by dietary interventions and inflammation, and its loss reduces weight gain upon HFD-feeding and alleviates epithelial damage upon injury.
Keywords:Colitis, Intestine, Obesity, RetSat, Animals, Mice
Source:American Journal of Physiology Endocrinology and Metabolism
ISSN:0193-1849
Publisher:American Physiological Society
Volume:327
Number:2
Page Range:E203-E216
Date:August 2024
Official Publication:https://doi.org/10.1152/ajpendo.00035.2024
PubMed:View item in PubMed

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