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Site-related white adipose tissue lipid-handling response to oleoyl-estrone treatment in overweight male rats
Authors:María del Mar Romero   José Antonio Fernández-López   Montserrat Esteve  Marià Alemany
Affiliation:(1) Department of Nutrition and Food Science, Faculty of Biology, University of Barcelona, Barcelona, Spain;(2) CIBER Obesity and Nutrition, Institute of Health Carlos III, Barcelona, Spain
Abstract:Background  Oleoyl-estrone (OE) decreases energy intake while maintaining glucose homeostasis, and energy expenditure at the expense of body fat. White adipose tissue (WAT) depots behave differently under starvation, postprandial state and pharmacologically induced lipolysis. Aim of the study  To understand the mechanism of massive lipid loss from WAT elicited by OE treatment. Methods  We used overweight male rats. Rats receiving OE (10 nmol/g) gavages were compared with controls and a pair-fed group. Whole fat pads from the mesenteric, retroperitoneal, epididymal and inguinal subcutaneous sites were excised and analyzed for lipid, DNA, mRNA and the expression of lipogenic, fatty acid transporters and lipase genes. Results  In OE and pair-fed rats, WAT weights decreased, with the limited loss of cells. Patterns of gene expression in most WAT sites were similar for OE and PF, suggesting a shared mechanism of fat mobilization, but in mesenteric WAT, PF increased lipogenic and fatty acid transporter gene expressions. However, OE inhibited lipogenic expressions more deeply than PF. Conclusions  White adipose tissue sites showed different expression patterns, hinting at relatively specialized functions in fat storage; thus, single site analyses cannot be extrapolated to whole WAT. Differences between mesenteric and the other sites suggest that ‘visceral fat’ should be reserved for this site only, and not applied to other abdominal fat depots (epididymal, retroperitoneal). Electronic supplementary material  The online version of this article (doi:) contains supplementary material, which is available to authorized users.
Keywords:White adipose tissue  Obesity  Oleoyl-estrone  Visceral fat  Lipogenesis
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