beta-cell adaptation in a mouse model of glucocorticoid-induced metabolic syndromeShow others and affiliations
2013 (English)In: Journal of Endocrinology, ISSN 0022-0795, E-ISSN 1479-6805, Vol. 219, no 3, p. 231-241Article in journal (Refereed) Published
Abstract [en]
Glucocorticoids (GCs) are stress hormones primarily responsible for mobilizing glucose to the circulation. Due to this effect, insulin resistance and glucose intolerance are concerns in patients with endogenous overproduction of GCs and in patients prescribed GC-based therapy. In addition, hypercortisolemic conditions share many characteristics with the metabolic syndrome. This study reports on a thorough characterization, in terms of glucose control and lipid handling, of a mouse model where corticosterone is given via the drinking water. C57BL/6J mice were treated with corticosterone (100 or 25 mu g/ml) or vehicle in their drinking water for 5 weeks after which they were subjected to insulin or glucose tolerance tests. GC-treated mice displayed increased food intake, body weight gain, and central fat deposit accumulations. In addition, the GC treatment led to dyslipidemia as well as accumulation of ectopic fat in the liver and skeletal muscle, having a substantial negative effect on insulin sensitivity. Also glucose intolerance and hypertension, both part of the metabolic syndrome, were evident in the GC-treated mice. However, the observed effects of corticosterone were reversed after drug removal. Furthermore, this study reveals insights into beta-cell adaptation to the GC-induced insulin resistance. Increased pancreatic islet volume due to cell proliferation, increased insulin secretion capacity, and increased islet chaperone expression were found in GC-treated animals. This model mimics the human metabolic syndrome. It could be a valuable model for studying the complex mechanisms behind the development of the metabolic syndrome and type 2 diabetes, as well as the multifaceted relations between GC excess and disease.
Place, publisher, year, edition, pages
BioScientifica , 2013. Vol. 219, no 3, p. 231-241
Keywords [en]
glucocorticoid, diabetes, insulin secretion, obesity, islet cells
National Category
Clinical Medicine
Identifiers
URN: urn:nbn:se:hig:diva-38202DOI: 10.1530/JOE-13-0189ISI: 000327761300005OAI: oai:DiVA.org:hig-38202DiVA, id: diva2:1646181
2014-01-072022-03-21Bibliographically approved