内科学
内分泌学
炎症
葡萄糖稳态
下调和上调
氧化应激
胰岛素
糖尿病
厌食
胰岛
生物
小岛
医学
胰岛素抵抗
生物化学
体重
基因
作者
Charlotte Lindfors,Abram Katz,Lars Selander,Jeanette E. Johansen,Giancarlo Marconi,Martin Schalling,Tomas Hökfelt,Per Olof Berggren,С. В. Зайцев,Ida Nilsson
出处
期刊:American Journal of Physiology-endocrinology and Metabolism
[American Physiological Society]
日期:2015-08-15
卷期号:309 (4): E418-E427
被引量:9
标识
DOI:10.1152/ajpendo.00081.2015
摘要
Inflammation and impaired mitochondrial oxidative phosphorylation are considered key players in the development of several metabolic disorders, including diabetes. We have previously shown inflammation and mitochondrial dysfunction in the hypothalamus of an animal model for anorexia, the anx/anx mouse. Moreover, increased incidence of eating disorders, e.g., anorexia nervosa, has been observed in diabetic individuals. In the present investigation we evaluated whether impaired mitochondrial phosphorylation and inflammation also occur in endocrine pancreas of anorectic mice, and if glucose homeostasis is disturbed. We show that anx/anx mice exhibit marked glucose intolerance associated with reduced insulin release following an intraperitoneal injection of glucose. In contrast, insulin release from isolated anx/anx islets is increased after stimulation with glucose or KCl. In isolated anx/anx islets there is a strong downregulation of the mitochondrial complex I (CI) assembly factor, NADH dehydrogenase (ubiquinone) 1α subcomplex, assembly factor 1 (Ndufaf1), and a reduced CI activity. In addition, we show elevated concentrations of free fatty acids (FFAs) in anx/anx serum and increased macrophage infiltration (indicative of inflammation) in anx/anx islets. However, isolated islets from anx/anx mice cultured in the absence of FFAs do not exhibit increased inflammation. We conclude that the phenotype of the endocrine pancreas of the anx/anx mouse is characterized by increased levels of circulating FFAs, as well as inflammation, which can inhibit insulin secretion in vivo. The anx/anx mouse may represent a useful tool for studying molecular mechanisms underlying the association between diabetes and eating disorders.
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