RETINOL BINDING PROTEIN-4 AND INSULIN RESISTANCE

视黄醇结合蛋白 4 和胰岛素抵抗

• 批准号: 6948214
• 负责人: TIMOTHY E. GRAHAM
• 金额: $ 12.88万
• 依托单位: BETH ISRAEL DEACONESS MEDICAL CENTER
• 依托单位国家: 美国
• 财政年份: 2004
• 资助国家: 美国
• 起止时间: 2004-09-15 至 2009-06-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6948214
• 关键词: adipose tissue; biomarker; fenretinide; gene expression; gene targeting; genetically modified animals; glucose; glucose transporter; insulin sensitivity /resistance; laboratory mouse; nuclear receptors; protein protein interaction; protein structure function; retinoate; retinoid binding proteins; tissue /cell culture; vitamin receptor

DESCRIPTION (provided by applicant): Reduction in the expression of the glucose transporter-4 in adipose tissue is one of the earliest changes that occur in human conditions characterized by insulin resistance, including type 2 diabetes. Mice harboring an adipose tissue-specific genetic knockout of Glut4 display reduced insulin-stimulated glucose transport in adipose tissue and develop systemic insulin resistance affecting hepatic glucose production and skeletal muscle glucose transport. Since only adipose tissue is genetically altered in this model, we hypothesized that one or more circulating factors causing systemic insulin resistance may be secreted into the circulation by adipose tissue with reduced Glut4 expression. We used Affymetrix global gene analysis to identify retinol binding protein-4 (RBP4) as a candidate molecule for mediating systemic insulin resistance in this model. The mRNA of RBP4 is up-regulated in adipose tissue, but not in liver, of adipose-Glut4 knockout mice. Serum levels of RBP4 are increased in adipose-Glut4 knockout mice and five other mouse models of insulin resistance, suggesting that RBP4 may be a marker for insulin resistance or hyperinsulinemia. However, we find that RBP4 knockout mice exhibit a phenotype of increased sensitivity to insulin. Thus, elevations of circulating RBP4 may serve not only as a marker but as an actual cause of systemic insulin resistance. In humans we find a strong correlation between serum RBP4 levels and insulin resistance measured by euglycemic hyperinsulinemic clamp, indicating that RBP4 could be a novel endocrine mediator of systemic insulin resistance in humans. To test the hypothesis that RBP4 is a cause of insulin resistance, we will analyze the metabolic features of mice with genetic alterations in RBP4 expression. We will test the effects of pharmacologically altering circulating RBP4 levels, either by treating with fenretinide, a drug that causes urinary wasting of RBP4, or by injecting purified RBP4. We will investigate potential mechanisms, both retinoid-dependent and retinoid-independent, by which RBP4 may influence insulin-glucose homeostasis

描述(由申请人提供)： 脂肪组织中葡萄糖转运蛋白-4的表达减少是以胰岛素抵抗为特征的人类条件下最早发生的变化之一，包括2型糖尿病。携带脂肪组织特异性GLUT4基因敲除的小鼠表现出胰岛素刺激的脂肪组织中葡萄糖运输减少，并出现全身性胰岛素抵抗，影响肝脏葡萄糖的产生和骨骼肌的葡萄糖运输。由于在这个模型中只有脂肪组织发生了基因改变，我们假设一个或多个导致系统性胰岛素抵抗的循环因子可能通过GLUT4表达减少的脂肪组织分泌到循环中。我们使用Affymetrix全局基因分析来确定视黄醇结合蛋白-4(RBP4)是该模型中介导全身性胰岛素抵抗的候选分子。在脂肪-GLUT4基因敲除小鼠中，RBP4的mRNA在脂肪组织中上调，而在肝脏中不表达。在脂肪-GLUT4基因敲除小鼠和其他五种胰岛素抵抗小鼠模型中，血清RBP4水平升高，表明RBP4可能是胰岛素抵抗或高胰岛素血症的标志。然而，我们发现RBP4基因敲除小鼠表现出对胰岛素敏感性增加的表型。因此，循环RBP4的升高不仅可以作为一个标志物，而且可以作为全身性胰岛素抵抗的实际原因。在人类中，我们发现血清RBP4水平与正常血糖高胰岛素钳夹法测量的胰岛素抵抗之间存在很强的相关性，表明RBP4可能是人类全身胰岛素抵抗的一种新的内分泌介质。为了验证RBP4是胰岛素抵抗的原因这一假设，我们将分析RBP4表达发生遗传变化的小鼠的代谢特征。我们将测试药物改变循环中的RBP4水平的效果，无论是通过治疗芬维甲素，一种导致RBP4尿液排泄的药物，还是通过注射纯化的RBP4。我们将研究RBP4可能影响胰岛素-葡萄糖稳态的潜在机制，包括视黄醇依赖和维甲酸非依赖机制。