Metabolic Signaling and Disease Program, Diabetes and Obesity Research Center, Orlando, Florida, USA.
Am J Physiol Endocrinol Metab. 2012 Feb 1;302(3):E334-43. doi: 10.1152/ajpendo.00409.2011. Epub 2011 Nov 15.
Glucagon-like peptide-1 (GLP-1) receptor knockout (Glp1r(-/-)) mice exhibit impaired hepatic insulin action. High fat (HF)-fed Glp1r(-/-) mice exhibit improved, rather than the expected impaired, hepatic insulin action. This is due to decreased lipogenic gene expression and triglyceride accumulation. The present studies overcome these secondary adaptations by acutely modulating GLP-1R action in HF-fed wild-type mice. The central GLP-1R was targeted given its role as a regulator of hepatic insulin action. We hypothesized that acute inhibition of the central GLP-1R impairs hepatic insulin action beyond the effects of HF feeding. We further hypothesized that activation of the central GLP-1R improves hepatic insulin action in HF-fed mice. Insulin action was assessed in conscious, unrestrained mice using the hyperinsulinemic euglycemic clamp. Mice received intracerebroventricular (icv) infusions of artificial cerebrospinal fluid, GLP-1, or the GLP-1R antagonist exendin-9 (Ex-9) during the clamp. Intracerebroventricular Ex-9 impaired the suppression of hepatic glucose production by insulin, whereas icv GLP-1 improved it. Neither treatment affected tissue glucose uptake. Intracerebroventricular GLP-1 enhanced activation of hepatic Akt and suppressed hypothalamic AMP-activated protein kinase. Central GLP-1R activation resulted in lower hepatic triglyceride levels but did not affect muscle, white adipose tissue, or plasma triglyceride levels during hyperinsulinemia. In response to oral but not intravenous glucose challenges, activation of the central GLP-1R improved glucose tolerance. This was associated with higher insulin levels. Inhibition of the central GLP-1R had no effect on oral or intravenous glucose tolerance. These results show that inhibition of the central GLP-1R deteriorates hepatic insulin action in HF-fed mice but does not affect whole body glucose homeostasis. Contrasting this, activation of the central GLP-1R improves glucose homeostasis in HF-fed mice by increasing insulin levels and enhancing hepatic insulin action.
胰高血糖素样肽-1 (GLP-1) 受体敲除 (Glp1r(-/-)) 小鼠表现出肝胰岛素作用受损。高脂肪 (HF) 喂养的 Glp1r(-/-) 小鼠表现出改善的肝胰岛素作用,而不是预期的受损,这是由于脂肪生成基因表达和甘油三酯积累减少。本研究通过急性调节 HF 喂养野生型小鼠中的 GLP-1R 作用来克服这些次要适应。由于其作为肝胰岛素作用调节剂的作用,靶向中枢 GLP-1R。我们假设中枢 GLP-1R 的急性抑制作用超出 HF 喂养的影响,损害肝胰岛素作用。我们进一步假设中枢 GLP-1R 的激活可改善 HF 喂养小鼠的肝胰岛素作用。使用高胰岛素-正葡萄糖钳夹术在清醒、不受约束的小鼠中评估胰岛素作用。在钳夹过程中,小鼠接受脑室内 (icv) 人工脑脊液、GLP-1 或 GLP-1R 拮抗剂 exendin-9 (Ex-9) 的输注。脑室内 Ex-9 削弱了胰岛素对肝葡萄糖产生的抑制作用,而脑室内 GLP-1 则改善了抑制作用。两种处理都不影响组织葡萄糖摄取。脑室内 GLP-1 增强了肝 Akt 的激活并抑制了下丘脑 AMP 激活的蛋白激酶。中枢 GLP-1R 的激活导致肝甘油三酯水平降低,但在高胰岛素血症期间不影响肌肉、白色脂肪组织或血浆甘油三酯水平。对口服而不是静脉内葡萄糖挑战的反应,中枢 GLP-1R 的激活改善了葡萄糖耐量。这与更高的胰岛素水平有关。中枢 GLP-1R 的抑制对口服或静脉内葡萄糖耐量没有影响。这些结果表明,抑制中枢 GLP-1R 会恶化 HF 喂养小鼠的肝胰岛素作用,但不会影响全身葡萄糖稳态。与此形成对比的是,中枢 GLP-1R 的激活通过增加胰岛素水平和增强肝胰岛素作用来改善 HF 喂养小鼠的葡萄糖稳态。
