REGULATION OF GLUCOSE METABOLISM BY CENTRAL INSULIN ACTION

H. Inoue
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Abstract

Insulin has been known to act on the hypothalamus, in particular the arcuate nucleus, in the central nervous system. Such central insulin action is not only involved in the regulation of energy metabolism via the regulation of food intake and heat production, but also plays an important role in glucose metabolism by regulating hepatic glucose production and glucose uptake by skeletal muscles. Studies on the intracerebroventricular administration of PI-3K inhibitors or sulfonylureas have demonstrated that hyperpolarization of agouti-related protein neurons induced by the activation of PI-3K signaling/KATP channels in the hypothalamic arcuate nucleus plays an important role in the suppression of hepatic glucose production mediated by central insulin action. Cutting of the vagus nerve overrides the suppression of hepatic glucose production by intracerebroventricular insulin administration, which suggests the involvement of autonomic nerves in central insulin action in the liver. The central insulin action-mediated suppression of hepatic glucose production is associated with decreased gene expression of enzymes involved in hepatic gluconeogenesis, and both increased interleukin-6 expression in hepatic non-parenchymal cells induced by central insulin action and associated activation of hepatic STAT3 play an important role in the suppression of gene expression of hepatic gluconeogenesis-related enzymes. In animal models of obesity and insulin resistance, the central insulin action-mediated hepatic glucose production control mechanism is impaired in both the hypothalamus and liver. Increased hepatic gluconeogenesis in obesity and type-2 diabetes has been attributed to impaired hepatic insulin signaling and increased expression of enzymes involved in hepatic gluconeogenesis due to hyperglycemia, but may also be partially attributed to the impairment of the central insulin action-mediated suppression of hepatic gluconeogenesis. Biomedical Reviews 2011; 22: 31-39.
中枢胰岛素作用对葡萄糖代谢的调节
已知胰岛素作用于中枢神经系统的下丘脑,特别是弓状核。这种胰岛素中枢作用不仅通过调节食物摄入和产热参与能量代谢的调节,还通过调节肝脏葡萄糖生成和骨骼肌葡萄糖摄取在葡萄糖代谢中发挥重要作用。脑室内给药PI-3K抑制剂或磺脲类药物的研究表明,下丘脑弓状核PI-3K信号通路/KATP通道激活诱导的刺痛症相关蛋白神经元的超极化在中枢胰岛素作用介导的肝糖生成的抑制中起重要作用。迷走神经的切断超过了脑室注射胰岛素对肝脏葡萄糖产生的抑制,这表明自主神经参与了肝脏的中枢胰岛素作用。中枢胰岛素作用介导的肝糖生成抑制与肝糖异生相关酶基因表达的降低有关,而中枢胰岛素作用诱导的肝非实质细胞白介素-6表达的增加和相关的肝STAT3的激活在抑制肝糖异生相关酶基因表达中起重要作用。在肥胖和胰岛素抵抗的动物模型中,中枢胰岛素作用介导的肝脏葡萄糖生成控制机制在下丘脑和肝脏中都受到损害。肥胖和2型糖尿病患者肝脏糖异生增加归因于高血糖导致的肝脏胰岛素信号通路受损和参与肝脏糖异生的酶表达增加,但也可能部分归因于胰岛素作用介导的肝糖异生中枢抑制功能受损。生物医学评论2011;22: 31 - 39。
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