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肝细胞中胰岛素和胰高血糖素受体信号的串扰。

Cross Talk Between Insulin and Glucagon Receptor Signaling in the Hepatocyte.

出版信息

Diabetes. 2022 Sep 1;71(9):1842-1851. doi: 10.2337/dbi22-0002.

Abstract

While the consumption of external energy (i.e., feeding) is essential to life, this action induces a temporary disturbance of homeostasis in an animal. A primary example of this effect is found in the regulation of glycemia. In the fasted state, stored energy is released to maintain physiological glycemic levels. Liver glycogen is liberated to glucose, glycerol and (glucogenic) amino acids are used to build new glucose molecules (i.e., gluconeogenesis), and fatty acids are oxidized to fuel long-term energetic demands. This regulation is driven primarily by the counterregulatory hormones epinephrine, growth hormone, cortisol, and glucagon. Conversely, feeding induces a rapid influx of diverse nutrients, including glucose, that disrupt homeostasis. Consistently, a host of hormonal and neural systems under the coordination of insulin are engaged in the transition from fasting to prandial states to reduce this disruption. The ultimate action of these systems is to appropriately store the newly acquired energy and to return to the homeostatic norm. Thus, at first glance it is tempting to assume that glucagon is solely antagonistic regarding the anabolic effects of insulin. We have been intrigued by the role of glucagon in the prandial transition and have attempted to delineate its role as beneficial or inhibitory to glycemic control. The following review highlights this long-known yet poorly understood hormone.

摘要

虽然消耗外源性能量(即进食)对生命至关重要,但这一行为会导致动物体内的内稳态暂时受到干扰。这种效应的一个主要例子存在于血糖调节中。在禁食状态下,储存的能量被释放出来以维持生理血糖水平。肝糖原分解为葡萄糖,甘油和(糖异生)氨基酸被用来合成新的葡萄糖分子,脂肪酸被氧化以满足长期能量需求。这种调节主要由反调节激素肾上腺素、生长激素、皮质醇和胰高血糖素驱动。相反,进食会导致各种营养物质(包括葡萄糖)的快速涌入,从而破坏内稳态。一致地,在胰岛素协调下的一系列激素和神经系统参与从禁食到进食状态的转变,以减少这种干扰。这些系统的最终作用是适当地储存新获得的能量,并恢复到内稳态的正常状态。因此,乍一看,人们很容易假设胰高血糖素在胰岛素的合成代谢作用方面是完全拮抗的。我们对胰高血糖素在进食过渡中的作用感到好奇,并试图阐明它对血糖控制是有益的还是抑制性的。以下综述强调了这种长期以来众所周知但仍知之甚少的激素。

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