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Glucose control of glucagon secretion—‘There’s a brand-new gimmick every year’

机译:胰高血糖素分泌的葡萄糖控制-每年都有一个全新的头

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摘要

Glucagon from the pancreatic α-cells is a major blood glucose-regulating hormone whose most important role is to prevent hypoglycaemia that can be life-threatening due to the brain’s strong dependence on glucose as energy source. Lack of blood glucose-lowering insulin after malfunction or autoimmune destruction of the pancreatic β-cells is the recognized cause of diabetes, but recent evidence indicates that diabetic hyperglycaemia would not develop unless lack of insulin was accompanied by hypersecretion of glucagon. Glucagon release has therefore become an increasingly important target in diabetes management. Despite decades of research, an understanding of how glucagon secretion is regulated remains elusive, and fundamentally different mechanisms continue to be proposed. The autonomous nervous system is an important determinant of glucagon release, but it is clear that secretion is also directly regulated within the pancreatic islets. The present review focuses on pancreatic islet mechanisms involved in glucose regulation of glucagon release. It will be argued that α-cell-intrinsic processes are most important for regulation of glucagon release during recovery from hypoglycaemia and that paracrine inhibition by somatostatin from the δ-cells shapes pulsatile glucagon release in hyperglycaemia. The electrically coupled β-cells ultimately determine islet hormone pulsatility by releasing synchronizing factors that affect the α- and δ-cells.
机译:胰腺α细胞中的胰高血糖素是主要的血糖调节激素,其最重要的作用是防止由于大脑强烈依赖葡萄糖作为能量来源而导致生命危险的低血糖症。胰腺β细胞功能异常或自身免疫破坏后缺乏降低血糖的胰岛素是公认的糖尿病原因,但最近的证据表明,除非缺乏胰岛素并伴有胰高血糖素的过度分泌,否则不会出现糖尿病性高血糖症。因此,胰高血糖素的释放已成为糖尿病管理中越来越重要的目标。尽管进行了数十年的研究,但对如何调节胰高血糖素分泌的了解仍然难以捉摸,并且仍在继续提出根本不同的机制。自主神经系统是胰高血糖素释放的重要决定因素,但很明显,胰岛内的分泌也受到直接调节。目前的审查集中在胰岛机制参与胰高血糖素释放的葡萄糖调节。有人认为,α细胞内在过程对于低血糖恢复过程中胰高血糖素释放的调节最重要,而生长激素抑制素从δ细胞中抑制旁分泌会形成高血糖时脉动性胰高血糖素的释放。电耦合的β细胞通过释放影响α细胞和δ细胞的同步因子来最终确定胰岛激素的搏动性。

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