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胰高血糖素分泌和转运途径在胰腺α细胞中的研究进展：高胰高血糖素血症的新途径、新蛋白和新靶点。

Pathways of Glucagon Secretion and Trafficking in the Pancreatic Alpha Cell: Novel Pathways, Proteins, and Targets for Hyperglucagonemia.

机构信息

Department of Pathology and Laboratory Medicine, Western University, London, ON, Canada.

Program in Metabolism and Diabetes, Lawson Health Research Institute, London, ON, Canada.

出版信息

Front Endocrinol (Lausanne). 2021 Sep 29;12:726368. doi: 10.3389/fendo.2021.726368. eCollection 2021.

DOI:10.3389/fendo.2021.726368

PMID:34659118

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8511682/

Abstract

Patients with diabetes mellitus exhibit hyperglucagonemia, or excess glucagon secretion, which may be the underlying cause of the hyperglycemia of diabetes. Defective alpha cell secretory responses to glucose and paracrine effectors in both Type 1 and Type 2 diabetes may drive the development of hyperglucagonemia. Therefore, uncovering the mechanisms that regulate glucagon secretion from the pancreatic alpha cell is critical for developing improved treatments for diabetes. In this review, we focus on aspects of alpha cell biology for possible mechanisms for alpha cell dysfunction in diabetes: proglucagon processing, intrinsic and paracrine control of glucagon secretion, secretory granule dynamics, and alterations in intracellular trafficking. We explore possible clues gleaned from these studies in how inhibition of glucagon secretion can be targeted as a treatment for diabetes mellitus.

摘要

糖尿病患者表现出高胰高血糖素血症，即胰高血糖素分泌过多，这可能是糖尿病高血糖的根本原因。1 型和 2 型糖尿病中，α 细胞对葡萄糖的分泌反应缺陷和旁分泌效应物可能导致高胰高血糖素血症的发生。因此，揭示调节胰腺 α 细胞分泌胰高血糖素的机制对于开发治疗糖尿病的新方法至关重要。在这篇综述中，我们重点介绍了α 细胞生物学的各个方面，以探讨糖尿病中 α 细胞功能障碍的可能机制：胰高血糖素原加工、胰高血糖素分泌的内在和旁分泌控制、分泌颗粒动力学以及细胞内运输的改变。我们探讨了这些研究中可能获得的一些线索，即抑制胰高血糖素分泌可作为治疗糖尿病的一种方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1aba/8511682/326aacf79706/fendo-12-726368-g001.jpg

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胰高血糖素分泌和转运途径在胰腺α细胞中的研究进展：高胰高血糖素血症的新途径、新蛋白和新靶点。

Pathways of Glucagon Secretion and Trafficking in the Pancreatic Alpha Cell: Novel Pathways, Proteins, and Targets for Hyperglucagonemia.

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