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胰岛内细胞间通讯在健康和疾病中的作用。

Intercellular Communication in the Islet of Langerhans in Health and Disease.

机构信息

Department of Cell Biology and Physiology, Washington University, St Louis, Missouri, USA.

出版信息

Compr Physiol. 2021 Jun 30;11(3):2191-2225. doi: 10.1002/cphy.c200026.

Abstract

Blood glucose homeostasis requires proper function of pancreatic islets, which secrete insulin, glucagon, and somatostatin from the β-, α-, and δ-cells, respectively. Each islet cell type is equipped with intrinsic mechanisms for glucose sensing and secretory actions, but these intrinsic mechanisms alone cannot explain the observed secretory profiles from intact islets. Regulation of secretion involves interconnected mechanisms among and between islet cell types. Islet cells lose their normal functional signatures and secretory behaviors upon dispersal as compared to intact islets and in vivo. In dispersed islet cells, the glucose response of insulin secretion is attenuated from that seen from whole islets, coordinated oscillations in membrane potential and intracellular Ca activity, as well as the two-phase insulin secretion profile, are missing, and glucagon secretion displays higher basal secretion profile and a reverse glucose-dependent response from that of intact islets. These observations highlight the critical roles of intercellular communication within the pancreatic islet, and how these communication pathways are crucial for proper hormonal and nonhormonal secretion and glucose homeostasis. Further, misregulated secretions of islet secretory products that arise from defective intercellular islet communication are implicated in diabetes. Intercellular communication within the islet environment comprises multiple mechanisms, including electrical synapses from gap junctional coupling, paracrine interactions among neighboring cells, and direct cell-to-cell contacts in the form of juxtacrine signaling. In this article, we describe the various mechanisms that contribute to proper islet function for each islet cell type and how intercellular islet communications are coordinated among the same and different islet cell types. © 2021 American Physiological Society. Compr Physiol 11:2191-2225, 2021.

摘要

血糖稳态需要胰腺胰岛的正常功能,胰岛分别从β-、α-和δ-细胞分泌胰岛素、胰高血糖素和生长抑素。每种胰岛细胞类型都具有葡萄糖感应和分泌作用的内在机制,但这些内在机制本身并不能解释从完整胰岛中观察到的分泌谱。分泌的调节涉及胰岛细胞类型之间和内部的相互关联的机制。与完整胰岛和体内相比,胰岛细胞在分散时会失去其正常的功能特征和分泌行为。在分散的胰岛细胞中,胰岛素分泌的葡萄糖反应比完整胰岛中的反应减弱,膜电位和细胞内 Ca 活性的协调振荡以及两相胰岛素分泌谱缺失,而胰高血糖素分泌显示出更高的基础分泌谱和与完整胰岛相反的葡萄糖依赖性反应。这些观察结果突出了胰岛内细胞间通讯的关键作用,以及这些通讯途径对适当的激素和非激素分泌以及血糖稳态的重要性。此外,由于细胞间胰岛通讯缺陷而导致的胰岛分泌产物的失调分泌与糖尿病有关。胰岛环境中的细胞间通讯包括多种机制,包括缝隙连接偶联的电突触、相邻细胞之间的旁分泌相互作用以及以旁分泌信号的形式的直接细胞间接触。在本文中,我们描述了有助于每种胰岛细胞类型的胰岛正常功能的各种机制,以及细胞间胰岛通讯如何在相同和不同的胰岛细胞类型之间协调。

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