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胰岛结构和细胞相互作用在胰岛素分泌控制中的作用。

Role of islet structure and cellular interactions in the control of insulin secretion.

机构信息

SAAD Centre for Pharmacy and Diabetes, Queen's University of Belfast, Northern Ireland, UK.

出版信息

Islets. 2011 Mar-Apr;3(2):41-7. doi: 10.4161/isl.3.2.14805. Epub 2011 Mar 1.

Abstract

Close cellular proximity and correct anatomical arrangement within islets are essential for normal patterns of insulin secretion. Thus, segregation of islets into single cells is associated with a dramatic decline in stimulus secretion-coupling and glucose-induced insulin release. Generation of pseudoislets from clonal islet cell lines provides a useful model to examine islet cell interactions and insulin secretion. Such studies have highlighted the functional importance of cell adhesion molecules and connexins. Pseudoislets comprising insulin-secreting cell lines have been shown to closely mimic primary islets in both size and morphology, displaying a significantly enhanced response to glucose, nutrients and drugs over equivalent monolayer cultures. Here, we consider the influence of islet structure and cellular interactions in the control of insulin secretion. The functional characteristics of pseudoislets derived from clonal beta-cell lines or a combination of alpha-, beta- and delta-cell lines are discussed in light of normal islet function and possible therapeutic application.

摘要

胰岛内细胞的紧密接近和正确的解剖排列对于正常的胰岛素分泌模式至关重要。因此,胰岛的分离成单个细胞与刺激-分泌偶联和葡萄糖诱导的胰岛素释放的显著下降有关。从克隆胰岛细胞系生成假胰岛提供了一个有用的模型来研究胰岛细胞相互作用和胰岛素分泌。这些研究强调了细胞黏附分子和连接蛋白的功能重要性。已显示由分泌胰岛素的细胞系组成的假胰岛在大小和形态上非常类似于原代胰岛,对葡萄糖、营养物质和药物的反应明显增强,超过等效的单层培养物。在这里,我们考虑胰岛结构和细胞相互作用对胰岛素分泌的控制。根据正常胰岛功能和可能的治疗应用,讨论了从克隆β细胞系或α、β和δ细胞系组合衍生的假胰岛的功能特征。

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