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葡萄糖而非氯化钾可减少小鼠β细胞中的膜下颗粒更新。

Glucose but not KCl diminishes submembrane granule turnover in mouse beta-cells.

作者信息

Brüning Dennis, Reckers Kirstin, Drain Peter, Rustenbeck Ingo

机构信息

Institute of Pharmacology and ToxicologyUniversity of Braunschweig, Braunschweig, Germany.

Department of Cell BiologyUniversity of Pittsburgh, Pittsburgh, Pennsylvania, USA.

出版信息

J Mol Endocrinol. 2017 Oct;59(3):311-324. doi: 10.1530/JME-17-0063. Epub 2017 Aug 1.

DOI:10.1530/JME-17-0063
PMID:28765259
Abstract

KCl depolarization is widely used to mimic the depolarization during glucose-stimulated insulin secretion. Consequently, the insulin secretion elicited by KCl is often regarded as the equivalent of the first phase of glucose-induced insulin secretion. Here, the effects of both stimuli were compared by measuring the secretion of perifused mouse islets, the cytosolic Ca concentration of single beta-cells and the mobility of submembrane insulin granules by TIRF microscopy of primary mouse beta-cells. Two cargo-directed granule labels were used namely insulin-EGFP and C-peptide-emGFP. The granule behaviour common to both was used to compare the effect of sequential stimulation with 40 mM KCl and 30 mM glucose and sequential stimulation with the same stimuli in reversed order. At the level of the cell secretory response, the sequential pulse protocol showed marked differences depending on the order of the two stimuli. KCl produced higher maximal secretion rates and diminished the response to the subsequent glucose stimulus, whereas glucose enhanced the response to the subsequent KCl stimulus. At the level of granule behaviour, a difference developed during the first stimulation phase in that the total number of granules, the short-term resident granules and the arriving granules, which are all parameters of granule turnover, were significantly smaller for glucose than for KCl. These differences at both the level of the cell secretory response and granule behaviour in the submembrane space are incompatible with identical initial response mechanisms to KCl and glucose stimulation.

摘要

氯化钾去极化被广泛用于模拟葡萄糖刺激胰岛素分泌过程中的去极化。因此,氯化钾引发的胰岛素分泌常被视为等同于葡萄糖诱导胰岛素分泌的第一阶段。在此,通过测量灌流小鼠胰岛的分泌、单个β细胞的胞质钙浓度以及利用原代小鼠β细胞的全内反射荧光显微镜观察质膜下胰岛素颗粒的移动性,比较了这两种刺激的效果。使用了两种靶向货物的颗粒标记物,即胰岛素 - 增强绿色荧光蛋白(insulin-EGFP)和C肽 - 增强型单体绿色荧光蛋白(C-peptide-emGFP)。利用两者共有的颗粒行为来比较用40 mM氯化钾和30 mM葡萄糖进行顺序刺激以及以相反顺序用相同刺激进行顺序刺激的效果。在细胞分泌反应水平上,顺序脉冲方案显示出明显差异,这取决于两种刺激的顺序。氯化钾产生更高的最大分泌速率,并减弱了对随后葡萄糖刺激的反应,而葡萄糖增强了对随后氯化钾刺激的反应。在颗粒行为水平上,在第一个刺激阶段出现了差异,即颗粒周转的所有参数,如颗粒总数、短期驻留颗粒和到达颗粒,葡萄糖刺激时比氯化钾刺激时显著更小。在细胞分泌反应水平和质膜下空间的颗粒行为水平上的这些差异与对氯化钾和葡萄糖刺激的相同初始反应机制不相符。

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