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胰岛素反应性细胞中GLUT4葡萄糖转运蛋白异构体的亚细胞定位与运输

Subcellular localization and trafficking of the GLUT4 glucose transporter isoform in insulin-responsive cells.

作者信息

Holman G D, Cushman S W

机构信息

Department of Biochemistry, University of Bath, Claverton Down, UK.

出版信息

Bioessays. 1994 Oct;16(10):753-9. doi: 10.1002/bies.950161010.

DOI:10.1002/bies.950161010
PMID:7980479
Abstract

The rate-limiting step in the uptake and metabolism of D-glucose by insulin target cells is thought to be glucose transport mediated by glucose transporters (primarily the GLUT4 isoform) localized to the plasma membrane. However, subcellular fractionation, photolabelling and immunocytochemical studies have shown that the pool of GLUT4 present in the plasma membrane is only one of many subcellular pools of this protein. GLUT4 has been found in occluded vesicles at the plasma membrane, clathrin-coated pits and vesicles, early endosomes, and tubulo-vesicular structures; the latter are analogous to known specialized secretory compartments. Tracking the movement of GLUT4 through these compartments, and defining the mechanism and site of action of insulin in stimulating this subcellular trafficking, are major topics of current investigation. Recent evidence focuses attention on the exocytosis of GLUT4 as the major site of insulin action. Increased exocytosis may be due to decreased retention of glucose transporters in an intracellular pool, or possibly to increased assembly of a vesicle docking and fusion complex. Although details are unknown, the presence in GLUT4 vesicles of a synaptobrevin homologue leads us to propose that a process analogous to that occurring in synaptic vesicle trafficking is involved in the assembly of GLUT4 vesicles into a form suitable for fusion with the plasma membrane. Evidence that the pathways of signalling from the insulin receptor and of GLUT4 vesicle exocytosis may converge at the level of the key signalling enzyme, phosphatidylinositol 3-kinase, is discussed.

摘要

胰岛素靶细胞摄取和代谢D-葡萄糖的限速步骤被认为是由定位于质膜的葡萄糖转运蛋白(主要是GLUT4亚型)介导的葡萄糖转运。然而,亚细胞分级分离、光标记和免疫细胞化学研究表明,质膜中存在的GLUT4库只是该蛋白众多亚细胞库之一。已在质膜处的封闭小泡、网格蛋白包被的小窝和小泡、早期内体以及管状小泡结构中发现了GLUT4;后者类似于已知的特殊分泌区室。追踪GLUT4在这些区室中的移动,并确定胰岛素刺激这种亚细胞运输的作用机制和作用位点,是当前研究的主要课题。最近的证据将注意力集中在GLUT4的胞吐作用上,认为这是胰岛素作用的主要位点。胞吐作用增加可能是由于细胞内池中葡萄糖转运蛋白的保留减少,或者可能是由于小泡对接和融合复合物的组装增加。尽管细节尚不清楚,但GLUT4小泡中存在突触小泡蛋白同系物,这使我们提出,类似于突触小泡运输中发生的过程参与了GLUT4小泡组装成适合与质膜融合的形式。本文还讨论了胰岛素受体信号传导途径和GLUT4小泡胞吐作用可能在关键信号酶磷脂酰肌醇3激酶水平上汇聚的证据。

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