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脂肪细胞中葡萄糖转运蛋白4(GLUT4)的保留需要两个细胞内胰岛素调节的转运步骤。

GLUT4 retention in adipocytes requires two intracellular insulin-regulated transport steps.

作者信息

Zeigerer Anja, Lampson Michael A, Karylowski Ola, Sabatini David D, Adesnik Milton, Ren Mindong, McGraw Timothy E

机构信息

Department of Biochemistry, Biophysics and Molecular Medicine, Weill Medical College of Cornell University, New York, New York 10021, USA.

出版信息

Mol Biol Cell. 2002 Jul;13(7):2421-35. doi: 10.1091/mbc.e02-02-0071.

Abstract

Insulin regulates glucose uptake into fat and muscle by modulating the distribution of the GLUT4 glucose transporter between the surface and interior of cells. The GLUT4 trafficking pathway overlaps with the general endocytic recycling pathway, but the degree and functional significance of the overlap are not known. In this study of intact adipocytes, we demonstrate, by using a compartment-specific fluorescence-quenching assay, that GLUT4 is equally distributed between two intracellular pools: the transferrin receptor-containing endosomes and a specialized compartment that excludes the transferrin receptor. These pools of GLUT4 are in dynamic communication with one another and with the cell surface. Insulin-induced redistribution of GLUT4 to the surface requires mobilization of both pools. These data establish a role for the general endosomal system in the specialized, insulin-regulated trafficking of GLUT4. Trafficking through the general endosomal system is regulated by rab11. Herein, we show that rab11 is required for the transport of GLUT4 from endosomes to the specialized compartment and for the insulin-induced translocation to the cell surface, emphasizing the importance of the general endosomal pathway in the specialized trafficking of GLUT4. Based on these findings we propose a two-step model for GLUT4 trafficking in which the general endosomal recycling compartment plays a specialized role in the insulin-regulated traffic of GLUT4. This compartment-based model provides the framework for understanding insulin-regulated trafficking at a molecular level.

摘要

胰岛素通过调节葡萄糖转运蛋白4(GLUT4)在细胞表面和内部之间的分布来调控脂肪和肌肉对葡萄糖的摄取。GLUT4的运输途径与一般的内吞循环途径重叠,但重叠的程度和功能意义尚不清楚。在这项对完整脂肪细胞的研究中,我们通过使用一种特定区室的荧光淬灭测定法证明,GLUT4在两个细胞内池之间均匀分布:含有转铁蛋白受体的内体和一个排除转铁蛋白受体的特殊区室。这些GLUT4池相互之间以及与细胞表面处于动态交流之中。胰岛素诱导的GLUT4向细胞表面的重新分布需要两个池的动员。这些数据确定了一般内体系统在GLUT4的特殊的、胰岛素调节的运输中的作用。通过一般内体系统的运输受rab11调节。在此,我们表明rab11是GLUT4从内体运输到特殊区室以及胰岛素诱导的向细胞表面转位所必需的,强调了一般内体途径在GLUT4特殊运输中的重要性。基于这些发现,我们提出了一个GLUT4运输的两步模型,其中一般内体循环区室在GLUT4的胰岛素调节运输中发挥特殊作用。这个基于区室的模型为在分子水平上理解胰岛素调节的运输提供了框架。

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