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胰岛素受体对突触融合蛋白 4 的磷酸化作用驱动出胞 SNARE 复合物的形成,将 GLUT4 递送至细胞表面。

Phosphorylation of Syntaxin 4 by the Insulin Receptor Drives Exocytic SNARE Complex Formation to Deliver GLUT4 to the Cell Surface.

机构信息

Department of Biology, University of York, Heslington YO10 5DD, UK.

Institute of Molecular Cell and Systems Biology, College of Medical Veterinary and Life Sciences, University of Glasgow, Glasgow G12 8QQ, UK.

出版信息

Biomolecules. 2023 Dec 2;13(12):1738. doi: 10.3390/biom13121738.

Abstract

A major consequence of insulin binding its receptor on fat and muscle cells is the stimulation of glucose transport into these tissues. This is achieved through an increase in the exocytic trafficking rate of the facilitative glucose transporter GLUT4 from intracellular stores to the cell surface. Delivery of GLUT4 to the cell surface requires the formation of functional SNARE complexes containing Syntaxin 4, SNAP23, and VAMP2. Insulin stimulates the formation of these complexes and concomitantly causes phosphorylation of Syntaxin 4. Here, we use a combination of biochemistry and cell biological approaches to provide a mechanistic link between these observations. We present data to support the hypothesis that Tyr-115 and Tyr-251 of Syntaxin 4 are direct substrates of activated insulin receptors, and that these residues modulate the protein's conformation and thus regulate the rate at which Syntaxin 4 forms SNARE complexes that deliver GLUT4 to the cell surface. This report provides molecular details on how the cell regulates SNARE-mediated membrane traffic in response to an external stimulus.

摘要

胰岛素与其在脂肪和肌肉细胞上的受体结合的一个主要后果是刺激葡萄糖向这些组织中的转运。这是通过增加易化葡萄糖转运蛋白 GLUT4 从细胞内储存到细胞表面的胞吐转运速率来实现的。GLUT4 递送到细胞表面需要形成包含 Syntaxin 4、SNAP23 和 VAMP2 的功能性 SNARE 复合物。胰岛素刺激这些复合物的形成,并同时导致 Syntaxin 4 的磷酸化。在这里,我们使用生物化学和细胞生物学方法的组合,为这些观察结果之间提供了一种机制联系。我们提供的数据支持了以下假设:Syntaxin 4 的 Tyr-115 和 Tyr-251 是激活的胰岛素受体的直接底物,这些残基调节蛋白质的构象,从而调节 Syntaxin 4 形成将 GLUT4 递送到细胞表面的 SNARE 复合物的速率。本报告提供了关于细胞如何响应外部刺激调节 SNARE 介导的膜运输的分子细节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e6ad/10741561/c4cb7ad67dad/biomolecules-13-01738-g001.jpg

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