Activation of G-protein coupled fMLP or PAF receptor directly triggers glucose transporter type 1 (GLUT1) translocation in Chinese hamster ovary (CHO) cells stably expressing fMLP or PAF receptor.

A. Hagi, H. Hayashi, K. Kishi, L. Wang, Y. Ebina
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引用次数: 6

Abstract

The chemoattractants, fMLP and PAF, stimulate glucose uptake in phagocytes to obtain an energy source for host defense. Glucose uptake in phagocytes is mainly regulated via glucose transporter type 1 (GLUT1). To examine molecular mechanisms of facilitated glucose uptake in response to fMLP or PAF, we established CHO cells stably expressing fMLP or PAF receptor with c-myc epitope tagged GLUT1 which could immunologically detect GLUT1 on the cell surface. In the CHO cells, both fMLP and PAF directly triggered GLUT1 translocation from the intracellular pool to the cell surface, and stimulated glucose uptake. Therefore, in phagocytes, we propose that fMLP and PAF also trigger GLUT1 translocation to stimulate glucose uptake as an energy source for host defense.
g蛋白偶联fMLP或PAF受体的激活直接触发葡萄糖转运蛋白1型(GLUT1)在稳定表达fMLP或PAF受体的中国仓鼠卵巢(CHO)细胞中的易位。
趋化剂fMLP和PAF刺激吞噬细胞摄取葡萄糖,为宿主防御提供能量来源。吞噬细胞的葡萄糖摄取主要通过葡萄糖转运蛋白1 (GLUT1)调节。为了研究fMLP或PAF促进葡萄糖摄取的分子机制,我们建立了稳定表达fMLP或PAF受体的CHO细胞,其c-myc表位标记为GLUT1,可以免疫检测细胞表面的GLUT1。在CHO细胞中,fMLP和PAF均直接触发GLUT1从细胞内池向细胞表面的易位,并刺激葡萄糖摄取。因此,在吞噬细胞中,我们提出fMLP和PAF也触发GLUT1易位,刺激葡萄糖摄取作为宿主防御的能量来源。
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