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葡萄糖转运蛋白8(GLUT8)含有一个[DE]XXXL[LI]分选基序,并定位于晚期内体/溶酶体区室。

GLUT8 contains a [DE]XXXL[LI] sorting motif and localizes to a late endosomal/lysosomal compartment.

作者信息

Augustin Robert, Riley Joan, Moley Kelle H

机构信息

Institute for Human Nutrition, Department of Pharmacology, 14482 Potsdam-Rehbrücke, Germany.

出版信息

Traffic. 2005 Dec;6(12):1196-212. doi: 10.1111/j.1600-0854.2005.00354.x.

Abstract

Glucose transporter 8 (GLUT8) contains a cytoplasmic N-terminal dileucine motif and localizes to a thus far unidentified intracellular compartment. Translocation of GLUT8 to the plasma membrane (PM) was found in insulin-treated mouse blastocysts. Using overexpression of GLUT8 in adipocytes and neuronal cells however, insulin treatment or depolarization of the cells did not lead to GLUT8 PM translocation in other studies. In addition, other experiments showing dynamin-dependent endocytosis of GLUT8 suggested that GLUT8 recycles between an endosomal compartment and the PM. To reveal the functional/physiological role of GLUT8, we studied its subcellular localization in 3T3L1, HEK293 and CHO cells. We show that GLUT8 does not co-localize with GLUT4 and does not redistribute to the PM after treatment with insulin, ionophores or okadaic acid in these cell lines. Once endocytosed, GLUT8 does not recycle to the PM. GLUT8 localizes to late endosomes and lysosomes. An interspecies GLUT8 - sequence alignment revealed the presence of a highly conserved late endosomal/lysosomal-targeting motif ([DE]XXXL[LI]). Changing the glutamate to arginine as found in GLUT4 (RRXXXLL) alters GLUT8 endocytosis and retains the transporter at the PM. Furthermore, sorting GLUT8 to late endosomes/lysosomes does not require prior presence of GLUT8 at the PM followed by its endocytosis. In summary, GLUT8 does not reside in a recycling vesicle pool and is distinct from GLUT4. From our data, we postulate a role for GLUT8 in transport of hexoses across intracellular membranes, for example in specific compartments of GLUT8 expression such as the acrosome of mature spermatozoa or secretory granules in neurons. Furthermore, a role for GLUT8 in hexose transport across the lysosomal membrane, a transport mechanism that has long been suggested but unexplained, is discussed.

摘要

葡萄糖转运蛋白8(GLUT8)含有一个位于细胞质的N端双亮氨酸基序,并定位于一个迄今尚未明确的细胞内区室。在胰岛素处理的小鼠囊胚中发现GLUT8易位至质膜(PM)。然而,在其他研究中,通过在脂肪细胞和神经元细胞中过表达GLUT8,胰岛素处理或细胞去极化并未导致GLUT8易位至质膜。此外,其他实验表明GLUT8的内吞作用依赖发动蛋白,这表明GLUT8在内体区室和质膜之间循环。为了揭示GLUT8的功能/生理作用,我们研究了其在3T3L1、HEK293和CHO细胞中的亚细胞定位。我们发现,在这些细胞系中,GLUT8与GLUT4不共定位,在用胰岛素、离子载体或冈田酸处理后也不会重新分布到质膜。一旦被内吞,GLUT8不会再循环至质膜。GLUT8定位于晚期内体和溶酶体。种间GLUT8序列比对显示存在一个高度保守的晚期内体/溶酶体靶向基序([DE]XXXL[LI])。将谷氨酸替换为GLUT4中发现的精氨酸(RRXXXLL)会改变GLUT8的内吞作用,并使转运蛋白保留在质膜上。此外,将GLUT8分选至晚期内体/溶酶体并不需要GLUT8事先存在于质膜上然后再被内吞。总之,GLUT8并不存在于再循环囊泡池中,且与GLUT4不同。根据我们的数据,我们推测GLUT8在己糖跨细胞内膜的转运中发挥作用,例如在GLUT8表达的特定区室中,如成熟精子的顶体或神经元中的分泌颗粒。此外,还讨论了GLUT8在己糖跨溶酶体膜转运中的作用,这一转运机制长期以来一直被提出但未得到解释。

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