Litcius/Paper detail

Lysosomal trafficking of the glucose transporter GLUT1 requires sequential regulation by TXNIP and ubiquitin

Susan J Qualls-Histed, Casey P. Nielsen, Jason A. MacGurn

2023iScience38 citationsDOIOpen Access PDF

Abstract

Glucose transporters are gatekeepers of cellular glucose metabolism. Understanding how their activity is regulated can provide insight into mechanisms of glucose homeostasis and diseases arising from dysregulation of glucose transport. Glucose stimulates endocytosis of the human glucose transporter GLUT1, but several important questions remain surrounding the intracellular trafficking itinerary of GLUT1. Here, we report that increased glucose availability triggers lysosomal trafficking of GLUT1 in HeLa cells, with a subpopulation of GLUT1 routed through ESCRT-associated late endosomes. This itinerary requires the arrestin-like protein TXNIP, which interacts with both clathrin and E3 ubiquitin ligases to promote GLUT1 lysosomal trafficking. We also find that glucose stimulates GLUT1 ubiquitylation, which promotes its lysosomal trafficking. Our results suggest that excess glucose first triggers TXNIP-mediated endocytosis of GLUT1 and, subsequently, ubiquitylation to promote lysosomal trafficking. Our findings underscore how complex coordination of multiple regulators is required for fine-tuning of GLUT1 stability at the cell surface.

Topics & Concepts

GLUT1Glucose transporterEndocytosisUbiquitinCell biologyEndosomeUbiquitin ligaseGlucose Transporter Type 1BiologyGlucose uptakeChemistryIntracellularBiochemistryCellInsulinEndocrinologyGeneCellular transport and secretionCalcium signaling and nucleotide metabolismMetabolism, Diabetes, and Cancer