Direct inhibition of the hexose transporter GLUT1 by tyrosine kinase inhibitors

Vera, JC; Reyes, AM; Velasquez, FV; Rivas, CI; Zhang, RH; Strobel P.; Slebe, JC; Nunez-Alarcon, J; Golde, DW

Abstract

The facilitative hexose transporter GLUT1 is a multifunctional protein that transports hexoses and dehydroascorbic acid, the oxidized form of vitamin C, and interacts with several molecules structurally unrelated to the transported substrates. Here we analyzed in detail the interaction of GLUT1 with a group of tyrosine kinase inhibitors that include natural products of the family of flavones and isoflavones and synthetic compounds such as the tyrphostins. These compounds inhibited, in a dose-dependent manner, the transport of hexoses and dehydroascorbic acid in human myeloid HL-60 cells, in transfected Chinese hamster ovary cells overexpressing GLUT1, and in normal human erythrocytes, and blocked the glucose-displaceable binding of cytochalasin B to GLUT1 in erythrocyte ghosts. Kinetic analysis of transport data indicated that only tyrosine kinase inhibitors with specificity for ATP binding sites inhibited the transport activity of GLUT1 in a competitive manner. In contrast, those inhibitors that are competitive with tyrosine but not with ATP failed to inhibit hexose uptake or did so in a noncompetitive manner. These results, together with recent evidence demonstrating that GLUT1 is a nucleotide binding protein, support the concept that the inhibitory effect on transport is related to the direct interaction of the inhibitors with GLUT1. We conclude that predicted nucleotide-binding motifs present in GLUT1 are important for the interaction of the tyrosine kinase inhibitors with the transporter and may participate directly in the binding transport of substrates by GLUT1.

Más información

Título según WOS: Direct inhibition of the hexose transporter GLUT1 by tyrosine kinase inhibitors
Título según SCOPUS: Direct inhibition of the hexose transporter GLUT1 by tyrosine kinase inhibitors
Título de la Revista: BIOCHEMISTRY
Volumen: 40
Número: 3
Editorial: AMER CHEMICAL SOC
Fecha de publicación: 2001
Página de inicio: 777
Página final: 790
Idioma: English
URL: http://pubs.acs.org/doi/abs/10.1021/bi001660j
DOI:

10.1021/bi001660j

Notas: ISI, SCOPUS