Human skin fibroblasts from ‘normal’ subjects were found to possess at least two hexose transport systems. One system was responsible for the uptake of 2-deoxy-D-glucose (dGlc), D-glucose and D-galactose, whereas the other was responsible primarily for the uptake of 3-O-methyl-D-glucose (MeGlc). The transport of dGlc was the rate-limiting step in the uptake process; over 97% of the internalized dGlc was phosphorylated and the specific activity of hexokinase was several times higher than that for dGlc transport. The dGlc transport system was activated by glucose starvation, and was very sensitive to inhibition by cytochalasin B and energy uncouplers. Fibroblasts isolated from a patient with symptoms of hypoglycaemia were found to differ from their normal counterparts in the dGlc transport system. They exhibited a much higher transport affinity for dGlc, D-glucose and D-galactose, with no change in the respective transport capacity. Transport was not the rate-limiting step in dGlc uptake by these cells. Moreover, the patient's dGlc transport system was no longer sensitive to inhibition by cytochalasin B and energy uncouplers. This suggested that the intrinsic properties of the patient's dGlc transport system were altered. It should be noted that the patient's dGlc transport system could still be activated by glucose starvation. Despite the changes in the dGlc transport system, the MeGlc transport system in the patient's fibroblasts remained unaltered. The observed difference in the properties of the two hexose transport systems in the ‘normal’ and the patient's fibroblasts strongly suggests that the two transport systems may be coded or regulated by different genes. The present finding provides the first genetic evidence from naturally occurring fibroblasts indicating the presence of two different hexose transport systems.
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February 1990
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Research Article|
February 01 1990
Use of a genetic variant to study the hexose transport properties of human skin fibroblasts Available to Purchase
O T Mesmer;
O T Mesmer
*Department of Biochemistry, University of Western Ontario, London, Ontario, Canada N6A 5C1
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B A Gordon;
B A Gordon
†Childrenɴs Psychiatric Research Institute, Sanatorium Road, London, Ontario, Canada N6A 4G6
‡Department of Paediatrics, University of Western Ontario, Children's Hospital of Western Ontario, 800 Commissioners Road E., London, Ontario, Canada N6A 4G5
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C A Rupar;
C A Rupar
†Childrenɴs Psychiatric Research Institute, Sanatorium Road, London, Ontario, Canada N6A 4G6
‡Department of Paediatrics, University of Western Ontario, Children's Hospital of Western Ontario, 800 Commissioners Road E., London, Ontario, Canada N6A 4G5
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T C Y Lo
T C Y Lo
*Department of Biochemistry, University of Western Ontario, London, Ontario, Canada N6A 5C1
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Publisher: Portland Press Ltd
Online ISSN: 1470-8728
Print ISSN: 0264-6021
© 1990 London: The Biochemical Society
1990
Biochem J (1990) 265 (3): 823–829.
Citation
O T Mesmer, B A Gordon, C A Rupar, T C Y Lo; Use of a genetic variant to study the hexose transport properties of human skin fibroblasts. Biochem J 1 February 1990; 265 (3): 823–829. doi: https://doi.org/10.1042/bj2650823
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