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The glucose sensor in HIT cells is the glucose transporter
Author(s) -
Ashcroft Stephen J.H.,
Stubbs Mark
Publication year - 1987
Publication title -
febs letters
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.593
H-Index - 257
eISSN - 1873-3468
pISSN - 0014-5793
DOI - 10.1016/0014-5793(87)80242-9
Subject(s) - glucose transporter , cytochalasin b , phloretin , snf3 , glut1 , insulin , medicine , glucose uptake , carbohydrate metabolism , endocrinology , glut2 , glut4 , transporter , chemistry , mannose , metabolism , glucose transporter type 1 , biochemistry , biology , cell , gene
The nature of the rate‐limiting step for glucose utilization by the clonal insulin‐producing cell line HIT‐T15 has been investigated. In contrast to the situation in islets of Langerhans, we find that the HIT cell glucose metabolism is limited by the rate of entry of glucose into the cell. This is evidenced by the low rate of sugar transport and by the marked reduction in the rate of glucose utilization elicited by inhibitors of the glucose transporter. As judged by competition with glucose, the HIT cell glucose transporter also transports mannose, 2‐deoxyglucose and 3‐ O ‐methylglucose but not L‐glucose or N ‐acetylglucosamine. The K m for glucose of the glucose transporter, measured as the concentration of glucose required for a half‐maximal rate of glucose utilization, is 4.3 mM, similar to the concentration reported to give half‐maximal insulin release. Glucose‐stimulated insulin release from HIT cells is inhibited by phloretin or cytochalasin B but not by mannoheptulose. We conclude that the secretory responses of HIT cells are consistent with the substrate‐site hypothesis, but that, in contrast to normal B‐cells, the glucose sensor which confers concentration‐dependence and specificity to sugar‐stimulated insulin release, is the glucose transporter.