Hexokinase II-deficient Mice

Type 2 diabetes is characterized by decreased rates of insulin-stimulated glucose uptake and utilization, reduced hexokinase II mRNA and enzyme production, and low basal levels of glucose 6-phosphate in insulin-sensitive skeletal muscle and adipose tissues. Hexokinase II is primarily expressed in mu...

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Veröffentlicht in:The Journal of biological chemistry 1999-08, Vol.274 (32), p.22517-22523
Hauptverfasser: Heikkinen, Sami, Pietilä, Marko, Halmekytö, Maria, Suppola, Suvikki, Pirinen, Eija, Deeb, Samir S., Jänne, Juhani, Laakso, Markku
Format: Artikel
Sprache:eng
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Zusammenfassung:Type 2 diabetes is characterized by decreased rates of insulin-stimulated glucose uptake and utilization, reduced hexokinase II mRNA and enzyme production, and low basal levels of glucose 6-phosphate in insulin-sensitive skeletal muscle and adipose tissues. Hexokinase II is primarily expressed in muscle and adipose tissues where it catalyzes the phosphorylation of glucose to glucose 6-phosphate, a possible rate-limiting step for glucose disposal. To investigate the role of hexokinase II in insulin action and in glucose homeostasis as well as in mouse development, we generated a hexokinase II knock-out mouse. Mice homozygous for hexokinase II deficiency (HKII −/− ) died at approximately 7.5 days post-fertilization, indicating that hexokinase II is vital for mouse embryogenesis after implantation and before organogenesis. HKII +/− mice were viable, fertile, and grew normally. Surprisingly, even though HKII +/− mice had significantly reduced (by 50%) hexokinase II mRNA and activity levels in skeletal muscle, heart, and adipose tissue, they did not exhibit impaired insulin action or glucose tolerance even when challenged with a high-fat diet.
ISSN:0021-9258
1083-351X
DOI:10.1074/jbc.274.32.22517