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Activation of PI 3-kinase by the hexosamine biosynthesis pathway |
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| Authors: | Filippis Christine Filippis Anthony Clark Stella Proietto Joseph |
| Institution: | Division of Endocrinology and Metabolism, Lady Davis Institute for Medical Research, Jewish General Hospital, McGill University, Room E-162, 3755 Chemin de la Côte-Ste-Catherine, Montreal, Quebec, Canada H3T 1E2 |
| Abstract: | It has been shown that hyperglycaemia-induced defects in glucose transport and insulin action are mediated by increased flux of excess glucose through the hexosamine biosynthesis pathway (HBP). We have previously demonstrated that in rat adipocytes, increased flux through the HBP activates protein kinase C (PKC). The aim of the present study was to explore the mechanism for HBP-mediated activation of PKC. We show that activation of the HBP by either high glucose or glucosamine causes the translocation of PKC-zeta/lambda and PKC-epsilon but not other PKC isoforms tested (alpha, beta, delta). This translocation was inhibited by wortmannin, a PI 3-kinase inhibitor. Both high glucose and glucosamine caused widespread cellular activation of PI 3-kinase. We demonstrate that HBP-mediated activation of PI 3-kinase has an insulin-like effect to translocate GLUT4. We conclude that an acute increase of glucose flux through the HBP activates PI 3-kinase. |
| Keywords: | β-Adrenergic receptors β3-Adrenergic receptor gene Glucocorticoids Dexamethasone Gene expression regulation Brown adipose tissue Thermogenesis Lipolysis Energy expenditure |
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