Literature DB >> 12082147

Functional consequence of targeting protein kinase B/Akt to GLUT4 vesicles.

Pierre-Henri Ducluzeau1, Laura M Fletcher, Gavin I Welsh, Jeremy M Tavaré.   

Abstract

We have investigated the role of protein kinase B (Akt) in the insulin-stimulated translocation of vesicles containing the insulin-responsive isoform of glucose transporter (GLUT4) to the plasma membrane of adipocytes. Previous reports have suggested that protein kinase B can bind to intracellular GLUT4 vesicles in an insulin-dependent manner, but the functional consequence of this translocation is not known. In this study we have artificially targeted constitutively active and kinase-inactive mutants of protein kinase B to intracellular GLUT4 vesicles by fusing them with the N-terminus of GLUT4 itself. We examined the effect of these mutants on the insulin-dependent translocation of the insulin-responsive amino peptidase IRAP (a bona fide GLUT4-vesicle-resident protein). A kinase-inactive protein kinase B targeted to GLUT4 vesicles was an extremely effective dominant-negative inhibitor of insulin-stimulated IRAP translocation to the plasma membrane. By contrast, a kinase-inactive protein kinase B expressed in the cytoplasm did not have an effect. The results suggest that protein kinase B has an important functional role at, or in the vicinity of, GLUT4 vesicles in the insulin-dependent translocation of those vesicles to the plasma membrane of adipocytes.

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Year:  2002        PMID: 12082147     DOI: 10.1242/jcs.115.14.2857

Source DB:  PubMed          Journal:  J Cell Sci        ISSN: 0021-9533            Impact factor:   5.285


  9 in total

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7.  Distinct Akt phosphorylation states are required for insulin regulated Glut4 and Glut1-mediated glucose uptake.

Authors:  Muheeb Beg; Nazish Abdullah; Fathima Shazna Thowfeik; Nasser K Altorki; Timothy E McGraw
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8.  Mild electrical stimulation with heat shock ameliorates insulin resistance via enhanced insulin signaling.

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9.  Resveratrol enhances GLUT-4 translocation to the caveolar lipid raft fractions through AMPK/Akt/eNOS signalling pathway in diabetic myocardium.

Authors:  S Varma Penumathsa; M Thirunavukkarasu; L Zhan; G Maulik; V P Menon; D Bagchi; N Maulik
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  9 in total

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