Tissue-specific overexpression of lipoprotein lipase causes tissue-specific insulin resistance

  1. Jason K. Kim*,,
  2. Jonathan J. Fillmore,
  3. Yan Chen*,
  4. Chunli Yu,
  5. Irene K. Moore,
  6. Marc Pypaert,
  7. E. Peer Lutz§,
  8. Yuko Kako§,
  9. Wanda Velez-Carrasco,
  10. Ira J. Goldberg§,
  11. Jan L. Breslow, and
  12. Gerald I. Shulman*,,,**
  1. *Howard Hughes Medical Institute and Departments of Internal Medicine, Cellular and Molecular Physiology, and Cell Biology, Yale University School of Medicine, New Haven, CT 06510; §Department of Medicine, Columbia University, New York, NY 10032; and Laboratory of Biochemical Genetics and Metabolism, Rockefeller University, New York, NY 10021

  1. Contributed by Jan L. Breslow

Abstract

Insulin resistance in skeletal muscle and liver may play a primary role in the development of type 2 diabetes mellitus, and the mechanism by which insulin resistance occurs may be related to alterations in fat metabolism. Transgenic mice with muscle- and liver-specific overexpression of lipoprotein lipase were studied during a 2-h hyperinsulinemic–euglycemic clamp to determine the effect of tissue-specific increase in fat on insulin action and signaling. Muscle–lipoprotein lipase mice had a 3-fold increase in muscle triglyceride content and were insulin resistant because of decreases in insulin-stimulated glucose uptake in skeletal muscle and insulin activation of insulin receptor substrate-1-associated phosphatidylinositol 3-kinase activity. In contrast, liver–lipoprotein lipase mice had a 2-fold increase in liver triglyceride content and were insulin resistant because of impaired ability of insulin to suppress endogenous glucose production associated with defects in insulin activation of insulin receptor substrate-2-associated phosphatidylinositol 3-kinase activity. These defects in insulin action and signaling were associated with increases in intracellular fatty acid-derived metabolites (i.e., diacylglycerol, fatty acyl CoA, ceramides). Our findings suggest a direct and causative relationship between the accumulation of intracellular fatty acid-derived metabolites and insulin resistance mediated via alterations in the insulin signaling pathway, independent of circulating adipocyte-derived hormones.

Footnotes

  • ** To whom reprint requests should be addressed at: Howard Hughes Medical Institute, Yale University School of Medicine, Boyer Center for Molecular Medicine, 295 Congress Avenue, BCMM 254C, Box 9812, New Haven, CT 06536-8012. E-mail: gerald.shulman{at}yale.edu.

  • Abbreviations:
    IRS,
    insulin receptor substrate;
    LPL,
    lipoprotein lipase;
    EGP,
    endogenous glucose production;
    PI,
    phosphatidylinositol;
    PKC-θ,
    protein kinase C-theta
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  1. Published online before print June 5, 2001, doi: 10.1073/pnas.121164498 PNAS June 19, 2001 vol. 98 no. 13 7522-7527
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