Abstract

This is a revised application originally designed to test the idea that specific protein tyrosine phosphatases (PTPases) have a role in regulation of the reversible tyrosine phosphorylation of the insulin receptor (IR) and its substrates. The PI's laboratory has provided compelling evidence for the involvement of PTPases in negative regulation of insulin action. Specifically, leucocyte common antigen related """"""""LAR"""""""" PTPase, a transmembrane receptor-type enzyme and PTP1B, a non-receptor-type phosphatase have been shown, by loading cells with neutralizing antibodies and by use of anti-sense methods, to dephosphorylate the insulin receptor and thus affect insulin action. Several submitted manuscripts document that LAR overexpression downregulates the effect of insulin as predicted if LAR inactivates the insulin receptor by dephosphorylation. An additional manuscript documents the physical interaction of LAR with the insulin receptor using anti-LAR antibodies to immunoprecipitate the LAR-IR complex. Paradoxically, LAR knockout mice appear phenotypically normal indicating there must be a redundant pathway. The present application proposes to: 1) Further characterize how LAR and PTP1B modulate the insulin receptor kinase in intact cells by osmotic loading of inhibitory antibodies and by cell transfections with constructs expressing dominant negative LAR. The proposed studies include looking at the phosphorylation state of IRS-1, Shc and the insulin receptor, and determining if LAR is co-localized in the endoplasmic reticulum with the insulin receptor. 2) Determine the molecular mechanism by which LAR and PTP1B regulate the kinase activity of the insulin receptor. Studies on the physical interaction of LAR and PTP1B with the insulin receptor are proposed along with determination of which tyrosines in the insulin receptor are dephosphorylated by these PTPases. 3) Evaluate whether certain PTPases have a catalytic specificity towards functional phosphotyrosines on IRS-1 and Shc as measured by PTPase induced changes in complex formation with adaptor proteins in vitro.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK043396-08
Application #
2838118
Study Section
Special Emphasis Panel (ZRG2-GMA-2 (01))
Program Officer
Margolis, Ronald N
Project Start
1991-08-01
Project End
2000-11-30
Budget Start
1998-12-21
Budget End
1999-11-30
Support Year
8
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Thomas Jefferson University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
061197161
City
Philadelphia
State
PA
Country
United States
Zip Code
19107

  Publications

Tang, Tao; Thompson, Joel C; Wilson, Patricia G et al. (2013) Decreased body fat, elevated plasma transforming growth factor-? levels, and impaired BMP4-like signaling in biglycan-deficient mice. Connect Tissue Res 54:5-13
Wu, Xiangdong; Chen, Keyang; Williams, Kevin Jon (2012) The role of pathway-selective insulin resistance and responsiveness in diabetic dyslipoproteinemia. Curr Opin Lipidol 23:334-44
Wu, Xiangdong; Williams, Kevin Jon (2012) NOX4 pathway as a source of selective insulin resistance and responsiveness. Arterioscler Thromb Vasc Biol 32:1236-45
Chen, Keyang; Liu, Ming-Lin; Schaffer, Lana et al. (2010) Type 2 diabetes in mice induces hepatic overexpression of sulfatase 2, a novel factor that suppresses uptake of remnant lipoproteins. Hepatology 52:1957-67
Williams, Kevin Jon; Chen, Keyang (2010) Recent insights into factors affecting remnant lipoprotein uptake. Curr Opin Lipidol 21:218-28
Goldstein, Barry J (2008) Inflammatory signaling: another drug target to improve glycemic control in type 2 diabetes. Clin Transl Sci 1:43-4
Hu, Taishan; Ramachandrarao, Satish P; Siva, Senthuran et al. (2005) Reactive oxygen species production via NADPH oxidase mediates TGF-beta-induced cytoskeletal alterations in endothelial cells. Am J Physiol Renal Physiol 289:F816-25
Goldstein, Barry J; Mahadev, Kalyankar; Kalyankar, Mahadev et al. (2005) Redox paradox: insulin action is facilitated by insulin-stimulated reactive oxygen species with multiple potential signaling targets. Diabetes 54:311-21
Wu, Xiangdong; Zhu, Li; Zilbering, Assaf et al. (2005) Hyperglycemia potentiates H(2)O(2) production in adipocytes and enhances insulin signal transduction: potential role for oxidative inhibition of thiol-sensitive protein-tyrosine phosphatases. Antioxid Redox Signal 7:526-37
Goldstein, Barry J; Mahadev, Kalyankar; Wu, Xiangdong et al. (2005) Role of insulin-induced reactive oxygen species in the insulin signaling pathway. Antioxid Redox Signal 7:1021-31

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