Abstract

The phosphorylated form of rat pp63, a hepatic glycoprotein, selectively inhibits both insulin receptor tyrosine kinase activity (IR-TKA) and insulin-mediated growth promotion, but does not affect several other insulin-mediated activities. Our new data suggest that the human protein, alpha2-HS-glycoprotein (alpha2-HSG), in its phosphorylated form, functions similarly to rat pp63 in inhibiting IR autophosphorylation, IR-TKA and insulin-dependent mitogenesis in a dose-dependent fashion, non-competitive with respect to insulin. Since our long-term objective is to investigate the role of IR-TKA in both the normal and insulin-resistant states of rats and humans, this dissection of insulin-mediated cellular functions, by pp63/alpha2-HSG, provides us with a novel approach. Using this natural IR-TKA inhibitor, we can now examine the role of IR-TKA in the delivery of specific insulin-mediated signals.
Our specific aims i nclude: (1) Investigation of effects of pp63/alpha2-HSG on metabolic and mitogenic actions of insulin and on functions of the insulin receptor in a rat hepatoma cell line, Epstein-Barr Virus transformed lymphocytes and transfected rat fibroblasts expressing normal insulin receptors, (2) Examination of synthesis and secretion of pp63/alpha2-HSG and characterization of specific activity of circulating pp63/alpha2-HSG in rat and human insulin resistant states in vivo (high-fat diet and obesity, respectively), (3) Examination of mechanisms underlying these observations by utilizing human insulin receptor mutants as well as monoclonal antibodies to the insulin receptor and to pp63/alpha2-HSG for modifying pp63/alpha2-HSG - insulin receptor interaction. Our preliminary data demonstrate that pp63 gene expression directly correlates with the degree of insulin resistance, in a rat high-fat diet model. These date support our contention that studies on regulation of pp63/alpha2-HSG specific activity will yield information critical to our understanding of impairment of insulin signaling in insulin-resistant conditions (diabetes mellitus, hypertension, obesity, and dyslipidemia).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK044382-03
Application #
2143769
Study Section
Metabolism Study Section (MET)
Project Start
1992-09-30
Project End
1995-09-29
Budget Start
1994-09-30
Budget End
1995-09-29
Support Year
3
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Wayne State University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
City
Detroit
State
MI
Country
United States
Zip Code
48202

  Publications

Mathews, Suresh T; Singh, Gurmant P; Ranalletta, Mollie et al. (2002) Improved insulin sensitivity and resistance to weight gain in mice null for the Ahsg gene. Diabetes 51:2450-8
Cintron, V J; Ko, M S; Chi, K D et al. (2001) Genetic mapping and functional studies of a natural inhibitor of the insulin receptor tyrosine kinase: the mouse ortholog of human alpha2-HS glycoprotein. Int J Exp Diabetes Res 1:249-63
Srinivas, P R; Deutsch, D D; Mathews, S T et al. (1996) Recombinant human alpha 2-HS glycoprotein inhibits insulin-stimulated mitogenic pathway without affecting metabolic signalling in Chinese hamster ovary cells overexpressing the human insulin receptor. Cell Signal 8:567-73
Srinivas, P R; Goustin, A S; Grunberger, G (1995) Baculoviral expression of a natural inhibitor of the human insulin receptor tyrosine kinase. Biochem Biophys Res Commun 208:879-85
Srinivas, P R; Grunberger, G (1994) Inhibitors of the insulin receptor tyrosine kinase. Pharmacol Ther 64:23-35
Srinivas, P R; Wagner, A S; Reddy, L V et al. (1993) Serum alpha 2-HS-glycoprotein is an inhibitor of the human insulin receptor at the tyrosine kinase level. Mol Endocrinol 7:1445-55