Abstract

The major objective of this proposal will be to gain greater insight into the molecular and cell biological mechanisms underlying the production of insulin and other peptide hormones of the islet of Langerhans, including their genetic bases, evolutionary origins and disorders which may contribute to the pathophysiology of diabetes and/or other diseases in man. Extensions of previous work and new projects are proposed in 8 areas: (1) Studies on the proteolytic mechanisms involved in the processing of prohormones, e.g. proinsulin, including the initiation of studies on the biosynthesis and transport of cathespin B precursors in islet cells, the mechanisms of targeting and activation of cathespin B precursors in secretion granules versus lysosomes, and investigation via molecular cloning of the complexity and tissue distribution of the multigene family of tissue proteinases containing cysteine in their active centers (cathespins B, H, L and papain). (2) Regulation of insulin biosynthesis in cells via translation and transcriptional control mechanisms, including the identification of regions in the insulin gene that may play a role in regulation of insulin production. (3) Studies on defects in insulin biosynthesis and structure due to mutations in the insulin gene, or others, and through development of improved genetic screening methods, evaluation of their contribution to the incidence of various forms of diabetes. (4) Studies on the evolution of insulin and related gene products, with particular emphasis on extending present studies to invertebrates and other more primitive species. (5) Studies on islet-central nervous system interrelationships, including studies via molecular cloning on the precursors of pancreatic polypeptide and TRH in islets and their counterparts in brain, as well as on the extra-pancreatic expression of insulin genes. (6) Development of new approaches to the molecular cloning and primary structural analysis of insulin receptors and their precursor forms. (7) New approaches to the study of prohormone structure and function via use of monoclonal antibodies or via expression, by means of DNA-mediated gene transfer methods, of altered precursor molecules having site-specific mutations that may affect their synthesis, folding, intracellular transport and routing, conversion to active forms or ultimate secretion and function as active hormones. (8) New studies on tumorigenesis in islet cells directed towards elucidating the possible roles of various cellular oncogenes in the genesis of islet cell tumors in man and animals and exploring the possible use of modified cellular oncogenes or their viral counterparts to generate new islet cell lines for investigational use.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK013914-20
Application #
3225161
Study Section
Metabolism Study Section (MET)
Project Start
1974-11-01
Project End
1989-11-30
Budget Start
1988-12-01
Budget End
1989-11-30
Support Year
20
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
University of Chicago
Department
Type
Schools of Medicine
DUNS #
225410919
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Park, Soo-Young; Ludwig, Michael Z; Tamarina, Natalia A et al. (2014) Genetic complexity in a Drosophila model of diabetes-associated misfolded human proinsulin. Genetics 196:539-55
Menting, John G; Yang, Yanwu; Chan, Shu Jin et al. (2014) Protective hinge in insulin opens to enable its receptor engagement. Proc Natl Acad Sci U S A 111:E3395-404
He, Bin Z; Ludwig, Michael Z; Dickerson, Desiree A et al. (2014) Effect of genetic variation in a Drosophila model of diabetes-associated misfolded human proinsulin. Genetics 196:557-67
Menting, John G; Whittaker, Jonathan; Margetts, Mai B et al. (2013) How insulin engages its primary binding site on the insulin receptor. Nature 493:241-5
Stein, Jeffrey; Milewski, Wieslawa M; Dey, Arunangsu (2013) The negative cell cycle regulators, p27(Kip1), p18(Ink4c), and GSK-3, play critical role in maintaining quiescence of adult human pancreatic ?-cells and restrict their ability to proliferate. Islets 5:156-69
Steiner, Donald F (2011) On the discovery of precursor processing. Methods Mol Biol 768:3-11
Stein, Jeffrey; Milewski, Wieslawa M; Hara, Manami et al. (2011) GSK-3 inactivation or depletion promotes ýý-cell replication via down regulation of the CDK inhibitor, p27 (Kip1). Islets 3:21-34
Steiner, Donald F (2011) Adventures with insulin in the islets of Langerhans. J Biol Chem 286:17399-421
Smith, Brian J; Huang, Kun; Kong, Geoffrey et al. (2010) Structural resolution of a tandem hormone-binding element in the insulin receptor and its implications for design of peptide agonists. Proc Natl Acad Sci U S A 107:6771-6
Wardman, Jonathan H; Zhang, Xin; Gagnon, Sandra et al. (2010) Analysis of peptides in prohormone convertase 1/3 null mouse brain using quantitative peptidomics. J Neurochem 114:215-25

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