Abstract

In response to the Request for Applications for Applications #DK 01-009, entitled """"""""Mouse Models of Diabetic Complications Consortium,"""""""" the Mouse Diabetic Nephropathy and Neuropathy United (MDNNU) at the University of Michigan will develop models of diabetic neuropathy and neuropathy in mice via state-of-the-art mouse engineering. The technology that emphasizes cell-type specific knockout strategies manipulating genes that will predispose diabetic mice to these two diabetic complications. The unit will comprise a number of investigators at the University of Michigan and two investigators at Johns Hopkins University, who have wide-ranging experience and expertise in mouse genetic engineering, mouse model investigation, and diabetic phenotyping. Rodent models of diabetes fail to develop changes that closely resemble human diabetic nephropathy or neuropathy. The reasons for the resistance to full-blown complications are likely manifold, but may include absence of important genetic susceptibility genes and, more simply, the life-span of rodents that is too limited to allow full development of complications. Our general strategic approach to this dilemma is to accelerate the injury of diabetes is predisposing critical cells in both the renal glomerulus and peripheral nerve to injury. Our strategy will be simpler: to alter expression of gene products known to be associated with cellular injury and which appear to be involved in diabetic complications, in order to directly prime glomerular and peripheral nerve cells in a cell type- and temporally-specific manner for injury once diabetes occurs. If successful, these models will show rapid progression of diabetic injury, will be easy and inexpensive to study because of this rapid and reproducible downhill course, and will provide excellent models for evaluation of potential therapeutic interventions. To best address the goals of this initiative to develop novel models of diabetic nephropathy and neuropathy, we will pursue the following aims: 1. Induce diabetes in mice which are null, heterozygote, or wild type for mitochondrial superoxide dismutase (SOD2). 2. Induce diabetes in mice which are null, heterozygote, or wild type for gamma glutamate cysteine ligase (GCLC). 3. Phenotype SOD2 and GCLC diabetic and control mice for nephopathy and neuropathy. 4. Create tetracycline-regulatable Cre-lox conditional knockout mice specific for peripheral neuron and/or podocyte-specific knockout of SOD2 and GCLC. 5. Fully develop and phenotype the cell-type specific conditional knockouts as suggested by phenotypic results in conventional knockouts.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01DK060994-02
Application #
6524678
Study Section
Special Emphasis Panel (ZDK1-GRB-4 (O2))
Program Officer
Ketchum, Christian J
Project Start
2001-09-30
Project End
2004-08-31
Budget Start
2002-09-01
Budget End
2003-08-31
Support Year
2
Fiscal Year
2002
Total Cost
$518,000
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
791277940
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Zhang, Hongyu; Nair, Viji; Saha, Jharna et al. (2017) Podocyte-specific JAK2 overexpression worsens diabetic kidney disease in mice. Kidney Int 92:909-921
Brosius, Frank C; Tuttle, Katherine R; Kretzler, Matthias (2016) JAK inhibition in the treatment of diabetic kidney disease. Diabetologia 59:1624-7
Brosius 3rd, Frank C; He, John Cijiang (2015) JAK inhibition and progressive kidney disease. Curr Opin Nephrol Hypertens 24:88-95
Dauch, Jacqueline R; Bender, Diane E; Luna-Wong, LucĂ­a A et al. (2013) Neurogenic factor-induced Langerhans cell activation in diabetic mice with mechanical allodynia. J Neuroinflammation 10:64
Cheng, Hsinlin T; Dauch, Jacqueline R; Porzio, Michael T et al. (2013) Increased axonal regeneration and swellings in intraepidermal nerve fibers characterize painful phenotypes of diabetic neuropathy. J Pain 14:941-7
Cheng, Hsinlin T; Dauch, Jacqueline R; Hayes, John M et al. (2012) Nerve growth factor/p38 signaling increases intraepidermal nerve fiber densities in painful neuropathy of type 2 diabetes. Neurobiol Dis 45:280-7
Dauch, Jacqueline R; Yanik, Brandon M; Hsieh, Wilson et al. (2012) Neuron-astrocyte signaling network in spinal cord dorsal horn mediates painful neuropathy of type 2 diabetes. Glia 60:1301-15
Kumar, P Anil; Brosius 3rd, Frank C; Menon, Ram K (2011) The glomerular podocyte as a target of growth hormone action: implications for the pathogenesis of diabetic nephropathy. Curr Diabetes Rev 7:50-5
Cheng, Hsinlin T; Dauch, Jacqueline R; Oh, Sang Su et al. (2010) p38 mediates mechanical allodynia in a mouse model of type 2 diabetes. Mol Pain 6:28
Wang, Youli; Heilig, Kathleen; Saunders, Thomas et al. (2010) Transgenic overexpression of GLUT1 in mouse glomeruli produces renal disease resembling diabetic glomerulosclerosis. Am J Physiol Renal Physiol 299:F99-F111

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