Abstract

(taken from the application) Diabetes mellitus is a significant health problem, affecting approximately 16 million people in the United States. Loss of sufficient insulin production by the pancreatic beta cell is a hallmark of both type I and type II diabetes. The homeobox transcription factor Pdx1 (pancreatic and duodenal homeobox gene 1; also known as IPF-1, IDX-1, STF-1) is a master regulator of pancreatic development, as its homozygous deletion leads to pancreatic agenesis in mice and men. In addition, heterozygous mutation of Pdx1/IPF-1 is linked to early onset non-insulin dependent diabetes mellitus (MODY4). Recently, the winged helix transcription factor HNF (hepatocyte nuclear factor) 3Beta was shown to be an important regulator of Pdx1 transcription in the developing pancreas. Consequently, it is likely that HNF3Beta plays an important role in the control of pancreatic development and that HNF3Beta mutations can contribute to the pathogenesis of diabetes. However, gene targeting of HNF3Beta has thus far been not informative in this regard, as embryos homozygous for a null mutation die before the onset of pancreatic development. Therefore, we propose to assess the function of HNF3Beta in pancreatic development and physiology through conditional gene targeting using the loxP/Cre recombinase system. In preliminary work required for this proposal we have already generated and tested mice homozygous for a loxP-flanked HNF3Beta gene, the HNF3BetaloxP/loxP mice, and obtained Beta-cell specific Cre-recombinase transgenic mice.
The specific aims of this proposal are: First, we will investigate whether HNF3Beta is required for pancreatic development through crosses of our HNF3Bet loxP/loxP mice with pancreas-specific Cre-recombinase transgenics. If our hypothesis is correct, deletion of HNF3Beta in the pancreas will lead to abnormal pancreatic development depending on the timing of deletion. Pancreatic development will be assessed by histological and immunohistochemical criteria. Second, through the use of a Beta-cell specific and steroid-inducible Cre-recombinase, we will address the question whether HNF3Beta also controls the maintenance of the specific cellular phenotype of the pancreatic Beta-cell If this is the case, induced deletion of HNF3Beta will be reflected in a perturbation of cell lineage allocation in the pancreatic islet and/or the regulation of glucose homeostasis. Together these studies will further our understanding of the transcriptional regulation of pancreatic development and the pathogenesis of diabetes. Insights gained about the role of HNF3Beta in Beta-cell function could be incorporated into future therapeutic strategies, including gene therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK055342-02
Application #
2906386
Study Section
Special Emphasis Panel (ZDK1-GRB-8 (O1))
Program Officer
Sato, Sheryl M
Project Start
1998-09-30
Project End
2003-09-29
Budget Start
1999-09-30
Budget End
2000-09-29
Support Year
2
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Genetics
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Santos, Gustavo Jorge Dos; Ferreira, Sandra Mara; Ortis, Fernanda et al. (2014) Metabolic memory of ß-cells controls insulin secretion and is mediated by CaMKII. Mol Metab 3:484-9
Zhang, Jia; McKenna, Lindsay B; Bogue, Clifford W et al. (2014) The diabetes gene Hhex maintains ?-cell differentiation and islet function. Genes Dev 28:829-34
Jiao, Yang; Rieck, Sebastian; Le Lay, John et al. (2013) CISH has no non-redundant functions in glucose homeostasis or beta cell proliferation during pregnancy in mice. Diabetologia 56:2435-45
Schaffer, Ashleigh E; Taylor, Brandon L; Benthuysen, Jacqueline R et al. (2013) Nkx6.1 controls a gene regulatory network required for establishing and maintaining pancreatic Beta cell identity. PLoS Genet 9:e1003274
Li, Zhaoyu; Tuteja, Geetu; Schug, Jonathan et al. (2012) Foxa1 and Foxa2 are essential for sexual dimorphism in liver cancer. Cell 148:72-83
Bramswig, Nuria C; Kaestner, Klaus H (2012) Organogenesis and functional genomics of the endocrine pancreas. Cell Mol Life Sci 69:2109-23
Rieck, Sebastian; Zhang, Jia; Li, Zhaoyu et al. (2012) Overexpression of hepatocyte nuclear factor-4? initiates cell cycle entry, but is not sufficient to promote ?-cell expansion in human islets. Mol Endocrinol 26:1590-602
Cui, Chang-Yi; Childress, Victoria; Piao, Yulan et al. (2012) Forkhead transcription factor FoxA1 regulates sweat secretion through Bestrophin 2 anion channel and Na-K-Cl cotransporter 1. Proc Natl Acad Sci U S A 109:1199-203
Gao, Nan; Le Lay, John; Qin, Wei et al. (2010) Foxa1 and Foxa2 maintain the metabolic and secretory features of the mature beta-cell. Mol Endocrinol 24:1594-604
May, Catherine Lee; Kaestner, Klaus H (2010) Gut endocrine cell development. Mol Cell Endocrinol 323:70-5

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