Abstract

NeuroD, a basic helix-loop-helix (bHLH) transcription factor, is required for islet formation and beta cell survival. We propose to determine the cellular basis for failure to form islets in NeuroD-null mice. Although NeuroD affects beta cells more than other cell types, loss of beta cells alone in other gene targeted mutant mice (e.g., PAX-4) does not result in failure to form islets. Thus, our mice provide an excellent opportunity to determine which cell types control islet biogenesis and whether islet formation has a direct role in maturation of beta cells. Here, we hypothesis that NeuroD affects development of cells other than beta cells, which are required for islet formation. As a first step to determine the role of NeuroD in generation of different cell types in the pancreas, we will perform a cell lineages analysis of NeuroAD expressing cells. Once we identify the non-beta cells that are of NeuroD-lineage, future experiments will include reintroduction of NeuroD into these cell types to restore islet formation. We also propose that NeuroD AND Nkx2.2, another essential pancreatic regulatory factor, are required for beta cell maintenance and regeneration in the adult islet. Nkx2.2 is a homeobox transcription factor that is required for the development and differentiation of three of the four endocrine cell types in embryonic mice: a deletion of Nkx2.2 adversely affects the development of alpha, beta and PP cells. NeuroD and Nkx2.2 are both high expressed in adult pancreatic beta cells, raising the possibility that they might also play roles in mature beta cells. In fact, while many NeuroD-null cells in the brain die during development, some die after morphological differentiation occurs, suggesting that NeuroD is required for maintenance of these neurons. Furthermore, several Nkx2 family members have been shown to play a role in cell-type maintenance in the tissues where they are expressed post-natally (Schott et al 1998; Shiratori et al 2001). Based on these observations and the expression patterns of both genes in mature beta cells, we hypothesize that NeuroD and Nkx2.2 are required for the maintenance and possibly regeneration of beta cells. To test this hypothesis, we propose to generate mice from which the neuroD or the Nkx2.2 allele will be conditionally eliminated in adult beta cells.
Specific Aim 1. Identify the cell types generated from NeuroD expressing cells.
Specific Aim 2. Determine whether NeuroD/Beta2 and Nkx2.2 are required for mature beta cell function and maintenance.
Specific Aim 3. Determine whether NeuroD and Nkx2.2 are required for beta cell regeneration.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program--Cooperative Agreements (U19)
Project #
5U19DK061248-02
Application #
6650610
Study Section
Special Emphasis Panel (ZDK1)
Project Start
2002-09-30
Project End
2003-07-31
Budget Start
Budget End
Support Year
2
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
University of Colorado Denver
Department
Type
DUNS #
065391526
City
Aurora
State
CO
Country
United States
Zip Code
80045

  Publications

Qu, Xiaoling; Afelik, Solomon; Jensen, Jan Nygaard et al. (2013) Notch-mediated post-translational control of Ngn3 protein stability regulates pancreatic patterning and cell fate commitment. Dev Biol 376:1-12
Nyeng, Pia; Bjerke, Maureen Ann; Norgaard, Gitte Anker et al. (2011) Fibroblast growth factor 10 represses premature cell differentiation during establishment of the intestinal progenitor niche. Dev Biol 349:20-34
Hill, Jonathon T; Chao, Christina S; Anderson, Keith R et al. (2010) Nkx2.2 activates the ghrelin promoter in pancreatic islet cells. Mol Endocrinol 24:381-90
Gu, Chunyan; Stein, Gretchen H; Pan, Ning et al. (2010) Pancreatic beta cells require NeuroD to achieve and maintain functional maturity. Cell Metab 11:298-310
Kobberup, Sune; Schmerr, Martin; Dang, My-Linh et al. (2010) Conditional control of the differentiation competence of pancreatic endocrine and ductal cells by Fgf10. Mech Dev 127:220-34
Juhl, Kirstine; Sarkar, Suparna A; Wong, Randall et al. (2008) Mouse pancreatic endocrine cell transcriptome defined in the embryonic Ngn3-null mouse. Diabetes 57:2755-61
Tessem, Jeffery S; Jensen, Jan N; Pelli, Hanna et al. (2008) Critical roles for macrophages in islet angiogenesis and maintenance during pancreatic degeneration. Diabetes 57:1605-17
Sarkar, S A; Kobberup, S; Wong, R et al. (2008) Global gene expression profiling and histochemical analysis of the developing human fetal pancreas. Diabetologia 51:285-97
Quayum, Nayeem; Kutchma, Alecksandr; Sarkar, Suparna A et al. (2008) GeneSpeed Beta Cell: an online genomics data repository and analysis resource tailored for the islet cell biologist. Exp Diabetes Res 2008:312060
Doyle, Michelle J; Sussel, Lori (2007) Nkx2.2 regulates beta-cell function in the mature islet. Diabetes 56:1999-2007

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