Abstract

The 5'-flanking region sequences located between-340 to -91 base pairs (bp) mediate pancreatic beta cell-specific and glucose-regulated transcription of the insulin gene. The C2 (-317/-311 bp)), A3 (-301 to - 196 bp), C1 (-118 and -107 bp), and E1 (-100 to -91 bp) elements are essential in control. The activators of insulin C2-, A3-, and E1- complement stimulated transcriptions are PAX6, PDX-1 and BETA2, respectively. Strikingly, gene ablation experiments performed have also clearly established an essential function in mice for each of these islet- enriched transcription factor during pancreatic development. In addition, heterozygous mutations in the Pdx-1 and BETA2 genes contribute to beta cell dysfunction in type 2 diabetes. These findings illustrate how the identification and characterization of the critical transcription regulators of islet-enriched products, like insulin, are essential for our understanding of the disease process affecting the beta cell. However, little is known about the protein(s) involved in C1 element stimulation. The RIPE3b1 factor DNA complex formed with these element in gel mobility shift assays is uniquely detected in beta cells extracts, and is selectively regulated in parallel with changes in insulin gene transcription in glucose- treated beta cells. These results strongly imply that the RIPE3b1 complex contains a DNA-binding protein(s) important in the physiological regulation of insulin transcription. The sequences comprising the C1 element are unrelated to those bound by any known transcription factor, strongly suggesting that RIPE3b1 will be a novel DNA-binding transcription. Our first objective will be to isolate and characterize the activation properties of the RIPE3b1 protein(s). Our second objective will be to examine how pancreatic development and islet beta cell function is affected in mice lacking RIPE3b1. These experiments will determine the role of the RIPE3b1 protein(s) in both cell-specific and glucose- modulated regulation of insulin gene transcription and during pancreaogenesis.

  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 #
3U19DK042502-12S2
Application #
6600016
Study Section
Special Emphasis Panel (ZDK1)
Project Start
2001-07-01
Project End
2002-09-29
Budget Start
Budget End
Support Year
12
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Type
DUNS #
004413456
City
Nashville
State
TN
Country
United States
Zip Code
37203

  Publications

Zhang, Juliet; Weinrich, Jarret A P; Russ, Jeffrey B et al. (2017) A Role for Dystonia-Associated Genes in Spinal GABAergic Interneuron Circuitry. Cell Rep 21:666-678
Kodama, Sota; Nakano, Yasuhiro; Hirata, Koji et al. (2016) Diabetes Caused by Elastase-Cre-Mediated Pdx1 Inactivation in Mice. Sci Rep 6:21211
Comer, John D; Pan, Fong Cheng; Willet, Spencer G et al. (2015) Sensory and spinal inhibitory dorsal midline crossing is independent of Robo3. Front Neural Circuits 9:36
Pan, Fong Cheng; Brissova, Marcela; Powers, Alvin C et al. (2015) Inactivating the permanent neonatal diabetes gene Mnx1 switches insulin-producing ?-cells to a ?-like fate and reveals a facultative proliferative capacity in aged ?-cells. Development 142:3637-48
Delgiorno, Kathleen E; Hall, Jason C; Takeuchi, Kenneth K et al. (2014) Identification and manipulation of biliary metaplasia in pancreatic tumors. Gastroenterology 146:233-44.e5
Baeyens, Luc; Lemper, Marie; Leuckx, Gunter et al. (2014) Transient cytokine treatment induces acinar cell reprogramming and regenerates functional beta cell mass in diabetic mice. Nat Biotechnol 32:76-83
von Figura, Guido; Morris 4th, John P; Wright, Christopher V E et al. (2014) Nr5a2 maintains acinar cell differentiation and constrains oncogenic Kras-mediated pancreatic neoplastic initiation. Gut 63:656-64
Pan, Fong Cheng; Bankaitis, Eric D; Boyer, Daniel et al. (2013) Spatiotemporal patterns of multipotentiality in Ptf1a-expressing cells during pancreas organogenesis and injury-induced facultative restoration. Development 140:751-64
Liu, Jing; Willet, Spencer G; Bankaitis, Eric D et al. (2013) Non-parallel recombination limits Cre-LoxP-based reporters as precise indicators of conditional genetic manipulation. Genesis 51:436-42
Potter, Leah A; Choi, Eunyoung; Hipkens, Susan B et al. (2012) A recombinase-mediated cassette exchange-derived cyan fluorescent protein reporter allele for Pdx1. Genesis 50:384-92

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