Literature DB >> 15024072

Overexpression of inducible cyclic AMP early repressor inhibits transactivation of genes and cell proliferation in pancreatic beta cells.

Akari Inada1, Yoshiyuki Hamamoto, Yoshiyuki Tsuura, Jun-ichi Miyazaki, Shinya Toyokuni, Yu Ihara, Koichiro Nagai, Yuichiro Yamada, Susan Bonner-Weir, Yutaka Seino.   

Abstract

Transcriptional control mediated by the cyclic AMP-responsive element (CRE) represents an important mechanism of gene regulation. To test our hypothesis that increased inducible cyclic AMP early repressor (ICER) Igamma inhibits function of CRE-binding proteins and thus disrupts CRE-mediated transcription in pancreatic beta cells, we generated transgenic mice with beta-cell-directed expression of ICER Igamma, a powerful repressor that is greatly increased in diabetes. Three transgenic lines clearly show that increased ICER Igamma expression in beta cells results in early severe diabetes. From birth islets were severely disorganized with a significantly increased proportion of alpha cells throughout the islet. Diabetes results from the combined effects of impaired insulin expression and a decreased number of beta cells. The decrease in beta cells appears to result from impaired proliferation rather than from increased apoptosis after birth. Cyclin A gene expression is impaired by the strong inhibition of ICER; the suppression of cyclin A results in a substantially decreased proliferation of beta cells in the postnatal period. These results suggest that CRE and CRE-binding factors have an important role in pancreatic beta-cell physiology not only directly by regulation of gene trans-activation but also indirectly by regulation of beta-cell mass.

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Year:  2004        PMID: 15024072      PMCID: PMC371116          DOI: 10.1128/MCB.24.7.2831-2841.2004

Source DB:  PubMed          Journal:  Mol Cell Biol        ISSN: 0270-7306            Impact factor:   4.272


  55 in total

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2.  Analysis of the role of the transcription factor ATF in the assembly of a functional preinitiation complex.

Authors:  T W Hai; M Horikoshi; R G Roeder; M R Green
Journal:  Cell       Date:  1988-09-23       Impact factor: 41.582

3.  Control of insulin gene expression in pancreatic beta-cells and in an insulin-producing cell line, RIN-5F cells. II. Regulation of insulin mRNA stability.

Authors:  M Welsh; D A Nielsen; A J MacKrell; D F Steiner
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4.  Cell-specific expression of the rat insulin gene: evidence for role of two distinct 5' flanking elements.

Authors:  T Edlund; M D Walker; P J Barr; W J Rutter
Journal:  Science       Date:  1985-11-22       Impact factor: 47.728

Review 5.  Nutrient regulation of insulin gene expression.

Authors:  K Docherty; A R Clark
Journal:  FASEB J       Date:  1994-01       Impact factor: 5.191

6.  Somatostatin gene expression in pancreatic islet cells is directed by cell-specific DNA control elements and DNA-binding proteins.

Authors:  A C Powers; F Tedeschi; K E Wright; J S Chan; J F Habener
Journal:  J Biol Chem       Date:  1989-06-15       Impact factor: 5.157

7.  The cdc2 kinase is a nuclear protein that is essential for mitosis in mammalian cells.

Authors:  K Riabowol; G Draetta; L Brizuela; D Vandre; D Beach
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8.  Control of insulin gene expression in pancreatic beta-cells and in an insulin-producing cell line, RIN-5F cells. I. Effects of glucose and cyclic AMP on the transcription of insulin mRNA.

Authors:  D A Nielsen; M Welsh; M J Casadaban; D F Steiner
Journal:  J Biol Chem       Date:  1985-11-05       Impact factor: 5.157

9.  A cluster of phosphorylation sites on the cyclic AMP-regulated nuclear factor CREB predicted by its sequence.

Authors:  G A Gonzalez; K K Yamamoto; W H Fischer; D Karr; P Menzel; W Biggs; W W Vale; M R Montminy
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10.  Leucine zipper structure of the protein CRE-BP1 binding to the cyclic AMP response element in brain.

Authors:  T Maekawa; H Sakura; C Kanei-Ishii; T Sudo; T Yoshimura; J Fujisawa; M Yoshida; S Ishii
Journal:  EMBO J       Date:  1989-07       Impact factor: 11.598

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  29 in total

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Review 2.  Protein phosphatases in pancreatic islets.

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3.  ICER induced by hyperglycemia represses the expression of genes essential for insulin exocytosis.

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4.  Adenylyl cyclase 8 is central to glucagon-like peptide 1 signalling and effects of chronically elevated glucose in rat and human pancreatic beta cells.

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5.  Establishment of a diabetic mouse model with progressive diabetic nephropathy.

Authors:  Akari Inada; Kojiro Nagai; Hidenori Arai; Jun-ichi Miyazaki; Keiko Nomura; Hiroshi Kanamori; Shinya Toyokuni; Yuichiro Yamada; Susan Bonner-Weir; Gordon C Weir; Atsushi Fukatsu; Yutaka Seino
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Review 6.  CREB and the CRTC co-activators: sensors for hormonal and metabolic signals.

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7.  Genome-wide analysis of cAMP-response element binding protein occupancy, phosphorylation, and target gene activation in human tissues.

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8.  Glucose- and metabolically regulated hepatic insulin gene therapy for diabetes.

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9.  Glucose controls CREB activity in islet cells via regulated phosphorylation of TORC2.

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10.  Repurposing cAMP-modulating medications to promote β-cell replication.

Authors:  Zhenshan Zhao; Yen S Low; Neali A Armstrong; Jennifer Hyoje Ryu; Sara A Sun; Anthony C Arvanites; Jennifer Hollister-Lock; Nigam H Shah; Gordon C Weir; Justin P Annes
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