Glucose regulation of insulin gene expression in pancreatic beta-cells.
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| Abstract |    :  
                  Production and secretion of insulin from the beta-cells of the pancreas is very crucial in maintaining normoglycaemia. This is achieved by tight regulation of insulin synthesis and exocytosis from the beta-cells in response to changes in blood glucose levels. The synthesis of insulin is regulated by blood glucose levels at the transcriptional and post-transcriptional levels. Although many transcription factors have been implicated in the regulation of insulin gene transcription, three beta-cell-specific transcriptional regulators, Pdx-1 (pancreatic and duodenal homeobox-1), NeuroD1 (neurogenic differentiation 1) and MafA (V-maf musculoaponeurotic fibrosarcoma oncogene homologue A), have been demonstrated to play a crucial role in glucose induction of insulin gene transcription and pancreatic beta-cell function. These three transcription factors activate insulin gene expression in a co-ordinated and synergistic manner in response to increasing glucose levels. It has been shown that changes in glucose concentrations modulate the function of these beta-cell transcription factors at multiple levels. These include changes in expression levels, subcellular localization, DNA-binding activity, transactivation capability and interaction with other proteins. Furthermore, all three transcription factors are able to induce insulin gene expression when expressed in non-beta-cells, including liver and intestinal cells. The present review summarizes the recent findings on how glucose modulates the function of the beta-cell transcription factors Pdx-1, NeuroD1 and MafA, and thereby tightly regulates insulin synthesis in accordance with blood glucose levels.  | 
        
| Year of Publication |    :  
                  2008 
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| Journal |    :  
                  The Biochemical journal 
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| Volume |    :  
                  415 
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| Issue |    :  
                  1 
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| Number of Pages |    :  
                  1-10 
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| Date Published |    :  
                  2008 
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| ISSN Number |    :  
                  0264-6021 
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| URL |    :  
                  https://portlandpress.com/biochemj/article-lookup/doi/10.1042/BJ20081029 
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| DOI |    :  
                  10.1042/BJ20081029 
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| Short Title |    :  
                  Biochem J 
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