Literature DB >> 12000309

Foxa3 (HNF-3gamma) binds to and activates the rat proglucagon gene promoter but is not essential for proglucagon gene expression.

Yuanfang Liu1, Wei Shen, Patricia L Brubaker, Klaus H Kaestner, Daniel J Drucker.   

Abstract

Members of the Forkhead box a (Foxa) transcription factor family are expressed in the liver, pancreatic islets and intestine and both Foxa1 and Foxa2 regulate proglucagon gene transcription. As Foxa proteins exhibit overlapping DNA-binding specificities, we examined the role of Foxa3 [hepatocyte nuclear factor (HNF)-3gamma] in control of proglucagon gene expression. Foxa3 was detected by reverse transcriptase PCR in glucagon-producing cell lines and binds to the rat proglucagon gene G2 promoter element in GLUTag enteroendocrine cells. Although Foxa3 increased rat proglucagon promoter activity in BHK fibroblasts, augmentation of Foxa3 expression did not increase proglucagon promoter activity in GLUTag cells. Furthermore, adenoviral Foxa3 expression did not affect endogenous proglucagon gene expression in islet or intestinal endocrine cell lines. Although Foxa3(-/-) mice exhibit mild hypoglycaemia during a prolonged fast, the levels of proglucagon-derived peptides and proglucagon mRNA transcripts were comparable in tissues from wild-type and Foxa3(-/-) mice. These findings identify Foxa3 as a member of the proglucagon gene G2 element binding-protein family that, unlike Foxa1, is not essential for control of islet or intestinal proglucagon gene expression in vivo.

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Year:  2002        PMID: 12000309      PMCID: PMC1222783          DOI: 10.1042/BJ20020095

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  64 in total

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Journal:  Diabetes Care       Date:  1993-10       Impact factor: 19.112

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Journal:  Development       Date:  1993-05       Impact factor: 6.868

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  6 in total

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3.  Expression of Id1 in adult, regenerating and developing pancreas.

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4.  Characterization of a novel Foxa (hepatocyte nuclear factor-3) site in the glucagon promoter that is conserved between rodents and humans.

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5.  Contrasting patterns of expression of transcription factors in pancreatic alpha and beta cells.

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6.  Stage-specific transcriptomic changes in pancreatic α-cells after massive β-cell loss.

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  6 in total

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