Transcriptional Regulation of the Phosphoenolpyruvate Carboxykinase Gene by Cooperation Between Hepatic Nuclear Factors

Mice deficient in hepatocyte nuclear factor 1 alpha (HNF-1␣) were produced by use of the Cre-loxP recombination system. HNF-1␣-null mice are viable but sterile and exhibit a phenotype reminiscent of both Laron-type dwarfism and non-insulin-dependent diabetes mellitus (NIDDM). In contrast to an earlier HNF-1␣-null mouse line that had been produced by use of standard gene disruption methodology (M. Pontoglio, J. Barra, M. Hadchouel, A. Doyen, C. Kress, J. P. Bach, C. Babinet, and M. Yaniv, Cell 84:575-585, 1996), these mice exhibited no increased mortality and only minimal renal dysfunction during the first 6 months of development. Both dwarfism and NIDDM are most likely due to the loss of expression of insulin-like growth factor I (IGF-I) and lower levels of insulin, resulting in stunted growth and elevated serum glucose levels, respectively. These results confirm the functional significance of the HNF-1␣ regulatory elements that had previously been shown to reside in the promoter regions of both the IGF-I and the insulin genes.

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Laron Dwarfism and Non-Insulin-Dependent Diabetes Mellitus in the Hnf-1α Knockout Mouse

Lee

Sauer

Gonzalez

1998

Molecular and Cellular Biology

247

239

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Hepatocyte Nuclear Factor-1α Recruits the Transcriptional Co-Activator p300 on the GLUT2 Gene Promoter

et al. 2002

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Mutations in the hepatocyte nuclear factor (HNF)-1␣ gene have been linked to subtype 3 of maturity-onset diabetes of the young (MODY), a disease characterized by a primary defect in insulin secretion. Here we show that the human GLUT2 gene is closely regulated by HNF-1␣ via sequences downstream of the transcriptional start site by interaction with transcriptional co-activator p300. The promoter region of the human GLUT2 gene was subcloned into luciferase expression plasmids that were transfected together with HNF-1␣ expression plasmid into a pancreatic ␤-cell line, HIT-T15, to evaluate transcriptional activities. HNF-1␣ enhanced human GLUT2 promoter activity sixfold. Sitedirect mutagenesis and footprint analyses showed that the HNF-1␣ binding site (؉200 to ؉218) is critical in human GLUT2 gene expression. Furthermore, mammalian two-hybrid and immunoprecipitation studies revealed the transactivation domain of HNF-1␣ (amino acids 391-540) to interact with both the NH 2 -terminal region (amino acids 180 -662) and the COOH-terminal region (amino acids 1,818 -2,079) of p300. These findings demonstrated that HNF-1␣ binds to the 5-untranslated region of GLUT2 and that p300 acts as a transcriptional co-activator for HNF-1␣. In addition, these results provided new insight into the regulatory function of HNF-1␣ by suggesting a molecular basis for human GLUT2 gene expression.

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Transcriptional Regulation of the Phosphoenolpyruvate Carboxykinase Gene by Cooperation Between Hepatic Nuclear Factors

Cited by 2 publications

References 76 publications

Laron Dwarfism and Non-Insulin-Dependent Diabetes Mellitus in the Hnf-1α Knockout Mouse

Laron Dwarfism and Non-Insulin-Dependent Diabetes Mellitus in the Hnf-1α Knockout Mouse

Hepatocyte Nuclear Factor-1α Recruits the Transcriptional Co-Activator p300 on the GLUT2 Gene Promoter

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