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J Biol Chem, Vol. 274, Issue 9, 5851-5860, February 26, 1999
Characterization of a Novel Calcium Response Element in the
Glucagon Gene
Ursel
Fürstenau,
Markus
Schwaninger,
Roland
Blume,
Eva-Maria
Jendrusch, and
Willhart
Knepel
From the Department of Molecular Pharmacology, University of
Göttingen, D-37070 Göttingen, Germany
To maintain blood glucose levels within narrow
limits, the synthesis and secretion of pancreatic islet hormones is
controlled by a variety of extracellular signals.
Depolarization-induced calcium influx into islet cells has been shown
to stimulate glucagon gene transcription through the transcription
factor cAMP response element-binding protein that binds to the glucagon
cAMP response element. By transient transfection of glucagon-reporter
fusion genes into islet cell lines, this study identified a second
calcium response element in the glucagon gene (G2 element, from 165
to 200). Membrane depolarization was found to induce the binding of a
nuclear complex with NFATp-like immunoreactivity to the G2 element.
Consistent with nuclear translocation, a comigrating complex was found
in cytosolic extracts of unstimulated cells, and the induction of
nuclear protein binding was blocked by inhibition of calcineurin
phosphatase activity by FK506. A mutational analysis of G2 function and
nuclear protein binding as well as the effect of FK506 indicate that
calcium responsiveness is conferred to the G2 element by NFATp
functionally interacting with HNF-3 binding to a closely associated
site. Transcription factors of the NFAT family are known to cooperate
with AP-1 proteins in T cells for calcium-dependent
activation of cytokine genes. This study shows a novel pairing of NFATp
with the cell lineage-specific transcription factor HNF-3 in islet
cells to form a novel calcium response element in the glucagon gene.
Copyright © 1999 by The American Society for Biochemistry and Molecular Biology, Inc.

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Copyright © 1999 by the American Society for Biochemistry and Molecular Biology.
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