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A more recent version of this article appeared on July 26, 2002
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M203645200v1
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Papers In Press, published online ahead of print May 14, 2002
J. Biol. Chem, 10.1074/jbc.M203645200
Submitted on April 15, 2002
Revised on May 9, 2002
Accepted on May 14, 2002

Physical interaction between GATA-5 and HNF-1alpha results in synergistic activation of the human lactase-phlorizin hydrolase promoter

Herbert M. van Wering, Inge L. Huibregtse, Sanne M. van der Zwan, Maartje S. de Bie, Lauren N. Dowling, Richard J. Grand, and Stephen D. Krasinski

Department of Medicine/GI, Children's Hospital, Harvard Medical School, Boston, MA 02115

Corresponding Author: Stephen.krasinski{at}tch.harvard.edu

GATA-4, -5, and -6 zinc finger and HNF-1alpha homeodomain transcription factors are expressed in the intestinal epithelium and synergistically activate the promoter of intestinal genes. Here, we demonstrate that GATA-5 and HNF-1alpha physically associate both in vivo and in vitro, and that this interaction is necessary for cooperative activation of the lactase-phlorizin hydrolase (LPH) promoter. Further, physical association is mediated by the C-terminal zinc finger of GATA factors and the homeodomain of HNF-1alpha . Deletion of HNF-1alpha activation domains or interruption of HNF-1 binding sites in the LPH promoter results in a complete loss of cooperativity, whereas deletion of GATA-5 activation domains or interruption of GATA binding sites results in a reduction, but not an elimination of cooperativity. We hypothesize that GATA/HNF-1alpha -cooperativity is mediated by HNF-1alpha through its activation domains which are oriented for high levels of activation through binding to DNA and physical association with GATA factors. These data suggest a paradigm whereby intestine-specific gene expression is regulated by unique interactions among tissue-restricted transcription factors co-expressed in the intestine. Parallel mechanisms in other tissue as well as in Drosophila suggest that zinc finger/homeodomain interactions are an efficient pathway of cooperative activation of gene transcription that has been conserved throughout evolution.


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