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Mol. Cell. Biol., Nov 1997, 6653-6662, Vol 17, No. 11
KJ Simon, DA Grueneberg and M Gilman
The human homeodomain protein Phox1 can impart serum-responsive
transcriptional activity to the c-fos serum response element (SRE) by
interacting with serum response factor (SRF). This activity is shared with
other Paired class homeodomains but not with more distantly related
homeodomains. To understand the mechanism of action of Phox1 at the SRE and
the basis for the selective activity of Paired class homeodomains in this
context, we performed a detailed mutagenesis of the Phox1 homeodomain. We
found that amino acid residues that contact the major groove of the DNA are
required for SRE activation in vivo, suggesting an in vivo requirement for
major-groove DNA contact by the homeodomain. In contrast, substitution of a
lysine residue in the N- terminal arm of the Phox1 homeodomain appeared to
abolish DNA binding without affecting activity in vivo. Certain
substitutions on the exposed surfaces of helices 1 and 2, not required for
DNA binding, abolished activity in vivo, suggesting that these surfaces
contact an accessory protein(s) required for this activity. We also found
that transfer of a single amino acid residue from the surface of Phox1
helix 1 to the corresponding position in the distantly related Deformed
(Dfd) homeodomain imparts to Dfd the ability to activate the SRE in vivo.
We propose that Phox1 interacts with one or more factors at the SRE, in
addition to SRF, and that the specificity of this interaction is determined
by residues on the surfaces of helices 1 and 2.
Copyright © 1997, American Society for Microbiology
Protein and DNA contact surfaces that mediate the selective action of the Phox1 homeodomain at the c-fos serum response element
Graduate Program in Molecular and Cellular Biology, State University of New York at Stony Brook, 11794, USA.
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