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J Biol Chem, Vol. 273, Issue 38, 24504-24512, September 18, 1998
RFX1, a Single DNA-binding Protein with a Split Dimerization
Domain, Generates Alternative Complexes
Yael
Katan-Khaykovich and
Yosef
Shaul
From the Department of Molecular Genetics, The Weizmann Institute
of Science, Rehovot 76100, Israel
The transcription of various viral and cellular
genes is regulated by palindromic and nonpalindromic DNA sites
resembling the EP element of the hepatitis B virus enhancer, which
generate similar DNA-protein complexes. The upper EP complex contains
homodimers of the transcription regulator RFX1. We show that RFX1
possesses a split, extended dimerization domain composed of several
evolutionarily conserved boxes, one of which was previously shown to
mediate dimerization. Such an unusually long and complex dimerization domain could potentially serve for generating multiple complexes. In
addition to the previously characterized complex, RFX1 generated a
novel DNA-protein complex of extremely low mobility, formed only with
palindromic DNA sites. Different deletions within the dimerization
domain altered the relative abundance of the two complexes, suggesting
an interplay between them. Formation of the low mobility complex
correlated with transcriptional repression, in that both activities
were mediated by several portions of the conserved region. Our results
propose a mechanism by which the extended dimerization domain mediates
the formation of alternative homodimeric complexes, which differ in the
nature of the intersubunit interaction. By participating in different
types of interactions, this domain may regulate the relative abundance
of the different complexes, thus affecting transcriptional
activity.
Copyright © 1998 by The American Society for Biochemistry and Molecular Biology, Inc.

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Copyright © 1998 by the American Society for Biochemistry and Molecular Biology.
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