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(Received for publication, March 14, 1997, and in revised form, April 8, 1997)
From the Department of Biological Science, Florida State
University, Tallahassee, Florida 32306-3050
H1 histones, found in all multicellular
eukaryotes, associate with linker DNA between adjacent nucleosomes,
presumably to keep the chromatin in a compact, helical state. The
identification of multiple histone H1 subtypes in vertebrates suggests
these proteins have specialized roles in chromatin organization and thus influence the regulation of gene expression in the multicellular organism. The mechanism by which the association of H1 with nucleosomal DNA is regulated is not completely understood, but affinity for different DNA sequences may play a role. Here we report that a specific
H1 subtype in the mouse, namely H1b, selectively binds to a regulatory
element within the protein-encoding sequence of a
replication-dependent mouse H3.2 gene. We have previously
shown that this coding region element,
, is the target of very
specific interactions in vitro with another nuclear factor
called the
factor. This element is required for normal gene
expression in stably transfected rodent cells. The mouse H1b protein
interacts poorly (100-fold lower affinity) with the comparable
"
" sequence of a replication-independent mouse H3.3 gene. This
H3.3 sequence differs at only 4 out of 22 nucleotide positions from the
H3.2 sequence. Our findings raise the possibility that this H1b protein plays a specific role in regulation of expression of the
replication-dependent histone gene family.
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