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(Received for publication, July 5, 1995) The specificity of expression in the liver of the human
apolipoprotein (apo) E/C-I gene locus is determined by a hepatic
control region (HCR) that is located 15 kilobases downstream of the
apoE gene. DNase I footprint studies of this sequence using nuclear
extracts identified a region of the HCR that is enriched in nuclear
protein-binding sites. Nuclease analysis of chromatin revealed
liver-specific DNase I-hypersensitive sites that were associated with
this region, and additional liver-specific nuclease-sensitive sites
associated with the apoE gene were identified. The HCR domain has a
limited binding affinity for the nuclear scaffold. The specific domain
required for liver expression was tested by ligating subfragments of
the HCR to the apoE gene and examining their activity in transgenic
mice. A segment of 319 nucleotides that contained several potential
regulatory sequences was required for full activity of liver-specific
transcription with shorter segments yielding much lower levels of
expression in the liver. All constructs that contained a fully active
HCR were expressed in approximately a copy-dependent manner, suggesting
that transgene expression was independent of integration position.
Taken together, the properties of the HCR are consistent with its
function as a locus control region for the liver-specific expression of
the apoE gene.
Volume 270,
Number 38,
Issue of September 22, pp. 22577-22585, 1995
©1995 by The American Society for Biochemistry and Molecular Biology, Inc.
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