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Vol. 63, Issue 4, 915-924, April 2003
Molecular Toxicology and Environmental Medicine Program, School of
Medicine and Dentistry, University of Rochester, Rochester, New York
To investigate possible species-specificity of aryl hydrocarbon
receptor (AhR)-mediated signal transduction pathways, activities of
2,3,7,8-tetrochlorodibenzo-p-dioxin (TCDD) and six
synthetic flavonoids were evaluated in mouse hepatoma and guinea pig
adenocarcinoma cells transfected with an AhR-responsive luciferase
reporter. Rank order potency in these two cell lines was similar for
the ability of these flavonoids to antagonize TCDD-induced reporter gene expression. However, in the presence of flavone alone, a species-specific difference in agonist activity was observed. In guinea
pig cells, several flavonoids demonstrated agonist activity up to 50%
of the maximum TCDD response. In mouse cells, however, no significant
agonist activity was observed at the same concentrations based on
luciferase enzyme activity, protein expression, and mRNA analysis.
Moreover, competitive ligand-binding assays, using
[3H]TCDD in cytosolic fractions, demonstrated that
3'-methoxy-4'-nitroflavone had a similar IC50 in both
recombinant cell lines, suggesting that the flavone has similar binding
affinity to receptors from both species. However, electrophoretic
mobility shift assay using the cytosolic fractions demonstrated that
this flavone elicited binding to the DRE by guinea pig but not mouse
AhR complex. The dependence of the AhR in this differential interaction
was further demonstrated using in vitro synthesized guinea pig and
mouse Ah receptors and mouse Arnt. Together, these data suggest that
the differential agonist/antagonist activity of these flavone
derivatives is caused by the efficacy of these flavonoids in eliciting
an AhR conformation that recognizes regulatory response elements in a
species-specific manner.
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