The Major Human Pregnane X Receptor (PXR) Splice Variant, PXR.2, Exhibits Significantly Diminished Ligand-Activated Transcriptional RegulationS
The pregnane X receptor (PXR; PXR.1) can be activated by structurally diverse lipophilic ligands. PXR.2, an alternatively spliced form of PXR, lacks 111 nucleotides encoding 37 amino acids in the ligand binding domain. PXR.2 bound a classic CYP3A4 PXR response element (PXRE) in electrophoretic mobil...
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Veröffentlicht in: | Drug metabolism and disposition 2009-02, Vol.37 (6), p.1295-1304 |
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Sprache: | eng |
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Zusammenfassung: | The pregnane X receptor (PXR; PXR.1) can be activated by structurally
diverse lipophilic ligands. PXR.2, an alternatively spliced form of PXR, lacks
111 nucleotides encoding 37 amino acids in the ligand binding domain. PXR.2
bound a classic CYP3A4 PXR response element (PXRE) in electrophoretic mobility
shift assays, but transfected PXR.2 failed to transactivate a
CYP3A4-promoter-luciferase reporter plasmid in HepG2 cells treated with
various PXR ligands. Cotransfection experiments showed that PXR.2 behaved as a
dominant negative, interfering with PXR.1/rifampin activation of
CYP3A4-PXRE-LUC. In HepG2 and LS180 cells stably transduced with PXR.1, PXR
target genes (
CYP3A4
,
MDR1
,
CYP2B6
, and
UGT1A1
) were higher than mock-transduced cells in the absence of
ligand and were further induced in the presence of rifampin. In contrast,
PXR.2 stably introduced into the same host cells failed to induce target genes
over levels in mock-transfected cells after drug treatment. Our homology
modeling suggests that ligands bind PXR.1 more favorably, probably because of
the presence of a key disordered loop region, which is missing in PXR.2. Yeast
two-hybrid assays revealed that, even in the presence of ligand, the
corepressors remain tightly bound to PXR.2, and coactivators are unable to
bind at helix 12. In summary, PXR.2 can bind to PXREs but fails to
transactivate target genes because ligands do not bind the ligand binding
domain of PXR.2 productively, corepressors remain tightly bound, and
coactivators are not recruited to PXR.2. |
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ISSN: | 0090-9556 1521-009X |
DOI: | 10.1124/dmd.108.025213 |