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Research ArticleArticle

Glucocorticoid Receptor Enhancement of Pregnane X Receptor-Mediated CYP2B6 Regulation in Primary Human Hepatocytes

Hongbing Wang, Stephanie R. Faucette, Darryl Gilbert, Summer L. Jolley, Tatsuya Sueyoshi, Masahiko Negishi and Edward L. LeCluyse
Drug Metabolism and Disposition May 2003, 31 (5) 620-630; DOI: https://doi.org/10.1124/dmd.31.5.620
Hongbing Wang
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Stephanie R. Faucette
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Darryl Gilbert
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Summer L. Jolley
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Tatsuya Sueyoshi
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Masahiko Negishi
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Edward L. LeCluyse
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Abstract

Although the glucocorticoid receptor (GR) facilitates the xenobiotic-induced expression of CYP2B in rodents, its role in the regulation of human CYP2B6 is unclear. In this report, the role of human GR in the regulation of CYP2B6 was evaluated using primary human hepatocytes and transfection assays with Huh7 cells. CYP2B6 expression was not induced in primary hepatocytes treated with dexamethasone (DEX) concentrations (0.01–1 μM) known to activate GR. In contrast, treatment with 0.1 μM DEX enhanced CYP2B6 induction by different pregnane X receptor (PXR) activators, including rifampin, phenytoin, clotrimazole, and phenobarbital. In Huh7 cells, cotransfection of human (h)GR and hPXR with CYP2B6-phenobarbital-responsive enhancer module (PBREM) reporter constructs revealed that all hPXR ligands induce CYP2B6 reporter gene activity, and this ligand-dependent activation is greatly enhanced by activated hGR. CYP2B6 reporter gene expression was not induced in the presence of hPXR ligands when hGR alone was cotransfected with CYP2B6 reporter construct. In hGR and human constitutive androstane receptor (hCAR) cotransfection assays, activated hGR increased the constitutive activation of PBREM reporter constructs by hCAR in the absence of inducers. In the presence of activated hGR and known inducers of CYP2B6, only PB treatment caused a further 2-fold activation of hCAR compared with control. These studies show that hGR is involved synergistically in the xenobiotic-responsive regulation of human CYP2B6 by hPXR and hCAR. Moreover, the results suggest that the GR-enhanced expression of CYP2B6 is mediated through an indirect mechanism that does not require increased expression of nuclear receptor.

Footnotes

  • Abbreviations used are::
    P450
    cytochrome P450
    PXR
    pregnane X receptor
    CAR
    constitutive androstane receptor
    PB
    phenobarbital
    GR
    glucocorticoid receptor
    MCM
    modified Chee's medium
    DEX
    dexamethasone
    RIF
    rifamipicin
    PHY
    phenytoin
    CLZ
    clotrimazole
    BUP
    bupropion
    PBREM
    phenobarbital-responsive enhancer module
    DMSO
    dimethyl sulfoxide
    HLN
    human liver number
    PCR
    polymerase chain reaction
    bp
    base pair(s)
    GRE
    glucocorticoids responsive element
    • Received October 23, 2002.
    • Accepted February 10, 2003.
  • U.S. Government
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Drug Metabolism and Disposition: 31 (5)
Drug Metabolism and Disposition
Vol. 31, Issue 5
1 May 2003
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Research ArticleArticle

Glucocorticoid Receptor Enhancement of Pregnane X Receptor-Mediated CYP2B6 Regulation in Primary Human Hepatocytes

Hongbing Wang, Stephanie R. Faucette, Darryl Gilbert, Summer L. Jolley, Tatsuya Sueyoshi, Masahiko Negishi and Edward L. LeCluyse
Drug Metabolism and Disposition May 1, 2003, 31 (5) 620-630; DOI: https://doi.org/10.1124/dmd.31.5.620

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Research ArticleArticle

Glucocorticoid Receptor Enhancement of Pregnane X Receptor-Mediated CYP2B6 Regulation in Primary Human Hepatocytes

Hongbing Wang, Stephanie R. Faucette, Darryl Gilbert, Summer L. Jolley, Tatsuya Sueyoshi, Masahiko Negishi and Edward L. LeCluyse
Drug Metabolism and Disposition May 1, 2003, 31 (5) 620-630; DOI: https://doi.org/10.1124/dmd.31.5.620
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