The Chinese herbal medicine Sophora flavescens activates pregnane X receptor

L Wang, F Li, J Lu, G Li, D Li, X Zhong, GL Guo… - Drug Metabolism and …, 2010 - ASPET
L Wang, F Li, J Lu, G Li, D Li, X Zhong, GL Guo, X Ma
Drug Metabolism and Disposition, 2010ASPET
Sophora flavescens (SF) is an herbal medicine widely used for the treatment of viral
hepatitis, cancer, viral myocarditis, gastrointestinal hemorrhage, and skin diseases. It was
recently reported that SF up-regulates CYP3A expression. The mechanism of SF-induced
CYP3A expression is unknown. In the current study, we tested the hypothesis that SF-
induced CYP3A expression is mediated by the activation of pregnane X receptor (PXR). We
used two cell lines, DPX2 and HepaRG, to investigate the role of PXR in SF-induced CYP3A …
Sophora flavescens (SF) is an herbal medicine widely used for the treatment of viral hepatitis, cancer, viral myocarditis, gastrointestinal hemorrhage, and skin diseases. It was recently reported that SF up-regulates CYP3A expression. The mechanism of SF-induced CYP3A expression is unknown. In the current study, we tested the hypothesis that SF-induced CYP3A expression is mediated by the activation of pregnane X receptor (PXR). We used two cell lines, DPX2 and HepaRG, to investigate the role of PXR in SF-induced CYP3A expression. The DPX2 cell line is derived from HepG2 cells with the stable transfection of human PXR and a luciferase reporter gene linked with a human PXR response element identified in the CYP3A4 gene promoter. In DPX2 cells, SF activated PXR in a concentration-dependent manner. We used a metabolomic approach to identify the chemical constituents in SF, which were further analyzed for their effect on PXR activation and CYP3A regulation. One chemical in SF, N-methylcytisine, was identified as an individual chemical that activated PXR. HepaRG is a highly differentiated hepatoma cell line that mimics human hepatocytes. In HepaRG cells, N-methylcytisine significantly induced CYP3A4 expression, and this induction was suppressed by the PXR antagonist sulforaphane. These results suggest that SF induces CYP3A expression via the activation of PXR.
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