Traditional Chinese Medicines Wu Wei Zi (Schisandra chinensis Baill) and Gan Cao (Glycyrrhiza uralensis Fisch) Activate Pregnane X Receptor and Increase Warfarin Clearance in Rats

doi:10.1124/jpet.105.094342

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First published on November 2, 2005; DOI: 10.1124/jpet.105.094342

0022-3565/06/3163-1369-1377$20.00
JPET 316:1369-1377, 2006

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CELLULAR AND MOLECULAR

Traditional Chinese Medicines Wu Wei Zi (Schisandra chinensis Baill) and Gan Cao (Glycyrrhiza uralensis Fisch) Activate Pregnane X Receptor and Increase Warfarin Clearance in Rats

Ying Mu, Jinnan Zhang, Shimin Zhang, Hong-Hao Zhou, David Toma, Songrong Ren, Leaf Huang, Maria Yaramus, Andrew Baum, Raman Venkataramanan, and Wen Xie

Center for Pharmacogenetics (Y.M., D.T., S.R., L.H., W.X.) and Departments of Pharmaceutical Sciences (Y.M., S.Z., D.T., S.R., L.H., R.V., W.X.) and Pharmacy and Therapeutics (M.Y.), University of Pittsburgh School of Pharmacy, Pittsburgh, Pennsylvania; Department of Chem-Pharmacology, Capital University of Medical Sciences in Beijing China, Beijing, China (J.Z.); Institute of Clinical Pharmacology, Central South University, Changsha, Hunan, China (H.-H.Z.); and Integrative Medicine, University of Pittsburgh Cancer Institute, Pittsburgh, Pennsylvania (A.B.)

The traditional Chinese medicines (TCMs) are essential componentsof alternative medicines. Many TCMs are known to alter the expressionof hepatic drug-metabolizing enzymes and transporters. The molecularmechanism by which TCMs and/or their constituents regulate enzymeand transporter expression, however, has remained largely unknown.In this report, we show that two TCMs, Wu Wei Zi (Schisandrachinensis Baill) and Gan Cao (Glycyrrhiza uralensis Fisch),and their selected constituents activate the xenobiotic orphannuclear receptor pregnane X receptor (PXR). Treatment with TCMextracts and the Schisandrol and Schisandrin constituents ofWu Wei Zi induced the expression of drug-metabolizing enzymesand transporters in reporter gene assays and in primary hepatocytecultures. The affected enzymes and transporters include CYP3Aand 2C isozymes and the multidrug resistance-associated protein2. In transient transfection and reporter gene assays, the Schisandrinconstituents of Wu Wei Zi had an estimated EC₅₀ of 2 and 1.25µM on hPXR and mPXR, respectively. Interestingly, mutationsthat were intended to alter the pore of the ligand-binding cavityof PXR had species-specific effects on the activities of theindividual Schisandrols and Schisandrins. In rats, the administrationof Wu Wei Zi and Gan Cao increased the metabolism of the coadministeredwarfarin, reinforcing concerns involving the safe use of herbalmedicines and other nutraceuticals to avoid PXR-mediated drug-druginteractions. Meanwhile, the activation of PXR and inductionof detoxifying enzymes provide a molecular mechanism for thehepatoprotective effects of certain TCMs.

Received August 17, 2005; accepted October 24, 2005.

Address correspondence to: Dr. Wen Xie, Center for Pharmacogenetics, 633 Salk Hall, University of Pittsburgh, Pittsburgh, PA 15261. E-mail: wex6{at}pitt.edu

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