Structural Disorder in the Complex of Human Pregnane X Receptor and the Macrolide Antibiotic Rifampicin

Chrencik, Jill E.; Orans, Jillian; Moore, Linda B.; Xue, Yu; Li, Peng; Collins, Jon L.; Wisely, G. Bruce; Lambert, Millard H.; Kliewer, Steven A.; Redinbo, Matthew R.

doi:10.1210/me.2004-0346

Cited by 183 publications

(217 citation statements)

References 28 publications

(61 reference statements)

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“…This product was cloned into the pTriEx1.1 expression plasmid (Clontech, UK) and sequenced to ensure 100% identity to the published sequence, In silico analysis: Ligand docking was undertaken using Autodock 4 suite and Autodock Tools for Windows (Morris et al 2009). Molecular coordinates for the crystal structure of PXR with rifampicin bound (Chrencik et al 2005) were obtained from the RCSB protein databank (Accession: 1SKX; http://www.rcsb.org/pdb/home/home.do), whereas three dimensional structures of statins were designed using Corina (http://www.molecular-networks.com/products/corina). Docking was undertaken using a 0.375Å grid centred upon the ligand-binding pocket of PXR, using a genetic algortim with the following parameters: 150 iterations; 100 population size; 1E+6 energy evaluations; 1E+5 maximum generations.…”

Section: Methodsmentioning

confidence: 99%

The statin class of HMG-CoA reductase inhibitors demonstrate differential activation of the nuclear receptors PXR, CAR and FXR, as well as their downstream target genes

et al. 2011

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Section: Methodsmentioning

confidence: 99%

The statin class of HMG-CoA reductase inhibitors demonstrate differential activation of the nuclear receptors PXR, CAR and FXR, as well as their downstream target genes

et al. 2011

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“…Docking of hyperforin was started from its X-ray position in 1M13. Subsequently, docking of rifampicin was started after superimposing the hPXR-rifampicin complex 1SKX (Chrencik et al, 2005) onto 1M13. The PXR antagonist A-792611 was built from the similar HIV-protease inhibitor in Protein Data Bank ID 3GGV (Degoey et al, 2009), guided by the structure drawing from Healan-Greenberg et al (2008).…”

Section: Cyp3a4 Reporter Gene Assaymentioning

confidence: 99%

Milk Thistle’s Active Components Silybin and Isosilybin: Novel Inhibitors of PXR-Mediated CYP3A4 Induction

et al. 2013

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Because cancer is often treated with combination therapy, unexpected pharmacological effects can occur because of drug-drug interactions. Several drugs are able to cause upregulation or downregulation of drug transporters or cytochrome P450 enzymes, particularly CYP3A4. Induction of CYP3A4 may result in decreased plasma levels and therapeutic efficacy of anticancer drugs. Since the pregnane X receptor (PXR) is one of the major transcriptional regulators of CYP3A4, PXR antagonists can possibly prevent CYP3A4 induction. Currently, a limited number of PXR antagonists are available. Some of these antagonists, such as sulphoraphane and coumestrol, belong to the so-called complementary and alternative medicines (CAM). Therefore, the aim was to determine the potential of selected CAM (b-carotene, Echinacea purpurea, garlic, Ginkgo biloba, ginseng, grape seed, green tea, milk thistle, saw palmetto, valerian, St. John's Wort, and vitamins B 6 , B 12 , and C) to inhibit PXR-mediated CYP3A4 induction at the transcriptional level, using a reporter gene assay and a real-time polymerase chain reaction assay in LS180 colon adenocarcinoma cells. Furthermore, computational molecular docking and a LanthaScreen time-resolved fluorescence resonance energy transfer (TR-FRET) PXR competitive binding assay were performed to explore whether the inhibiting CAM components interact with PXR. The results demonstrated that milk thistle is a strong inhibitor of PXR-mediated CYP3A4 induction. The components of milk thistle responsible for this effect were identified as silybin and isosilybin. Furthermore, computational molecular docking revealed a strong interaction between both silybin and isosilybin and PXR, which was confirmed in the TR-FRET PXR assay. In conclusion, silybin and isosilybin might be suitable candidates to design potent PXR antagonists to prevent drug-drug interactions via CYP3A4 in cancer patients.

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“…For example, coadministration of rifampicin, a hPXR activator used for treatment of tuberculosis (Chrencik et al, 2005) with a variety of drugs [including oral contraceptives (Ma et al, 2008), the anesthetic midazolam (Backman et al, 1996), and HIV protease inhibitors (Ivanovic et al, 2008)], resulted in decreased drug efficacy mainly due to hPXR-mediated increased expression of CYP3A4 (Ivanovic et al, 2008;Ma et al, 2008;di Masi et al, 2009). Thus, identification of novel hPXR activators among commercial drugs is important in predicting hPXR-mediated drug-drug interactions.…”

Section: Introductionmentioning

confidence: 99%

“…Crystal structures of the hPXR ligand-binding domain (LBD) indicate that its binding cavity is much larger than that of other NR family members (Xu et al, 2004;Chrencik et al, 2005;di Masi et al, 2009). Several key amino acid residues are responsible for the high flexibility of its binding site that is critical for recognizing promiscuous ligands of various dimensions and chemical properties (Ekins et al, 2009).…”

Section: Introductionmentioning

confidence: 99%

Identification and Validation of Novel Human Pregnane X Receptor Activators among Prescribed Drugs via Ligand-Based Virtual Screening

Pan

Li²,

Gregory³

et al. 2010

Drug Metab Dispos

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ABSTRACT:Human pregnane X receptor (hPXR) plays a key role in regulating metabolism and clearance of endogenous and exogenous substances. Identification of novel hPXR activators among commercial drugs may aid in avoiding drug-drug interactions during coadministration. We applied ligand-based computational approaches for virtual screening of a commonly prescribed drug database (SCUT). Bayesian classification models were generated with a training set comprising 177 compounds using Fingerprints and 117 structural descriptors. A cell-based luciferase reporter assay was used for evaluation of chemical-mediated hPXR activation in HepG2 cells. All compounds were tested at 10 M concentration with rifampicin and dimethyl sulfoxide as positive and negative controls, respectively. The Bayesian models showed specificity and overall prediction accuracy up to 0.92 and 0.69 for test set compounds. Screening the SCUT database with this model retrieved 105 hits and 17 compounds from the top 25 hits were chosen for in vitro testing. The reporter assay confirmed that nine drugs, i.e., fluticasone, nimodipine, nisoldipine, beclomethasone, finasteride, flunisolide, megestrol, secobarbital, and aminoglutethimide, were previously unidentified hPXR activators. Thus, the present study demonstrates that novel hPXR activators can be efficiently identified among U.S. Food and Drug Administrationapproved and commonly prescribed drugs, which should lead to detection and prevention of potential drug-drug interactions.

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Structural Disorder in the Complex of Human Pregnane X Receptor and the Macrolide Antibiotic Rifampicin

Cited by 183 publications

References 28 publications

The statin class of HMG-CoA reductase inhibitors demonstrate differential activation of the nuclear receptors PXR, CAR and FXR, as well as their downstream target genes

The statin class of HMG-CoA reductase inhibitors demonstrate differential activation of the nuclear receptors PXR, CAR and FXR, as well as their downstream target genes

Milk Thistle’s Active Components Silybin and Isosilybin: Novel Inhibitors of PXR-Mediated CYP3A4 Induction

Identification and Validation of Novel Human Pregnane X Receptor Activators among Prescribed Drugs via Ligand-Based Virtual Screening

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