Pregnane X Receptor Protects HepG2 Cells from BaP-Induced DNA Damage

doi:10.1093/toxsci/kfn058

ToxSci Advance Access originally published online on April 1, 2008
Toxicological Sciences 2008 104(1):67-73; doi:10.1093/toxsci/kfn058

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Pregnane X Receptor Protects HepG2 Cells from BaP-Induced DNA Damage

Christine Naspinski^*, Xinsheng Gu^*, Guo-Dong Zhou, Susanne U. Mertens-Talcott^*, Kirby C. Donnelly^*^, and Yanan Tian^*^,1

^* College of Veterinary Medicine and Biomedical Sciences School of Rural Public Health, Texas A&M University System Health Science Center, College Station, Texas 77843

¹ To whom correspondence should be addressed at Department of Veterinary Physiology and Pharmacology, Mail Stop 4466, Texas A&M University, College Station, TX 77843. Fax: (979) 458-4485. E-mail: ytian{at}cvm.tamu.edu.

Received December 4, 2007; accepted March 14, 2008

Abstract

Pregnane X receptor (PXR) is a nuclear receptor that coordinatelyregulates transcriptional expression of both phase I and phaseII metabolizing enzymes. PXR plays an important role in thepharmacokinetics of a broad spectrum of endogenous and xenobioticcompounds and appears to have evolved in part to protect organismsfrom toxic xenobiotics. Metabolism of benzo[a]pyrene (BaP),a well-established carcinogen and ubiquitous environmental contaminant,can result in either detoxification or bioactivation to itsgenotoxic forms. Therefore, PXR could modulate the genotoxicityof BaP by changing the balance of the metabolic pathways infavor of BaP detoxification. To examine the role of PXR in BaPgenotoxicity, BaP–DNA adduct formation was measured by³²P-postlabeling in BaP-treated parental HepG2 cells and humanPXR-transfected HepG2 cells. The presence of transfected PXRsignificantly reduced the level of adducts relative to parentalcells by 50–65% (p < 0.001), demonstrating that PXRprotects liver cells from genotoxicity induced by exposure toBaP. To analyze potential PXR-regulated detoxification pathwaysin liver cells, a panel of genes involved in phase I and phaseII metabolism and excretion was surveyed with real-time quantitativereverse transcription PCR. The messenger RNA levels of CYP1A2,GSTA1, GSTA2, GSTM1, UGT1A6, and BCRP (ABCG2) were significantlyhigher in cells overexpressing PXR, independent of exposureto BaP. In addition, the total GST enzymatic activity, whichfavors the metabolic detoxification of BaP, was significantlyincreased by the presence of PXR (p < 0.001), independentof BaP exposure. Taken together, these results suggest thatPXR plays an important role in protection against DNA damageby polycyclic aromatic hydrocarbons (PAHs) such as BaP, andthat these protective effects may be through a coordinated regulationof genes involved in xenobiotic metabolism.

Key Words: benzo[a]pyrene; pregnane X receptor; DNA adducts; HepG2.

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