Dexamethasone Differentially Regulates Expression of Carboxylesterase Genes in Humans and Rats

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Vol. 28, Issue 2, 186-191, February 2000

Dexamethasone Differentially Regulates Expression of Carboxylesterase Genes in Humans and Rats

Weizhu Zhu,¹ Li Song,¹ He Zhang, Lynn Matoney, Edward LeCluyse,² and Bingfang Yan

Department of Biomedical Sciences, University of Rhode Island, Kingston, Rhode Island.

Carboxylesterases play important roles in the metabolism of endogenous and foreign compounds, therefore, xenobiotic regulationof carboxylesterase gene expression has both physiological andpharmacological significance. We previously reported that livermicrosomal esterase activity was significantly decreased in ratstreated with dexamethasone accompanied by a decrease in immunoreactiveproteins of rat hydrolase A, B, and C. The aim of this study wasto determine whether the suppressed expression of these enzymeswas linked to the change of the mRNA levels, and whether culturedhepatocytes responded similar to whole animals to this chemical.Northern blotting analyses demonstrated that the levels of thecorresponding mRNA were markedly decreased in rats treated withdexamethasone, suggesting that the suppressed expression is achievedthrough trans-suppression and/or increased degradation of thetranscripts. Exposure of cultured rat hepatocytes to nanomolarlevels of dexamethasone markedly decreased the levels of immunoreactiveproteins of hydrolase A, B, and C. In contrast, exposure of culturedhuman hepatocytes to dexamethasone caused a slight increase inHCE-1 and HCE-2, two major forms of human liver microsomal carboxylesterases.The inductive effects in human hepatocytes were observed onlywhen micromolar concentrations of dexamethasone were used. Theseresults suggest that a major species difference exists regardingthe regulation of carboxylesterase gene expression by dexamethasone.Both the glucocorticoid receptor and the pregnane X receptor areknown to mediate dexamethasone action. Differential concentrationsrequired suggest that suppression of rat hydrolases is mediatedby the glucocorticoid receptor, whereas the induction of humancarboxylesterases is mediated by the pregnane Xreceptor.

¹ Equal contributions were made by theseauthors.

² Present address: Department of Drug Delivery and Disposition, School of Pharmacy, University of North Carolina at Chapel Hill,Chapel Hill, NC27599.

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