Induction of multidrug resistance gene expression during... : Hepatology (original) (raw)
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Induction of multidrug resistance gene expression during cholestasis in rats and nonhuman primates
Schrenk, Dieter1; Gant, Timothy W.1; Preisegger, Karl-Heinz1; Silverman, Jeffrey A.1; Marino, Pamela A.1; Thorgeirsson, Snorri S. M.D.*, 1
1_Laboratory of Experimental Carcinogenesis, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892_
*Address reprint requests to: National Cancer Institute, Building 37, Room 3C28, Bethesda, MD 20892
Received August 06, 1992; accepted December 10, 1992; previously published online December 05, 2005
Abstract
P-glycoprotein, an energy-dependent plasma membrane drug-efflux pump capable of reducing the intracellular concentration of a variety of hydrophobic xenobiotics, is encoded by mdr 1, a member of the multidrug-resistant (mdr) gene family. The physiological function of this protein is unknown. Because of its location on the bile canalicular domain of the hepatocyte, we and others have hypothesized that P-glycoprotein may have a physiological role as a biliary transporter of xenobiotics and endobiotics and that its expression may therefore be altered in cholestasis. Both obstructive and α-naphthylisothiocyanate-induced cholestasis increased mdr 1a and 1b gene expression in rat liver. Hepatic P-glycoprotein levels were also increased, and the protein remained localized at the biliary hepatocyte domain. Induction of mdr 1a and mdr 1b gene expression in rat liver was accomplished by means of increased transcription. α-Naphthylisothiocyanate-induced cholestasis in cynomolgus monkeys increased hepatic expression of both the mdr 1 and 2 genes. To investigate the possible role of P-glycoprotein as a biliary efflux transporter, biliary excretion of vinblastine, a representative substrate of P-glycoprotein, was studied in rats. Increased hepatic mdr messenger RNA and P-glycoprotein levels, mediated by the xenobiotic inducer 2-acetylaminofluorene, resulted in a significant increase in biliary excretion of vinblastine, which was antagonized by the P-glycoprotein inhibitor verapamil. These findings suggest that P-glycoprotein functions as a biiary efflux pump for xenobiotics and, possibly, for unidentified physiological inducers that may mediate increased transcription of the mdr gene observed during cholestasis. (Hepatology 1993;17:854-860.)
Copyright © 1993 American Association for the Study of Liver Diseases.