Quesnot, Nicolas; Bucher, Simon; Gade, Christina; Vlach, Manuel; Vene, Elise; Valença, Samuel; Gicquel, Thomas; Holst, Helle; Robin, Marie-Anne; Loyer, Pascal

doi:10.1007/s00204-018-2300-2

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Title: Production of chlorzoxazone glucuronides via cytochrome P4502E1 dependent and independent pathways in human hepatocytes.
Authors: Quesnot, Nicolas; Bucher, Simon; Gade, Christina; Vlach, Manuel; Vene, Elise; Valença, Samuel; Gicquel, Thomas; Holst, Helle; Robin, Marie-Anne; Loyer, Pascal
Abstract: CYP2E1 activity is measured in vitro and in vivo via hydroxylation of the Chlorzoxazone (CHZ) producing the 6-hydroxychlorzoxazone (OH-CHZ) further metabolized as a glucuronide excreted in urine. Thus, the quantification of the OH-CHZ following enzymatic hydrolysis of CHZ-derived glucuronide appears to be a reliable assay to measure the CYP2E1 activity without direct detection of this glucuronide. However, OH-CHZ hydrolyzed from urinary glucuronide accounts for less than 80% of the CHZ administrated dose in humans leading to postulate the production of other unidentified metabolites. Moreover, the Uridine 5′-diphospho-glucuronosyltransferase (UGT) involved in the hepatic glucuronidation of OH-CHZ has not yet been identified. In this study, we used recombinant HepG2 cells expressing CYP2E1, metabolically competent HepaRG cells, primary hepatocytes and precision-cut human liver slices to identify metabolites of CHZ (300 μM) by high pressure liquid chromatography-UV and liquid-chromatography-mass spectrometry analyses. Herein, we report the detection of the CHZ-O-glucuronide (CHZ-O-Glc) derived from OH-CHZ in culture media but also in mouse and human urine and we identified a novel CHZ metabolite, the CHZ-N-glucuronide (CHZ-N-Glc), which is resistant to enzymatic hydrolysis and produced independently of CHZ hydroxylation by CYP2E1. Moreover, we demonstrate that UGT1A1, 1A6 and 1A9 proteins catalyze the synthesis of CHZ-O-Glc while CHZ-N-Glc is produced by UGT1A9 specifically. Together, we demonstrated that hydrolysis of CHZ-O-Glc is required to reliably quantify CYP2E1 activity because of the rapid transformation of OH-CHZ into CHZ-O-Glc and identified the CHZ-N-Glc produced independently of the CYP2E1 activity. Our results also raise the questions of the contribution of CHZ-N-Glc in the overall CHZ metabolism and of the quantification of CHZ glucuronides in vitro and in vivo for measuring UGT1A activities.
Subjects: HYDROXYLATION; CHLORZOXAZONE; LIVER cells; GLUCURONIDES; HYDROLYSIS; METABOLITES; HIGH performance liquid chromatography
Publication: Archives of Toxicology, 2018, Vol 92, Issue 10, p3077
ISSN: 0340-5761
Publication type: Academic Journal
DOI: 10.1007/s00204-018-2300-2

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Production of chlorzoxazone glucuronides via cytochrome P4502E1 dependent and independent pathways in human hepatocytes.

Quesnot, Nicolas; Bucher, Simon; Gade, Christina; Vlach, Manuel; Vene, Elise; Valença, Samuel; Gicquel, Thomas; Holst, Helle; Robin, Marie-Anne; Loyer, Pascal

HYDROXYLATION; CHLORZOXAZONE; LIVER cells; GLUCURONIDES; HYDROLYSIS; METABOLITES; HIGH performance liquid chromatography

Archives of Toxicology, 2018, Vol 92, Issue 10, p3077

0340-5761

Academic Journal

10.1007/s00204-018-2300-2