Hepatic metabolism of chlorinated derivatives of bisphenol A (ClBPA) and interspecies differences between rats and humans.

Arch Toxicol

Department of Environmental and Occupational Health, School of Public Health, CReSP, Université de Montréal, Montreal, QC, Canada.

Published: March 2022

During chlorination treatments of drinking water, aqueous bisphenol A (BPA) can react with chlorine to form chlorinated derivatives of BPA (mono, di, tri and tetra-chlorinated derivatives) or ClBPA. These emerging substances are endocrine disruptors associated with obesity, type II diabetes (TD2M) and myocardial infarction. ClBPA are present in different human biological matrices but their toxicokinetics remain unknown. The aim of this study was to measure and compare the metabolic kinetics in the liver of four ClBPA (ClBPA, ClBPA, ClBPA and ClBPA) between compounds and between species (Sprague-Dawley rats vs humans). To estimate their metabolic constants (V, K, Intrinsic clearance), metabolic assays were performed in hepatocyte suspensions. Assays revealed that metabolic constants of ClBPA can greatly vary depending on substances and species. While ClBPA and ClBPA show similar unbound intrinsic clearances (ClintU) in rat incubation media, values for ClBPA and ClBPA are very different (3.109 and 0.684 mL/min/106 hepatocytes, respectively). Unlike in rats, human results are quite different as ClBPA and ClBPA have similar unbound intrinsic clearances, while ClBPA and ClBPA diverge (0.350 and 1.363 mL/min/106 hepatocytes, respectively). In both species, ClBPA and Cl3BPA have relatively similar clearances, and ClBPA is very different from ClBPA. Although we quantified the proportion of sulfo- and glucurono-metabolites, other metabolites may have been formed (e.g., glutathione, disulfate, or oxidative metabolites). This study showed that chlorination had an impact on hepatic intrinsic clearance of ClBPA in rats and humans and measured values will be valuable for the development of PBPK models for use in exposure assessment.

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Source
http://dx.doi.org/10.1007/s00204-021-03217-7DOI Listing

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