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Journal of Toxicology and Environmental Health, Part A
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Volume 68, 2005 - Issue 4
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Original Articles

Characterization of the Metabolic Interaction between Trihalomethanes and Chloroacetic Acids using Rat Liver Microsomes

Annie St-Pierre TOXHUM (Groupe de recherche en toxicologie humaine), Département de Santé Environnementale et Santé au Travail, Université de Montréal, Montréal, Québec, Canada
,
Kannan Krishnan TOXHUM (Groupe de recherche en toxicologie humaine), Département de Santé Environnementale et Santé au Travail, Université de Montréal, Montréal, Québec, Canada
&
Robert Tardif TOXHUM (Groupe de recherche en toxicologie humaine), Département de Santé Environnementale et Santé au Travail, Université de Montréal, Montréal, Québec, CanadaCorrespondence[email protected]
Pages 287-298 | Published online: 24 Feb 2007
 
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Abstract

The aim of this study was to investigate the in vitro metabolism of trihalomethanes (THMs) in the presence of trichloroacetic acid (TCA), dichloracetic acid (DCA), monochloroacetic acid (MCA), and 4-methylpyrazole (4-MP) using liver microsomes from male Sprague-Dawley rats. Using the vial equilibration technique, initial experiments were carried out with starting concentrations of approximately 40 ppm THMs and 12–22 mMchloroacetic acids.The results indicated a mutual metabolic inhibition between THMs present as binary or quaternary mixtures. Although DCA and MCA had no influence on THMs, TCA produced a marked inhibition of the metabolism of all THMs: chloroform (CHCl3) (55%), bromodichloromethane (BDCM) (34%), dibromochloromethane (DBCM) (30%), and bromoform (TBM) (23%). The presence of 4-MP also reduced THM metabolism, the importance of which decreased in the following order: CHCl3 > BDCM > DBCM = TBM. In further vial equilibration experiments, using 9–140 ppm as starting concentrations of THMs, enzyme kinetic parameters (i.e., Michaelis constant, K m, and maximum velocity, V max) were determined both in the absence and in the presence of TCA (12.2 mM). Results are consistent with a competitive inhibition between TCA and CHCl3, whereas the metabolic inhibition of BDCM and TMB by TCA was non-competitive. As for DBCM, results suggest a more complex pattern of inhibition. These results suggest that CYP2E1 is involved in the metabolism of THMs as well as in the metabolic interaction between THMs and TCA.

We thank Mylène Beaudoin for her excellent technical assistance during this study. This work was supported by the Toxic Substances Research Initiative (TSRI) of Health Canada and Environment Canada

Notes

We thank Mylène Beaudoin for her excellent technical assistance during this study. This work was supported by the Toxic Substances Research Initiative (TSRI) of Health Canada and Environment Canada

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