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S Ouwerkerk-Mahadevan, JH van Boom and GJ Mulder
Division of Toxicoloy, Leiden/Amsterdam Center for Drug Research, The Netherlands.
Glutathione S-transferases (GSTs) play a major role in the (de- )toxification of many endogenous and xenobiotic substrates. To assess their contribution in (de-)toxification, specific in vivo inhibitors that ideally are selective for a single isoenzyme of GST are required. In the present study, selective inhibition of the alpha class GST by the glutathione analog (R)-5-ethyloxycarbonyl-2-gamma-(S)-glutamylamino- N-2-hept ylpentamide (Et-R-Hep) was studied. In rat liver cytosol and in isolated rat hepatocytes, only the conjugation of the (S)-enantiomer of (RS)-2-bromoisovalerylurea (BIU), which is conjugated mainly by alpha class GST 2-2 (Te Koppele et al., Biochem. J. 252:137-142, 1988), was inhibited by Et-R-hep. The conjugation of (R)-BIU, which is mainly catalyzed by millimicron class GSTs 3-3 and 4-4, was unaffected. In anesthetized rats to which an infusion of (RS)-BIU was administered, the biliary excretion of the glutathione conjugate of (S)-BIU was inhibited by up to 67% after administration of Et-R-hep (an i.v. bolus dose of 200 mu mol/kg followed by an infusion of 6.7 mu mol/min/kg for 30 min). The extent of inhibition decreased gradually to reach 40% at the end of the experiment (4 hr after administration of the inhibitor). The conjugation of (R)-BIU was unaffected. Thus, the inhibitor Et-R-Hep shows preferential inhibition of the alpha-GST substrate (S)-BIU. Although Et-R-Hep is not specific for alpha class GST, it may be used to assess the role of this class of GST in (de)-toxification and conjugation in vivo.
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  S. Ouwerkerk-Mahadevan, R. G. Tirona, R. A. Ripping, J. H. T. M. Ploemen, P. J. van Bladeren, K. S. Pang, J. H. van Boom, and G. J. Mulder Inhibition of Glutathione Conjugation by Glutathione Analogues in the Perfused Rat Liver. Effect of Esterification on the Potency of gamma -L-Glutamyl-alpha -(D-2-Aminoadipyl)- N-2-Heptylamine Drug Metab. Dispos., October 1, 1997; 25(10): 1137 - 1143. [Abstract] [Full Text]
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