TY - JOUR T1 - Evaluation of the Kinetics of β-Elimination Reactions of Selenocysteine Se-Conjugates in Human Renal Cytosol: Possible Implications for the Use as Kidney Selective Prodrugs JF - Journal of Pharmacology and Experimental Therapeutics JO - J Pharmacol Exp Ther SP - 762 LP - 769 VL - 294 IS - 2 AU - Martijn Rooseboom AU - Nico P. E. Vermeulen AU - Ioanna Andreadou AU - Jan N. M. Commandeur Y1 - 2000/08/01 UR - http://jpet.aspetjournals.org/content/294/2/762.abstract N2 - This study was performed to evaluate whether selenocysteine Se-conjugates are substrates for human cysteine conjugate β-lyase enzymes. By testing kidney cytosols of three different humans, we studied interindividual differences in β-lyase enzymes in humans. A series of 22 selenocysteine Se-conjugates were tested in rat and human kidney cytosols to compare their ability to form selenol compounds by β-elimination. All compounds appeared to be good substrates for rat and human cysteine conjugate β-lyase enzymes. The β-lyase activity toward the selenocysteine Se-conjugates was comparable with those of the known nephrotoxic cysteine S-conjugateS-(2-chloro-1,1,2-trifluoroethyl)-l-cysteine in rats and humans. In rat kidney cytosol, between 22- and 877-fold higher β-elimination rates were observed compared with human kidney cytosol. Significant correlations (P < .0001) between three human kidney cytosols in β-lyase activities were found within the tested series of 22 compounds. Specific β-lyase activities and intrinsic clearances of β-elimination reactions ranged up to 3-fold, indicating that there are quantitative rather than qualitative interindividual differences in β-eliminating enzymes in humans. Furthermore, Se-alkyl selenocysteine conjugates showed a sterically dependent bioactivation to selenol compounds in humans but not in rats. The present study supports the hypothesis that selenocysteine Se-conjugates may be useful as prodrugs to target pharmacologically active selenol compounds (e.g., antitumor or chemoprotective) to the kidney in humans. The American Society for Pharmacology and Experimental Therapeutics ER -