Abstract
The formation of cysteine S-conjugates is thought to play an important role in the nephrotoxicity of haloalkenes such as trichloroethene, tetrachloroethene and hexachlorobutadiene. Glutathione S-conjugates formed from these haloalkenes in the liver are processed to the corresponding cysteine S-conjugates, which may be N-acetylated to mercapturic acids and may be accumulated in the kidney. Haloalkene-derived cysteine S-conjugates are also substrates for cysteine conjugate β-lyases and reactive intermediates are formed in this reaction. The equilibrium between cysteine S-conjugate and mercapturic acid thus influences the extent of β-lyase dependent bioactivation and subsequently the nephrotoxicity of S-conjugates. In this study,␣we compared the rates of N-acetylation in vitro and the biotransformation, excretion and nephro‐ toxicity of S-(1,2-dichlorovinyl)-l-cysteine (1,2-DCVC), S-(2,2-dichlorovinyl)-l-cysteine (2,2-DCVC), S-(1,2,2-trichlorovinyl)-l-cysteine (TCVC) and S-(1,2,3,4,4-pentachlorobutadienyl)-l-cysteine (PCBC) in rats after i.v. injection (40 μmoles/kg). Marked differences in the extent of enzymatic N-acetylation were observed; N-acetylation was most efficient with 2,2-DCVC and least efficient with 1,2-DCVC. In urine, within 48 h, most of the given 2,2-DCVC (77% of the recovered dose) and 1,2-DCVC (92%) were recovered as the corresponding mercapturic acids. In contrast, a higher percentage of cysteine S-conjugate and less of the mercapturic acid were recovered in urine after administration of PCBC and TCVC (50 and 23% of dose as mercapturic acid), respectively. Histopathological examination of the kidneys and urine clinical chemistry showed marked differences in the extent of renal damage. Necroses of the proximal tubules were found after TCVC, PCBC and 1,2-DCVC administration in male, but not in female rats. These differences in nephrotoxicity do not correlate with the balance of acetylation/deacetylation. The higher toxicity observed in male rats may indicate the involvement of other parameters such as uptake mechanisms.
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Received: 30 April 1997 / Accepted: 26 August 1997
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Birner, G., Bernauer, U., Werner, M. et al. Biotransformation, excretion and nephrotoxicity of haloalkene-derived cysteine S-conjugates. Arch Toxicol 72, 1–8 (1997). https://doi.org/10.1007/s002040050461
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DOI: https://doi.org/10.1007/s002040050461