SEQUENTIAL OXIDATION AND GLUTATHIONE ADDITION TO 1,4-BENZOQUINONE - CORRELATION OF TOXICITY WITH INCREASED GLUTATHIONE SUBSTITUTION
- 1 December 1988
- journal article
- research article
- Vol. 34 (6) , 829-836
Abstract
The chemical reaction of 1,4-benzoquinone with glutathione results in the formation of adducts that exhibit increasing degrees of glutathione substitution. Purification of these adducts and analysis by 1H and 13C nuclear magnetic resonance spectroscopy revealed the products of the reaction to be 2-(glutathion-S-yl)hydroquinone; 2,3-(diglutathion-S-yl)hydroquinone; 2,5-(diglutathion-S-yl)hydroquinone; 2,6(diglutathion-S-yl)hydroquinone; 2,3,5-(triglutathion-S-yl)hydroquinone; and 2,3,5,6-(tetraglutathion-S-yl)hydroquinone. The initial conjugation of 1,4-benzoquinone with glutathione did not significantly affect the oxidation potential of the compound. However, subsequent oxidation and glutathione addition resulted in the formation of conjugates that, dependent upon the position of addition, become increasingly more difficult to oxidize. Increased glutathione substitutions, which resulted in an increase in oxidation potentials, paradoxically resulted in enhanced nephrotoxicity. The triglutathion-S-yl conjugate was the most nephrotoxicant; the diglutathion-S-yl conjugates exhibited similar degrees of nephrotoxicity; the mono- and tetraglutathion-S-yl conjugates were not toxic. Thus, with the exception of the fully substituted isomer, the severity of renal necrosis correlated with the extent of glutathione substitution. The lack of toxicity of the fully substituted isomer is probably a consequence of its inability to alkylate tissue components. Thus, the conjugation of glutathione with quinones does not necessarily result in detoxification, even when the resulting conjugates are more stable to oxidation. The inhibition of .gamma.-glutamyl transpeptidase by AT-125 protected against 2,3,5-(triglutathion-S-yl)hydroquinone-mediated nephrotoxicity. It is suggested that other extra-renal sites expressing relatively high levels of .gamma.-glutamyl transpeptidase might therefore also be susceptible to hydroquinone-linked glutathione conjugate toxicity. This pathway might also contribute to the carcinogenicity and mutagenicity of certain quinones.This publication has 26 references indexed in Scilit:
- Alteration by phenobarbital of membrane-associated enzymes including gamma glutamyl transpeptidase in mouse liver neoplasmsCarcinogenesis: Integrative Cancer Research, 1980
- The inhibition of γ-glutamyl transpeptidase and glutathione metabolism of isolated rat kidney cells by L-(αS, 5S)-α-amino-3-chloro-4, 5-dihydro-5-isoxazoleacetic acid (AT-125; NSC-163501)Biochemical and Biophysical Research Communications, 1980
- INHIBITION OF GAMMA-GLUTAMYL-TRANSFERASE TRANSPEPTIDASE FROM HUMAN PANCREATIC-CARCINOMA CELLS BY (ALPHA-S,5S)-ALPHA-AMINO-3-CHLORO-4,5-DIHYDRO-5-ISOXAZOLEACETIC ACID (AT-125 - NSC-163501)1980
- N-ACYL-GAMMA-GLUTAMYL DERIVATIVES OF SULFAMETHOXAZOLE AS MODELS OF KIDNEY-SELECTIVE PRODRUGS1980
- Metabolism of γ-glutamyl dopamide and its carboxylic acid estersBiochemical Pharmacology, 1980
- Structural analogs of L-glutamic acid .gamma.-(4-hydroxyanilide) and .gamma.-(3,4-dihydroxyanilide) as potential agents against melanomaJournal of Medicinal Chemistry, 1979
- Differences in the isoelectric focusing patterns of gamma-glutamyl transpeptidase from normal and cancerous rat mammary tissue.Proceedings of the National Academy of Sciences, 1978
- GAMMA-GLUTAMYL DOPA - KIDNEY-SPECIFIC DOPAMINE PRECURSOR1978
- Glutathione and Gamma Glutamyl Transpeptidase in Rat Liver During Chemical Carcinogenesis23JNCI Journal of the National Cancer Institute, 1976
- Studies on Quinone-Thioethers. I. Mechanism of Formation and Properties of Thiodione*Biochemistry, 1963