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Vol. 304, Issue 1, 121-129, January 2003
Departments of Anatomy and Cell Biology (E.J.M., P.G.F.) and
Pharmacology and Toxicology (W.J.R.), Queen's University,
Kingston, Ontario, Canada
Hepatotoxicity induced by 1,1-dichloroethylene (DCE) is mediated by
cytochrome P450-dependent metabolism to reactive intermediates, including the epoxide. We have tested the hypothesis that mitochondria are a primary target of toxicity by investigating dose- and
time-dependent effects of DCE on mitochondrial respiration.
Hepatotoxicity, as assessed by serum alanine aminotransferase (ALT)
activity, was evaluated. We have also determined the effectiveness of
N-acetyl-L-cysteine (NAC) in protecting
against respiratory perturbations and hepatotoxicity. Liver
mitochondria were isolated 2 h after DCE (50, 75, 100, 125, and
150 mg/kg) treatment. Glutamate (complex I)- and succinate (complex
II)-supported mitochondrial respiration was assessed by measurement of
state 3 (ADP-stimulated) and state 4 (resting) rates of oxygen
consumption. The corresponding respiratory control ratios (RCRs, state
3/state 4) and ADP:O ratios were then calculated. A DCE dose of 125 mg/kg significantly inhibited glutamate- and succinate-supported state
3 respiration, leading to a significant reduction in corresponding RCRs
and ADP:O ratios. In time-dependent studies, state 3 respiration rates
and RCRs for glutamate-supported respiration were significantly
decreased as early as 20 min after DCE (125 mg/kg) treatment, whereas
those for succinate-supported respiration were significantly decreased
at 90 min. Additionally, ADP:O ratios for glutamate-supported
respiration were significantly decreased starting at 60 min, and those
for succinate-supported respiration at 90 min. Alterations in
mitochondrial function preceded significant increases in ALT activity,
which was first manifested at 2 h. Pretreatment with NAC (1200 mg/kg) abrogated DCE-induced GSH depletion and inhibited disturbances
in mitochondrial respiration. Moreover, NAC protected against increased
ALT activity, suggesting that the protective effect of NAC is due to
increased GSH for conjugation reactions and/or its antioxidant
property. These results showed that DCE-mediated mitochondrial
dysfunction is an early event that preceded the onset of hepatotoxicity.
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