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The molecular mechanisms of diallyl disulfide and diallyl sulfide induced hepatocyte cytotoxicity
Authors:D Truong
Institution:Graduate Department of Pharmaceutical Sciences, Faculty of Pharmacy, University of Toronto, 144 College St, Toronto, Ontario, Canada M5S 3M2
Abstract:Diallyl disulfide (DADS) and diallyl sulfide (DAS) are the major metabolites found in garlic oil and have been reported to lower cholesterol and prevent cancer. The molecular cytotoxic mechanisms of DADS and DAS have not been determined.The cytotoxic effectiveness of hydrogen versus allyl sulfides towards hepatocytes was found to be as follows: NaHS > DADS > DAS. Hepatocyte mitochondrial membrane potential was decreased and reactive oxygen species (ROS) and TBARS formation was increased by all three allyl sulfides. (1) DADS induced cytotoxicity was prevented by the H2S scavenger hydroxocobalamin, which also prevented cytochrome oxidase dependent mitochondrial respiration suggesting that H2S inhibition of cytochrome oxidase contributed to DADS hepatocyte cytotoxicity. (2) DAS cytotoxicity on the other hand was prevented by hydralazine, an acrolein trap. Hydralazine also prevented DAS induced GSH depletion, decreased mitochondrial membrane potential and increased ROS and TBARS formation. Chloral hydrate, the aldehyde dehydrogenase 2 inhibitor, however had the opposite effects, which could suggest that acrolein contributed to DAS hepatocyte cytotoxicity.
Keywords:DADS  diallyl disulfide  DAS  diallyl sulfide  NaHS  sodium hydrosulfide  H2S  hydrogen sulfide  PM  propyl mercaptan  AM  allyl mercaptan  AMS  allyl methyl sulfide  AMSO  allyl methyl sulfoxide  AMSO2  allyl methyl sulfone  DASO  diallyl sulfone  DASO2  diallyl sulfoxide  ROS  reactive oxygen species  TBARS  thiobarbituric acid reactive species  ALDH2  aldehyde dehydrogenase 2  DTT  dithiothreitol  GST  glutathione-s-transferase
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