Lipid peroxidation, protein synthesis, and protection by calcium EDTA in paracetamol injury to isolated hepatocytes |
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Authors: | D Beales D P Hue A E McLean |
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Affiliation: | 1. Department of Oceanography, Dalhousie University, 1355 Oxford Street, P.O. Box 15000, Halifax, Nova Scotia B3H 4R2, Canada;2. Bedford Institute of Oceanography, Department of Fisheries and Oceans, Dartmouth, Nova Scotia B2Y 4A2, Canada;3. Antarctic Climate & Ecosystems Cooperative Research Centre, University of Tasmania, Hobart, Tasmania, Australia |
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Abstract: | ![]() Hepatocytes from rats treated with phenobarbitone were exposed to 10 mM paracetamol for 1 hr and then incubated in buffered Ringer solution. Enzyme leakage and trypan blue entry became severe in the paracetamol treated cells some 2 hr after the end of exposure. These signs of cell injury could be blocked by 4 mM CaEDTA added during or after paracetamol exposure. CaEDTA did not alter covalent binding of [14C]paracetamol. Ca2+ free media did not prevent paracetamol injury. Lipid peroxidation was observed in cells but could be blocked without protecting the cells. Protein synthesis was depressed early on in cells previously exposed to paracetamol, CaEDTA did not protect against this inhibition. These observations suggest that an early cytoplasmic lesion develops into a later lethal lesion at the cell surface. |
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