Inhibition of ferrous‐induced lipid peroxidation by pyrimido‐pyrimidine derivatives in human liver membranes

The effects of pyrimido‐pyrimidine derivatives (dipyridamole, RA‐642, and RA‐233) on lipid peroxidation, using d‐α‐tocopherol as standard, were studied in enriched membrane fractions from human and rat hepatocytes. Equimolar concentrations of ferrous sulfate and ascorbic acid were used to induce lip...

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Veröffentlicht in:	Lipids 1992-03, Vol.27 (3), p.192-194
Hauptverfasser:	Cruz, J. P., Carrasco, T., Ortega, G., Cuesta, F. Sanchez
Format:	Artikel
Sprache:	eng
Schlagworte:	Animals Ascorbic Acid - pharmacology Biological and medical sciences Cardiotonic Agents - pharmacology Cell Membrane - drug effects Cell Membrane - metabolism Dipyridamole - pharmacology Ferrous Compounds - pharmacology General and cellular metabolism. Vitamins Humans Kinetics Lipid Peroxidation - drug effects Liver - metabolism Malondialdehyde - metabolism Medical sciences Mopidamol - pharmacology Pharmacology. Drug treatments Pyrimidines - pharmacology Rats Species Specificity Vitamin E - pharmacology
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Zusammenfassung:	The effects of pyrimido‐pyrimidine derivatives (dipyridamole, RA‐642, and RA‐233) on lipid peroxidation, using d‐α‐tocopherol as standard, were studied in enriched membrane fractions from human and rat hepatocytes. Equimolar concentrations of ferrous sulfate and ascorbic acid were used to induce lipid peroxidation. The amount of peroxidized lipids observed in membrane fractions from human liver was smaller than in those from rat liver. In both species, however, pyrimido‐pyrimidine derivatives, except for RA‐233 in rat liver, inhibited lipid peroxidation dose‐dependently in the following sequence: RA‐642 > dipyridamole > d‐α‐tocopherol RA‐233.
ISSN:	0024-4201 1558-9307
DOI:	10.1007/BF02536177