Acrylate and methacrylate esters: Relationship of hemolytic activity and in vivo toxicity
Author(s) -
Dillingham E. O.,
Lawrence W. H.,
Autian J.,
Schmalz G.
Publication year - 1983
Publication title -
journal of biomedical materials research
Language(s) - English
Resource type - Journals
eISSN - 1097-4636
pISSN - 0021-9304
DOI - 10.1002/jbm.820170606
Subject(s) - lipophilicity , hemolysis , steric effects , chemistry , in vivo , toxicity , substituent , methyl methacrylate , acrylate , acute toxicity , stereochemistry , ether , medicinal chemistry , organic chemistry , biology , polymerization , polymer , microbiology and biotechnology , monomer , immunology
Quantitative hemolysis assays of acrylate and methacrylate esters provided estimates of the intrinsic hemolytic activity ( H i the slope of the concentration‐response curve) and the concentrations effecting 5% ( H 5 ) and 50% ( H 50 ) hemolysis. The dependence of hemolytic activity and LD 50 (mice) on physical properties (lipophilicity, molar refraction, and molecular volume) of the esters was determined by multiple regression analysis. The observed correlations were: H i , R 2 = 0.94; H 5 , R 2 = 0.95; H 50 , R 2 = 0.94; and LD 50 , R 2 (all compounds) = 0.80, R 2 (all compounds less the methyl esters) = 0.94. The difference of the methyl esters was associated with the smaller steric volume of the methyl ester substituent and the presence (methacrylates) or absence (acrylates) of the branched methyl group. Associative steric contributions of the branched methyl group and the ester substituents were probably responsible for greater variability in the methyacrylate series. The results were consistent with the conclusion that the mechanism of the action of the esters is membrane mediated and relatively nonspecific and that in vivo biotransformation was not a significant factor. Also, long‐term toxic liability of the esters may be more closely related to intrinsic toxicity than acute toxicity.
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