Abstract

Increasing evidence indicates that low density lipoprotein (LDL) has to be modified to induce foam cell formation. One such modification, oxidation of LDL, generates a number of highly reactive short chain-length aldehydic fragments of oxidized fatty acids capable of conjugating with lysine residues of apoprotein B. By immunizing animals with homologous malondialdehyde-modified LDL (MDA-LDL), 4-hydroxynonenal-LDL (4-HNE-LDL), and Cu+(+)-oxidized LDL, we developed polyvalent and monoclonal antibodies against three epitopes found in oxidatively modified LDL. The present article characterizes an antiserum and monoclonal antibody (MAL-2 and MDA2, respectively) specific for MDA-lysine, and an antiserum and monoclonal antibody (HNE-6 and NA59, respectively) specific for 4-HNE-lysine. In addition, a monoclonal antibody (OLF4-3C10) was developed against an as yet undefined epitope generated during Cu++ oxidation of LDL. With these antibodies, we demonstrated that MDA-lysine and 4-HNE-lysine adducts develop on apo-lipoprotein B during copper-induced oxidation of LDL in vitro. The application of these antibodies for immunocytochemical demonstration of oxidized lipoproteins in atherosclerotic lesions of progressive severity is described in the companion article. These antibodies should prove useful in studying the role of oxidatively modified lipoproteins as well as other oxidatively modified proteins in atherogenesis.

Keywords

Monoclonal antibodyAntiserumEpitopeLysineChemistryAntibodyLow-density lipoproteinBiochemistryLipoproteinMolecular biologyOxidative phosphorylationMonoclonalPolyclonal antibodiesAmino acidBiologyCholesterolImmunology

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Publication Info

Year
1990
Type
article
Volume
10
Issue
3
Pages
325-335
Citations
614
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Wulf Palinski, Seppo Ylä‐Herttuala, Michael E. Rosenfeld et al. (1990). Antisera and monoclonal antibodies specific for epitopes generated during oxidative modification of low density lipoprotein.. Arteriosclerosis An Official Journal of the American Heart Association Inc , 10 (3) , 325-335. https://doi.org/10.1161/01.atv.10.3.325

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DOI
10.1161/01.atv.10.3.325