Molecular location of a species-specific epitope on the hamster scrapie agent protein.

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J Virol. 1991 July; 65(7): 3667-3675

Molecular location of a species-specific epitope on the hamster scrapie agent protein.

D C Bolton, S J Seligman, G Bablanian, D Windsor, L J Scala, K S Kim, C M Chen, R J Kascsak and P E Bendheim

Department of Molecular Biology, New York State Institute for Basic Research in Developmental Disabilities, Staten Island 10314.

ABSTRACT

Scrapie is a transmissible neurodegenerative disease of sheepand goats. An abnormal host protein, Sp33-37, is the major proteincomponent of the scrapie agent and the only known disease- oragent-specific macromolecule. Two monoclonal antibodies (MAbs),4H8 (immunoglobulin G2b [IgG2b]) and 6B11 (IgG1), produced byimmunizing mice with the intact hamster 263K scrapie agent protein,Sp33-37Ha, were found to have species specificity similar tothat reported previously for MAb 3F4 (IgG2a), which was producedby using PrP-27-30 as the immunogen (R. J. Kascsak, R. Rubenstein,P. A. Merz, M. Tonna-DeMasi, R. Fersko, R. I. Carp, H. M. Wisniewski,and H. Diringer, J. Virol. 61:3688-3693, 1987). These antibodiesall bound to Sp33-37 derived from hamster but not from mousecells. Competitive binding assays demonstrated that all threeMAbs bound to the same or overlapping sites on Sp33-37Ha. Themolecular location of the epitope for these antibodies was determinedto within 10 residues by using an antigen competition enzyme-linkedimmunosorbent assay in which synthetic peptides spanning Sp33-37Haresidues 79 to 93 or 84 to 93 specifically inhibited bindingof these antibodies to plates coated with purified Sp33-37Ha.A synthetic peptide with the mouse-specific sequence (83 to92) that differed from the hamster sequence by substitutionat two positions (MetHa-87----LeuMo-86 and MetHa-90----ValMo-89)did not inhibit antibody binding to Sp33-37Ha. MAb 3F4 bindingto hamster Sp33-37 was eliminated by chemical modification ofSp33-37Ha with diethylpyrocarbonate or succinic anhydride andby cleavage with CNBr or trypsin. The effect of diethylpyrocarbonateon MAb 3F4 binding was not reversed by hydroxylamine treatment.MAb 3F4 binding was not affected by prolonged exposure of Sp33-37Hato 70% formic acid or by boiling in sodium dodecyl sulfate.We conclude that the epitope for these MAbs is a linear determinantthat includes Met-87, Lys-88, and Met-90 and that Met-90 isprobably the major species-specific determinant.

J Virol. 1991 July; 65(7): 3667-3675

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