Degenerate binding of tyrosinase peptides to MHC II Ad/Ed molecules

被引:0
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作者
Mittelman, Abraham
Lucchese, Guglielmo
Stufano, Angela
Kanduc, Darja
机构
[1] New York Med Coll, Dept Med Oncol, Valhalla, NY 10595 USA
[2] New York Med Coll, Dept Microbiol & Immunol, Valhalla, NY 10595 USA
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中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Recently we defined the tyrosinase (233247-)IPYWDWRDAEKCDIC peptide as the pentadecamer sequence hosting the linear determinant of the anti-tyrosinase MAb T311. In order to understand the molecular features that render epitopic the amino acid tyrosinase(233-247) sequence, we 1) analyzed the MHC II affinity of the tyrosinase (233-247)IPYWDWRDAEKCDIC peptide using RankPep as a binding prediction program, and 2) experimentally verified the actual peptide-MHC II interaction by carrying out peptide electrophoretic mobility shift assays. Nine random tyrosinase peptides were used as controls. Under the conditions used in this study, it was found that all of the ten tyrosinase peptides were capable of binding to Ad/Ed molecules in the gel-shift binding assay. Moreover, there was no correlation between the theoretical predicted Ad/Ed affinity and the experimental actual peptide binding. We conclude that Ad/Ed binding potential appears ininfluential in the defining of tyrosinase (233-247) IPYWDWRDAEKCDIC peptide epitopicity.
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页码:231 / 239
页数:9
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