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Peptide selection by MHC class I molecules.

T N Schumacher ,
M L De Bruijn ,
L N Vernie ,
W M Kast ,
C J Melief ,
J J Neefjes ,
H L Ploegh

Abstract

Synthetic peptides have been used to sensitize target cells and thereby screen for epitopes recognized by T cells. Most epitopes of cytotoxic T lymphocytes can be mimicked by synthetic peptides of 12-15 amino acids. Although in specific cases, truncations of peptides improves sensitization of target cells, no optimum length for binding to major histocompatibility complex (MHC) class I molecules has been defined. We have now analysed synthetic peptide captured by empty MHC class I molecules of the mutant cell line RMA-S. We found that class I molecules preferentially bound short peptides (nine amino acids) and selectively bound these peptides even when they were a minor component in a mixture of longer peptides. These results may help to explain the difference in size restriction of T-cell epitopes between experiments with synthetic peptides and those with naturally processed peptides.

More about this publication

Nature

Volume 350
Issue nr. 6320
Pages 703-6
Publication date 25-04-1991

Full text links

Publisher website (DOI) 10.1038/350703a0
Europe PubMed Central 1708852
Pubmed 1708852

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