Prediction of promiscuous peptides that bind HLA class I molecules
- 1 June 2002
- journal article
- research article
- Published by Wiley in Immunology & Cell Biology
- Vol. 80 (3) , 280-285
- https://doi.org/10.1046/j.1440-1711.2002.01088.x
Abstract
Promiscuous T-cell epitopes make ideal targets for vaccine development. We report here a computational system, multipred, for the prediction of peptide binding to the HLA-A2 supertype. It combines a novel representation of peptide/MHC interactions with a hidden Markov model as the prediction algorithm. multipred is both sensitive and specific, and demonstrates high accuracy of peptide-binding predictions for HLA-A∗0201, ∗0204, and ∗0205 alleles, good accuracy for ∗0206 allele, and marginal accuracy for ∗0203 allele. multipred replaces earlier requirements for individual prediction models for each HLA allelic variant and simplifies computational aspects of peptide-binding prediction. Preliminary testing indicates that multipred can predict peptide binding to HLA-A2 supertype molecules with high accuracy, including those allelic variants for which no experimental binding data are currently available.Keywords
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