Porcine major histocompatibility complex (MHC) class I molecules and analysis of their peptide-binding specificities

Lasse Eggers Pedersen, Mikkel Harndahl, Michael Rasmussen, Kasper Lamberth, William T. Golde, Ole Lund, Morten Nielsen, Soren Buus

    Research output: Contribution to journalJournal articleResearchpeer-review

    Abstract

    In all vertebrate animals, CD8+ cytotoxic T lymphocytes (CTLs) are controlled by major histocompatibility complex class I (MHC-I) molecules. These are highly polymorphic peptide receptors selecting and presenting endogenously derived epitopes to circulating CTLs. The polymorphism of the MHC effectively individualizes the immune response of each member of the species. We have recently developed efficient methods to generate recombinant human MHC-I (also known as human leukocyte antigen class I, HLA-I) molecules, accompanying peptide-binding assays and predictors, and HLA tetramers for specific CTL staining and manipulation. This has enabled a complete mapping of all HLA-I specificities (“the Human MHC Project”). Here, we demonstrate that these approaches can be applied to other species. We systematically transferred domains of the frequently expressed swine MHC-I molecule, SLA-1*0401, onto a HLA-I molecule (HLA-A*11:01), thereby generating recombinant human/swine chimeric MHC-I molecules as well as the intact SLA-1*0401 molecule. Biochemical peptide-binding assays and positional scanning combinatorial peptide libraries were used to analyze the peptide-binding motifs of these molecules. A pan-specific predictor of peptide–MHC-I binding, NetMHCpan, which was originally developed to cover the binding specificities of all known HLA-I molecules, was successfully used to predict the specificities of the SLA-1*0401 molecule as well as the porcine/human chimeric MHC-I molecules. These data indicate that it is possible to extend the biochemical and bioinformatics tools of the Human MHC Project to other vertebrate species.
    Original languageEnglish
    JournalImmunogenetics
    Volume63
    Issue number12
    Pages (from-to)821-834
    ISSN0093-7711
    DOIs
    Publication statusPublished - 2011

    Keywords

    • Binding predictions
    • Recombinant MHC
    • Peptide specificity

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