H. G. Rammensee scite author profile

Minor histocompatibility (H) antigens can be peptides derived from cellular proteins that are presented on the cell surface by major histocompatibility complex (MHC) class I molecules. This is similar to viral antigens, because in both cases cytotoxic T lymphocytes (CTLs) recognize artificially produced peptides loaded on target cells. Naturally processed minor H peptides were found to be similar to those artificial CTL-epitopes, as far as size and hydrophobicity is concerned. The peptides studied were isolated from a transfectant that expressed a model CTL-defined antigen, beta-galactosidase, from male cells that express H-Y, which has been known operationally since 1955, and from cells that express H-4, known since 1961.

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Interaction of the immunodominant MBP peptide 87-106 with multiple sclerosis-associated HLA DR- and -DQ molecules

Vogt¹,

Kropshofer²,

Kalbus³

et al. 1994

Journal of Neuroimmunology

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A prominent natural H-2 Kd ligand is derived from protein tyrosine kinase JAK1

et al. 1993

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Several HLA alleles share overlapping peptide specificities.

et al. 1995

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Herein we describe the establishment of assays to measure peptide binding to purified HLA-B*0701, -B*0801, -B*2705, -B*3501-03, -B*5401, -Cw*0401, -Cw*0602, and -Cw*0702 molecules. The binding of known peptide epitopes or naturally processed peptides correlates well with HLA restriction or origin, underscoring the immunologic relevance of these assays. Analysis of the sequences of various HLA class I alleles suggested that alleles with peptide motifs characterized by proline in position 2 and aromatic or hydrophobic residues at their C-terminus shared key consensus residues at positions 9, 63, 66, 67, and 70 (B pocket) and residue 116 (F pocket). Prediction of the peptide-binding specificity of HLA-B*5401, on the basis of this consensus B and F pocket structure, verified this hypothesis and suggested that a relatively large family of HLA-B alleles (which we have defined as the HLA-B7-like supertype) may significantly overlap in peptide binding specificity. Availability of quantitative binding assays allowed verification that, indeed, many (25%) of the peptide ligands carrying proline in position 2 and hydrophobic/aromatic residues at the C-terminus (the B7-like supermotif) were capable of binding at least three of five HLA-B7-like supertype alleles. Identification of epitopes carrying the B7-like supermotif and binding to a family of alleles represented in over 40% of individuals from all major ethnic groups may be of considerable use in the design of peptide vaccines.

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Minimal structure of lipopeptides for in vivo priming of cytotoxic T-lymphocytes

Wiesmüller¹,

Deres²,

Schild³

et al. 1991

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H. G. Rammensee

Characterization of Naturally Occurring Minor Histocompatibility Peptides Including H-4 and H-Y

Interaction of the immunodominant MBP peptide 87-106 with multiple sclerosis-associated HLA DR- and -DQ molecules

A prominent natural H-2 Kd ligand is derived from protein tyrosine kinase JAK1

Several HLA alleles share overlapping peptide specificities.

Minimal structure of lipopeptides for in vivo priming of cytotoxic T-lymphocytes

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