Literature DB >> 8778027

Role of polymorphic residues of human leucocyte antigen-DR molecules on the binding of human immunodeficiency virus peptides.

S Jurcevic1, C Praud, H L Coppin, A Bertrand, S Ricard, M Thomsen, F Lakhdar-Ghazal, C De Preval.   

Abstract

A study was made of the binding properties of 96 human immunodeficiency virus peptides to human leucocyte antigen (HLA)-DR1 and HLA-DR103 molecules, which differ by three amino acids at positions 67, 70 and 71 in the beta chains. The affinity of the peptides was characterized by their inhibitory concentrations in competitive binding assays which displace half of the labelled influenza haemagglutinin peptide HA306-318 (IC50). Among the high-affinity peptides (IC50 < or = 1 microM), seven bound to DR1, three to DR103 and five equally well to both alleles (promiscuous peptides). Thirty-two other peptides showed medium or low affinity for DR molecules. The role of polymorphic residues was analysed using six mutated DR molecules, intermediates between DR1 and DR103 and differing by one or two substitutions at positions 67, 70 or 71. We reached the same conclusions when using DR1-specific or DR103-specific peptides: modification of residue 70 had no effect on peptide affinity, but single substitution at positions 67 or 71 decreased the allele specificity of the peptides while double substitution at 67 and 71 completely reversed the peptide specificity. In functional assays, DR-binding peptides are able to outcompete specific T-cell proliferation. Furthermore, modification at position 67 or 70 significantly affects the T-cell response and mutation at position 71 abolishes completely the T-cell proliferation. Thus, the polymorphic positions 67 and 71 contributed to the peptide binding with direct effects on T-cell receptor (TCR) recognition while position 70 seems to be mostly engaged in TCR interactions. Furthermore, our results suggest that polymorphic residues may select allele-specific peptides and also influence the conformation of promiscuous peptides.

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Year:  1996        PMID: 8778027      PMCID: PMC1384110          DOI: 10.1046/j.1365-2567.1996.458547.x

Source DB:  PubMed          Journal:  Immunology        ISSN: 0019-2805            Impact factor:   7.397


  25 in total

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2.  On the interaction of promiscuous antigenic peptides with different DR alleles. Identification of common structural motifs.

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3.  Conformational and structural characteristics of peptides binding to HLA-DR molecules.

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4.  The specificity of alloreactive T cells is determined by MHC polymorphisms which contact the T cell receptor and which influence peptide binding.

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Journal:  J Immunol       Date:  1990-03-01       Impact factor: 5.422

6.  Characterization of the specificity of peptide binding to four DR haplotypes.

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7.  Isolation and characterization of antigen-Ia complexes involved in T cell recognition.

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9.  Peptide binding to HLA-DR1: a peptide with most residues substituted to alanine retains MHC binding.

Authors:  T S Jardetzky; J C Gorga; R Busch; J Rothbard; J L Strominger; D C Wiley
Journal:  EMBO J       Date:  1990-06       Impact factor: 11.598

10.  Regulation of antigen presentation by acidic pH.

Authors:  P E Jensen
Journal:  J Exp Med       Date:  1990-05-01       Impact factor: 14.307

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