Journal article

The impact of human leukocyte antigen (HLA) micropolymorphism on ligand specificity within the HLA-B*41 allotypic family

C Bade-Döding, A Theodossis, S Gras, L Kjer-Nielsen, B Eiz-Vesper, A Seltsam, T Huyton, J Rossjohn, J McCluskey, R Blasczyk

Haematologica | Published : 2011

Abstract

Background Polymorphic differences between human leukocyte antigen (HLA) molecules affect the specificity and conformation of their bound peptides and lead to differential selection of the T-cell repertoire. Mismatching during allogeneic transplantation can, therefore, lead to immunological reactions. Design and Methods We investigated the structure-function relationships of six members of the HLA-B*41 allelic group that differ by six polymorphic amino acids, including positions 80, 95, 97 and 114 within the antigen-binding cleft. Peptide-binding motifs for B*41:01, *41:02, *41:03, *41:04, *41:05 and *41:06 were determined by sequencing self-peptides from recombinant B*41 molecules by electr..

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University of Melbourne Researchers

Grants

Awarded by German Jose Carreras Leukemia Foundation (DJCLS)


Awarded by German Federal Ministry of Education and Research


Funding Acknowledgements

this work was supported by the German Jose Carreras Leukemia Foundation (DJCLS R05/27f) and the German Federal Ministry of Education and Research (reference number: 01E00802).