A Small, Variable, and Irregular Killer Cell Ig-Like Receptor Locus Accompanies the Absence of MHC-C and MHC-G in Gibbons

The killer cell Ig-like receptors (KIRs) of NK cells recognize MHC class I ligands and function in placental reproduction and immune defense against pathogens. During the evolution of monkeys, great apes, and humans, an ancestral KIR3DL gene expanded to become a diverse and rapidly evolving gene fam...

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Bibliographic Details
Published in:The Journal of immunology (1950) 2010-02, Vol.184 (3), p.1379-1391
Main Authors: Abi-Rached, Laurent, Kuhl, Heiner, Roos, Christian, ten Hallers, Boudewijn, Zhu, Baoli, Carbone, Lucia, de Jong, Pieter J, Mootnick, Alan R, Knaust, Florian, Reinhardt, Richard, Parham, Peter, Walter, Lutz
Format: Article
Language:English
Subjects:
Amino Acid Sequence
Animals
Antigenic Variation - genetics
Antigenic Variation - immunology
Base Sequence
Chromosomes, Artificial, Bacterial - immunology
Evolution, Molecular
Gene Deletion
Genetic Loci - immunology
Haplotypes - immunology
Histocompatibility Antigens Class I - genetics
Humans
Hylobates - genetics
Hylobates - immunology
Immunoglobulin Variable Region - genetics
Macaca mulatta
Molecular Sequence Data
Pan troglodytes
Pongo
Receptors, KIR - genetics
Receptors, KIR - metabolism
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Summary:The killer cell Ig-like receptors (KIRs) of NK cells recognize MHC class I ligands and function in placental reproduction and immune defense against pathogens. During the evolution of monkeys, great apes, and humans, an ancestral KIR3DL gene expanded to become a diverse and rapidly evolving gene family of four KIR lineages. Characterizing the KIR locus are three framework regions, defining two intervals of variable gene content. By analysis of four KIR haplotypes from two species of gibbon, we find that the smaller apes do not conform to these rules. Although diverse and irregular in structure, the gibbon haplotypes are unusually small, containing only two to five functional genes. Comparison with the predicted ancestral hominoid KIR haplotype indicates that modern gibbon KIR haplotypes were formed by a series of deletion events, which created new hybrid genes as well as eliminating ancestral genes. Of the three framework regions, only KIR3DL3 (lineage V), defining the 5' end of the KIR locus, is present and intact on all gibbon KIR haplotypes. KIR2DL4 (lineage I) defining the central framework region has been a major target for elimination or inactivation, correlating with the absence of its putative ligand, MHC-G, in gibbons. Similarly, the MHC-C-driven expansion of lineage III KIR genes in great apes has not occurred in gibbons because they lack MHC-C. Our results indicate that the selective forces shaping the size and organization of the gibbon KIR locus differed from those acting upon the KIR of other hominoid species.
ISSN:0022-1767
1550-6606
DOI:10.4049/jimmunol.0903016