| Literature DB >> 10894168 |
S I Khakoo1, R Rajalingam, B P Shum, K Weidenbach, L Flodin, D G Muir, F Canavez, S L Cooper, N M Valiante, L L Lanier, P Parham.
Abstract
That NK cell receptors engage fast-evolving MHC class I ligands suggests that they, too, evolve rapidly. To test this hypothesis, the structure and class I specificity of chimpanzee KIR and CD94:NKG2 receptors were determined and compared to their human counterparts. The KIR families are divergent, with only three KIR conserved between chimpanzees and humans. By contrast, CD94:NKG2 receptors are conserved. Whereas receptors for polymorphic class I are divergent, those for nonpolymorphic class I are conserved. Although chimpanzee and human NK cells exhibit identical receptor specificities for MHC-C, they are mediated by nonorthologous KIR. These results demonstrate the rapid evolution of NK cell receptor systems and imply that "catching up" with class I is not the only force driving this evolution.Entities:
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Year: 2000 PMID: 10894168 DOI: 10.1016/s1074-7613(00)80219-8
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745