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The Journal of Immunology, 2004, 173: 1819-1825.
Copyright © 2004 by The American Association of Immunologists

MHC Class I-Independent Recognition of NK-Activating Receptor KIR2DS41

Gil Katz*, Roi Gazit*, Tal I. Arnon*, Tsufit Gonen-Gross*, Gabi Tarcic*, Gal Markel*, Raizy Gruda*, Hagit Achdout*, Olga Drize{dagger}, Sharon Merims{dagger} and Ofer Mandelboim2,*

* Lautenberg Center for General and Tumor Immunology, Hadassah Medical School, Hebrew University, Jerusalem, Israel; and {dagger} Sharett Institute of Oncology, Hadassah Medical Center, Jerusalem, Israel

Natural killer cells are capable of killing tumor and virus-infected cells. This killing is mediated primarily via the natural cytotoxicity receptors, including NKp46, NKp44, NKp30, and by the NKG2D receptor. Killer cell Ig-like receptors (KIRs) are mainly involved in inhibiting NK killing (inhibitory KIRs) via interaction with MHC class I molecules. Some KIRs, however, have been found to enhance NK killing when interacting with MHC class I molecules (activating KIRs). We have previously demonstrated that KIR2DS4, an activating KIR, recognizes the HLA-Cw4 protein. The interaction observed was weak and highly restricted to HLA-Cw4 only. These findings prompted us to check whether KIR2DS4 might have additional ligand(s). In this study, we show that KIR2DS4 is able to also interact with a non-class I MHC protein expressed on melanoma cell lines and on a primary melanoma. This interaction is shown to be both specific and functional. Importantly, site-directed mutagenesis analysis reveals that the amino acid residues involved in the recognition of this novel ligand are different from those interacting with HLA-Cw4. These results may shed new light on the function of activating KIRs and their relevance in NK biology.




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