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The Journal of Immunology, 2002, 169: 22-30.
Copyright © 2002 by The American Association of Immunologists

Ly-49s3 Is a Promiscuous Activating Rat NK Cell Receptor for Nonclassical MHC Class I-Encoded Target Ligands1

Christian Naper*,{dagger}, Shigenari Hayashi*, Lise Kveberg{dagger}, Eréne C. Niemi*, Lewis L. Lanier{ddagger}, John T. Vaage2,3,{dagger},§ and James C. Ryan2,*

* Veterans Affairs Medical Center, Northern California Institute for Research and Education, and University of California, San Francisco, CA 94121; {dagger} Department of Anatomy, University of Oslo, Oslo, Norway; {ddagger} Department of Microbiology and Immunology and Cancer Research Institute, University of California, San Francisco, CA 94143; and § Institute of Immunology, Rikshospitalet, University Hospital, Oslo, Norway

Previous studies of the rapid rejection of MHC-disparate lymphocytes in rats, named allogeneic lymphocyte cytotoxicity, have indicated that rat NK cells express activating receptors for nonclassical MHC class I allodeterminants from the RT1-C/E/M region. Using an expression cloning system that identifies activating receptors associated with the transmembrane adapter molecule DAP12, we have cloned a novel rat Ly-49 receptor that we have termed Ly-49 stimulatory receptor 3 (Ly-49s3). A newly generated anti-Ly-49s3 Ab, mAb DAR13, identified subpopulations of resting and IL-2-activated NK cells, but not T or B lymphocytes. Depletion of Ly-49s3-expressing NK cells drastically reduced alloreactivity in vitro, indicating that this subpopulation is responsible for a major part of the observed NK alloreactivity. DAR13-mediated blockade of Ly-49s3 inhibited killing of MHC-congenic target cells from the av1, n, lv1, and c haplotypes, but not from the u or b haplotypes. A putative ligand was mapped to the nonclassical MHC class I region (RT1-C/E/M) using intra-MHC recombinant strains. Relative numbers of Ly-49s3+ NK cells were reduced, and surface levels of Ly-49s3 were lower, in MHC congenic strains expressing the putative Ly-49s3 ligand(s). In conclusion, we have identified a novel Ly-49 receptor that triggers rat NK cell-mediated responses.




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