Journal
JOURNAL OF EXPERIMENTAL MEDICINE
Volume 205, Issue 8, Pages 1829-1841Publisher
ROCKEFELLER UNIV PRESS
DOI: 10.1084/jem.20072446
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Funding
- Howard Hughes Medical Institute
- Barnes Jewish Hospital Foundation
- National Institutes of Health [K08 A1071016-01]
- Washington University Pilot and Feasibility program [DDRCC 5P30 DK052574]
- Max Kade Foundation
- Department of Pathology and Immunology
- Rheumatic Diseases Core Center [P30-AR48335]
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Natural killer (NK) cell tolerance mechanisms are incompletely understood. One possibility is that they possess self-specific activation receptors that result in hyporesponsiveness unless modulated by self-major histocompatability complex (MHC)-specific inhibitory receptors. As putative self-specific activation receptors have not been well characterized, we studied a transgenic C57BL/6 mouse that ubiquitously expresses m157 (m157-Tg), which is the murine cytomegalovirus (MCMV)-encoded ligand for the Ly49H NK cell activation receptor. The transgenic mice were more susceptible to MCMV infection and were unable to reject m157-Tg bone marrow, suggesting defects in Ly49H(+) NK cells. There was a reversible hyporesponsiveness of Ly49H(+) NK cells that extended to Ly49H-independent stimuli. Continuous Ly49H-m157 interaction was necessary for the functional defects. Interestingly, functional defects occurred when mature wild-type NK cells were adoptively transferred to m157-Tg mice, suggesting that mature NK cells may acquire hyporesponsiveness. Importantly, NK cell tolerance caused by Ly49H-m157 interaction was similar in NK cells regardless of expression of Ly49C, an inhibitory receptor specific for a self-MHC allele in C57BL/6 mice. Thus, engagement of self-specific activation receptors in vivo induces an NK cell tolerance effect that is not affected by self-MHC-specific inhibitory receptors.
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