Structure/Function Relationship of Activating Ly-49D and Inhibitory Ly-49G2 NK Receptors

Author:

Ortaldo John R.1,Winkler-Pickett Robin1,Willette-Brown Jami1,Wange Ronald L.2,Anderson Stephen K.3,Palumbo Gregory J.4,Mason Llewellyn H.1,McVicar Daniel W.1

Affiliation:

1. *Laboratory of Experimental Immunology, Division of Basic Sciences, and

2. §Laboratory of Biological Chemistry, National Institute of Aging, National Institutes of Health, Baltimore, MD 21224.

3. †Intramural Research Support Program, Science Applications International Corporation-Frederick, National Cancer Institute-Frederick Cancer Research and Development Center, Frederick, MD 21702;

4. ‡University of Oklahoma, Health Sciences Center, Oklahoma City, OK 73104; and

Abstract

AbstractMurine NK cells express Ly-49 family receptors capable of either inhibiting or activating lytic function. The overlapping patterns of expression of the various receptors have complicated their precise biochemical characterization. Here we describe the use of the Jurkat T cell line as the model for the study of Ly-49s. We demonstrate that Ly-49D is capable of delivering activation signals to Jurkat T cells even in the absence of the recently described Ly-49D-associated chain, DAP-12. Ly-49D signaling in Jurkat leads to tyrosine phosphorylation of TCRζ and requires Syk/Zap70 family kinases and arginine 54 of Ly-49D, suggesting that Ly-49D signals via association with TCRζ. Coexpression studies in 293-T cells confirmed the ability of Ly-49D to associate with TCRζ. In addition, we have used this model to study the functional interactions between an inhibitory Ly-49 (Ly-49G2) and an activating Ly-49 (Ly-49D). Ly-49G2 blocks activation mediated by Ly-49D in an immunoreceptor tyrosine-based inhibitory motif (ITIM)-dependent manner. In contrast, Ly-49G2 was incapable of inhibiting activation by the TCR even though human killer cell inhibitory receptor (KIR) (KIR3DL2(GL183)) effectively inhibits TCR. Both the ability of Ly-49G2 to block Ly-49D activation and the failure of Ly-49G2 to inhibit TCR signaling were confirmed in primary murine NK cells and NK/T cells, respectively. These data demonstrate the dominant effects of the inhibitory receptors over those that activate and suggest an inability of the Ly-49 type II inhibitory receptors to efficiently inhibit type I transmembrane receptor signaling in T cells and NK cells.

Publisher

The American Association of Immunologists

Subject

Immunology,Immunology and Allergy

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