Cutting Edge: Lectin-Like Transcript-1 Is a Ligand for the Inhibitory Human NKR-P1A Receptor

David B. Rosen; Jayaram Bettadapura; Mohammed Alsharifi; Porunelloor A. Mathew; Hilary S. Warren; Lewis L. Lanier

doi:10.4049/jimmunol.175.12.7796

Cutting Edge: Lectin-Like Transcript-1 Is a Ligand for the Inhibitory Human NKR-P1A Receptor

David B. Rosen(Cancer Research Institute), Jayaram Bettadapura(Australian National University), Mohammed Alsharifi(Australian National University), Porunelloor A. Mathew(University of North Texas), Hilary S. Warren(Australian National University), Lewis L. Lanier(Cancer Research Institute)

The Journal of Immunology

December 1, 2005

10.4049/jimmunol.175.12.7796

Cited by 281Open Access

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Abstract

Increasingly, roles are emerging for C-type lectin receptors in immune regulation. One receptor whose function has remained largely enigmatic is human NKR-P1A (CD161), present on NK cells and subsets of T cells. In this study, we demonstrate that the lectin-like transcript-1 (LLT1) is a physiologic ligand for NKR-P1A. LLT1-containing liposomes bind to NKR-P1A+ cells, and binding is inhibited by anti-NKR-P1A mAb. Additionally, LLT1 activates NFAT-GFP reporter cells expressing a CD3zeta-NKR-P1A chimeric receptor; reciprocally, reporter cells with a CD3zeta-LLT1 chimeric receptor are stimulated by NKR-P1A. Moreover, LLT1 on target cells can inhibit NK cytotoxicity via interactions with NKR-P1A.

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