Abstract

NKp30 (NCR3, CD337) is a natural cytotoxicity receptor, expressed on subsets of human peripheral blood NK cells, involved in NK cell killing of tumor cells and immature dendritic cells. The cellular ligand for NKp30 has remained elusive, although evidence that membrane-associated heparan sulfate (HS) proteoglycans are involved in the recognition of cellular targets by NKp30 was recently reported. The data presented in this report show conclusively that HS glycosaminoglycans (GAG) are not ligands for NKp30. We show that removing HS completely from the cell surface of human 293-EBNA cells with mammalian heparanase does not affect binding of rNKp30/human IgG1 Fc chimera complexes or binding of multimeric liposome-rNKp30 complexes. Removing HS from 293-EBNA cells, culture-generated DC, MM-170 malignant melanoma cells, or HeLa cells does not affect the NKp30-dependent killing of these cells by NK cells. We show further that the GAG-deficient hamster pgsA-745 cells that lack HS and the GAG-expressing parent CHO-K1 cells are both killed by NK cells, with killing of both cell lines inhibited to the same extent by anti-NKp30 mAb. From these results we conclude that HS GAG are not ligands for NKp30, leaving open the question as to the nature of the cellular ligand for this important NK cell activation receptor.

Highlights

  • NKp30 (NCR3, CD337) is a natural cytotoxicity receptor, expressed on subsets of human peripheral blood NK cells, involved in NK cell killing of tumor cells and immature dendritic cells

  • We show that heparan sulfate (HS) expressed on 293-EBNA cells and other human cells, and on Chinese hamster ovary (CHO)-K1 cells, is not a ligand for NKp30

  • We showed that HS is not a ligand for NKp30 on culturegenerated dendritic cells (DC), MM-170 malignant melanoma cells, and HeLa cells (Fig. 3)

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Summary

Abbreviations used in this paper

DC, dendritic cell; NCR, natural cytotoxicity receptor; GAG, glycosaminoglycan; HS, heparan sulfate; CHO, Chinese hamster ovary. Binding studies with recombinant NCR fusion proteins [9, 14] have identified cells expressing ligands for these receptors. By these assays, ligands for the NKp46 and/or NKp30 are detected on human, simian, and hamster cells. Evidence that the sulfated glycosaminoglycan (GAG), heparan sulfate (HS), is involved in the recognition of cellular targets by NKp46 and NKp30 was recently reported [15] Such a widely distributed carbohydrate epitope expressed on a variety of protein and/or lipid structures would nicely explain the broad cellular distribution of the ligands for the NCR. These studies do not support the notion that HS is a ligand for NKp30

Materials and Methods
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