Intact NKG2D-Independent Function of NK Cells Chronically Stimulated with the NKG2D Ligand Rae-1

Marine Champsaur; Joshua N. Beilke; Kouetsu Ogasawara; Ulrich H. Koszinowski; Stipan Jonjic; Lewis L. Lanier

Journal ArticleOPEN ACCESS

Intact NKG2D-Independent Function of NK Cells Chronically Stimulated with the NKG2D Ligand Rae-1

Champsaur M
Beilke J
Ogasawara K
et al.

The Journal of Immunology (2010) 185(1) 157-165

DOI: 10.4049/jimmunol.1000397

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Abstract

Human tumors frequently express membrane-bound or soluble NK group 2, member D (NKG2D) ligands. This results in chronic engagement of NKG2D on the surfaces of NK and CD8+ T cells and rapid internalization of the receptor. Although it is well appreciated that this phenomenon impairs NKG2D-dependent function, careful analysis of NKG2D-independent functions in cells chronically stimulated through NKG2D is lacking. Using a mouse model of chronic NKG2D ligand expression, we show that constant exposure to NKG2D ligands does not functionally impair NK cells and CD8+ T cells in the context of viral infection.

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Champsaur, M., Beilke, J. N., Ogasawara, K., Koszinowski, U. H., Jonjic, S., & Lanier, L. L. (2010). Intact NKG2D-Independent Function of NK Cells Chronically Stimulated with the NKG2D Ligand Rae-1. The Journal of Immunology, 185(1), 157–165. https://doi.org/10.4049/jimmunol.1000397

Intact NKG2D-Independent Function of NK Cells Chronically Stimulated with the NKG2D Ligand Rae-1

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