Cross-linking a mAb to NKR-P2/NKG2D on dendritic cells induces their activation and maturation leading to enhanced anti-tumor immune response

doi:10.1093/intimm/dxm024

International Immunology Advance Access originally published online on March 15, 2007
International Immunology 2007 19(5):591-607; doi:10.1093/intimm/dxm024

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Cross-linking a mAb to NKR-P2/NKG2D on dendritic cells induces their activation and maturation leading to enhanced anti-tumor immune response

Raghvendra M. Srivastava, Ch. Varalakshmi and Ashok Khar

Centre for Cellular and Molecular Biology, Uppal Road, Hyderabad 500007, India

Corresponding to: A. Khar; E-mail: khar{at}ccmb.res.in

NKR-P2/NKG2D is the chief tumor recognition receptor of NK cellsand some T cells, which recognizes stress inducible ligandson tumors and mediates cell activation. We have recently reportedthe involvement of NKR-P2 in rat dendritic cell (DC) activation.We demonstrate the potential of agonistic anti-NKR-P2 mAb (1A6),which mimics the NKR-P2 ligand and induces activation and maturationof DCs. Interaction of DCs with 1A6 enhances nitric oxide-mediatedapoptosis in tumor cells. Cross-linking of NKR-P2 with mAb1A6up-regulates MHC II, CD86, CD1a, antigen-presentation functionand decreases endocytic activity of DC, thus drives DCs to playa pivotal role in adaptive immune responses. NKR-P2 cross-linkingwith 1A6 also induced the secretion of inflammatory cytokines,IL-1ß, tumor necrosis factor- ${alpha}$ , IFN- ${gamma}$ and IL-12 by DCs.Blocking of 1A6-mediated activation and maturation with inhibitorsof PI3K, p38K and ERK1/2K suggests involvement of MAP kinasein signal transduction. 1A6 cross-linking activates nuclearfactor kappa B, which acts as key executioner of DC activation.Administration of 1A6 antibody induces rapid regression andprotective immune responses against transplantable tumors, suggestingmAb induced activation and maturation of DCs, leading to enhancedanti-tumor immune response.

Keywords: apoptosis, dendritic cells, maturation, NKR-P2/NKG2D, nitric oxide

Transmitting editor: W. Yokoyama

Received 8 August 2006, accepted 7 February 2007.

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