Molecular Cloning of NKp46: A Novel Member of the Immunoglobulin Superfamily Involved in Triggering of Natural Cytotoxicity

Pessino, A.; Sivori, Simona; Bottino, Cristina; Malaspina, Angela; Morelli, Luigia; Moretta, Lorenzo; Biassoni, Roberto; Moretta, Alessandro

doi:10.1084/jem.188.5.953

Cited by 498 publications

(448 citation statements)

References 35 publications

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“…Down-regulation of NKp46 occurs in a manner that closely parallels that of mitochondrial membrane depolarization, several hours before cell death. Because NKp46 is downregulated very early, this seems to be an active process that would presumably quickly limit CD56 dim NK cells' ability to lyse NKp46 ligand-expressing targets, such as tumor cells (34,35). H 2 O 2 exposure has been shown to inhibit NK cytotoxic ability against K562 cells (31,33,36), and signaling through NKp46 is very important for lysis of K562 cells by freshly isolated NK cells (35).…”

Section: Discussionmentioning

confidence: 99%

The CD16−CD56bright NK Cell Subset Is Resistant to Reactive Oxygen Species Produced by Activated Granulocytes and Has Higher Antioxidative Capacity Than the CD16+CD56dim Subset

Harlin

Hanson

Johansson

et al. 2007

The Journal of Immunology

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Human NK cells can be divided into CD56dim and CD56bright subsets. These two types of NK cells respond to different types of stimuli, with CD56dim NK cells having direct cytotoxic ability and CD56bright NK cells having mainly an immunoregulatory function. We show that the CD16+CD56dim NK subset is characterized by sensitivity to cell death induced by activated granulocytes. We identified hydrogen peroxide (H2O2) as the major effector molecule responsible for the cytotoxic effect of granulocytes on CD56dim NK cells, because the ability of granulocytes to kill CD56dim NK cells was completely abrogated in the presence of the hydrogen peroxide scavenger catalase. When exposing NK cells to H2O2, CD56dim cells showed rapid mitochondrial depolarization and down-regulation of activating NKRs, eventually resulting in cell death, whereas CD56bright cells remained unaffected. The difference in sensitivity to H2O2 was mirrored by a difference in intracellular oxidation levels between CD56dim and CD56bright NK cells, and cell lysates from the latter subset possessed a greater ability to block H2O2-mediated oxidation. Our data may explain the preferential accumulation of CD56bright NK cells often seen in environments rich in reactive oxygen species, such as at sites of chronic inflammation and in tumors.

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Section: Discussionmentioning

confidence: 99%

The CD16−CD56bright NK Cell Subset Is Resistant to Reactive Oxygen Species Produced by Activated Granulocytes and Has Higher Antioxidative Capacity Than the CD16+CD56dim Subset

Harlin

Hanson

Johansson

et al. 2007

The Journal of Immunology

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“…Anti-NKp30 (F252, IgM) and anti-NKp46 (KL247, IgM,), which were from hybridoma supernatants were used at 1/2 dilutions. All Ab concentrations for blocking studies were chosen based on published information (34,36,38). F(abЈ) 2 of the NKG2D mAb (clone 1D11) were prepared using immobilized ficin (Pierce) according to the manufacturer's instructions.…”

Section: Experimental Protocols and Abs For Blocking Nk Cell Activatimentioning

confidence: 99%

NKp46 and NKG2D Recognition of Infected Dendritic Cells Is Necessary for NK Cell Activation in the Human Response to Influenza Infection

Draghi

Pashine

Sanjanwala

et al. 2007

The Journal of Immunology

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179

169

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At an early phase of viral infection, contact and cooperation between dendritic cells (DCs) and NK cells activates innate immunity, and also influences recruitment, when needed, of adaptive immunity. Influenza, an adaptable fast-evolving virus, annually causes acute, widespread infections that challenge the innate and adaptive immunity of humanity. In this study, we dissect and define the molecular mechanisms by which influenza-infected, human DCs activate resting, autologous NK cells. Three events in NK cell activation showed different requirements for soluble mediators made by infected DCs and for signals arising from contact with infected DCs. IFN-α was mainly responsible for enhanced NK cytolysis and also important for CD69 up-regulation, whereas IL-12 was necessary for enhancing IFN-γ production. Increased CD69 expression and IFN-γ production, but not increased cytolysis, required recognition of influenza-infected DCs by two NK cell receptors: NKG2D and NKp46. Abs specific for these receptors or their known ligands (UL16-binding proteins 1–3 class I-like molecules for NKG2D and influenza hemagglutinin for NKp46) inhibited CD69 expression and IFN-γ production. Activation of NK cells by influenza-infected DCs and polyinosinic:polycytidylic acid (poly(I:C))-treated DCs was distinguished. Poly(I:C)-treated DCs did not express the UL16-binding protein 3 ligand for NKG2D, and in the absence of the influenza hemagglutinin there was no involvement of NKp46.

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“…However, human NK cell clones established from fetal liver, which do not rearrange TCRb, TCRc, or TCRd genes, expressed CD3d, CD3c, and CD3e proteins in their cytoplasm, but not on their cell surface, and CD3e is transcribed by IL-2 activated human peripheral blood NK cells [7]. Both mouse and human NK cells express CD3f, which associates with NKp46 [8], and in humans with CD16 (FccRIII) [9] and NKp30 [10]. Collectively, these prior studies have established that NK cells that do not rearrange their TCR genes can express germline TCR transcripts and can express CD3 subunit proteins.…”

Section: Tcr Rearrangement and Expressionmentioning

confidence: 99%

Back to the future –defining NK cells and T cells

Lanier

2007

Eur J Immunol

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In this issue of the European Journal of Immunology (EJI), Stewart et al. report about a population of cd-T cells expressing an extensive repertoire of NK cell receptors, and the presence of non-rearranged germline TCRd transcripts in conventional NK cells. These findings and other recent studies highlight the similarities of NK cells and T cells and the problems in discriminating between these two lineages.

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Molecular Cloning of NKp46: A Novel Member of the Immunoglobulin Superfamily Involved in Triggering of Natural Cytotoxicity

Cited by 498 publications

References 35 publications

The CD16−CD56bright NK Cell Subset Is Resistant to Reactive Oxygen Species Produced by Activated Granulocytes and Has Higher Antioxidative Capacity Than the CD16+CD56dim Subset

The CD16−CD56bright NK Cell Subset Is Resistant to Reactive Oxygen Species Produced by Activated Granulocytes and Has Higher Antioxidative Capacity Than the CD16+CD56dim Subset

NKp46 and NKG2D Recognition of Infected Dendritic Cells Is Necessary for NK Cell Activation in the Human Response to Influenza Infection

Back to the future –defining NK cells and T cells

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