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Novel APC-like properties of human NK cells directly regulate T cell activation
Jacob Hanna, … , Jane H. Buckner, Ofer Mandelboim
Jacob Hanna, … , Jane H. Buckner, Ofer Mandelboim
Published December 1, 2004
Citation Information: J Clin Invest. 2004;114(11):1612-1623. https://doi.org/10.1172/JCI22787.
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Article Immunology

Novel APC-like properties of human NK cells directly regulate T cell activation

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Abstract

Initiation of the adaptive immune response is dependent on the priming of naive T cells by APCs. Proteomic analysis of unactivated and activated human NK cell membrane–enriched fractions demonstrated that activated NK cells can efficiently stimulate T cells, since they upregulate MHC class II molecules and multiple ligands for TCR costimulatory molecules. Furthermore, by manipulating antigen administration, we show that NK cells possess multiple independent unique pathways for antigen uptake. These results highlight NK cell–mediated cytotoxicity and specific ligand recognition by cell surface–activating receptors on NK cells as unique mechanisms for antigen capturing and presentation. In addition, we analyzed the T cell–activating potential of human NK cells derived from different clinical conditions, such as inflamed tonsils and noninfected and CMV-infected uterine decidual samples, and from transporter-associated processing antigen 2–deficient patients. This in vivo analysis revealed that proinflammatory, but not immune-suppressive, microenvironmental requirements can selectively dictate upregulation of T cell–activating molecules on NK cells. Taken together, these observations offer new and unexpected insights into the direct interactions between NK and T cells and suggest novel APC-like activating functions for human NK cells.

Authors

Jacob Hanna, Tsufit Gonen-Gross, Jonathan Fitchett, Tony Rowe, Mark Daniels, Tal I. Arnon, Roi Gazit, Aviva Joseph, Karoline W. Schjetne, Alexander Steinle, Angel Porgador, Dror Mevorach, Debra Goldman-Wohl, Simcha Yagel, Michael J. LaBarre, Jane H. Buckner, Ofer Mandelboim

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Figure 2

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Assessment of the functionality of NK cells as costimulators for T cells...
Assessment of the functionality of NK cells as costimulators for T cells. (A) Representative characterization of UaNK and ANK cells used in this study. Cells were stained for CD56 and for CD3, CD14, CD20, NKp46, or NKp30. (B) UaNK and ANK cells were stained for the expression of MHC class II or ligands for TCR costimulatory molecules. (C) RT-PCR of B7-H3 expression on ANK and UaNK cells. (D) Proliferation of CD4+ T cells in the presence of irradiated ANK or UaNK cells with or without suboptimal levels of anti-CD3. Proliferation was determined after 48 hours. Prior to cell harvesting, supernatant from each well was taken for measurement of IL-2 and IFN-γ. (E) Data obtained from 3 independent experiments are presented to show the effect of CTLA-4Ig fusion protein or CD99Ig fusion protein (25 μg/ml). Values are mean ± SD for triplicate samples. **P < 0.01 by Student’s t test. One representative data set is shown out of 3_12 obtained.

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ISSN: 0021-9738 (print), 1558-8238 (online)

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