Please use this identifier to cite or link to this item: https://doi.org/10.1186/1756-9966-29-134
Title: Ex-vivo expanded human NK cells express activating receptors that mediate cytotoxicity of allogeneic and autologous cancer cell lines by direct recognition and antibody directed cellular cytotoxicity
Authors: Voskens, C.J
Watanabe, R
Rollins, S
Campana, D 
Hasumi, K
Mann, D.L
Keywords: natural killer cell receptor
EGFR protein, human
epidermal growth factor receptor
immunoglobulin receptor
ligand
monoclonal antibody
allogeneic cancer cell
article
autologous cancer cell
cancer cell
cancer cell culture
cell expansion
cytotoxicity
ex vivo study
human
human cell
lymphocyte
natural killer cell
peripheral blood mononuclear cell
priority journal
protein expression
stomach cancer
antibody dependent cellular cytotoxicity
cell proliferation
cell separation
coculture
immunology
immunophenotyping
lymphocyte activation
phenotype
stomach tumor
time
tumor cell line
Antibodies, Monoclonal
Antibody-Dependent Cell Cytotoxicity
Cell Line, Tumor
Cell Proliferation
Cell Separation
Coculture Techniques
Humans
Immunophenotyping
Killer Cells, Natural
Ligands
Lymphocyte Activation
Phenotype
Receptor, Epidermal Growth Factor
Receptors, Immunologic
Stomach Neoplasms
Time Factors
Issue Date: 2010
Publisher: BMC
Citation: Voskens, C.J, Watanabe, R, Rollins, S, Campana, D, Hasumi, K, Mann, D.L (2010). Ex-vivo expanded human NK cells express activating receptors that mediate cytotoxicity of allogeneic and autologous cancer cell lines by direct recognition and antibody directed cellular cytotoxicity. Journal of Experimental and Clinical Cancer Research 29 (1) : 134. ScholarBank@NUS Repository. https://doi.org/10.1186/1756-9966-29-134
Rights: Attribution 4.0 International
Abstract: Background: The possibility that autologous NK cells could serve as an effective treatment modality for solid tumors has long been considered. However, implementation is hampered by (i) the small number of NK cells in peripheral blood, (ii) the difficulties associated with large-scale production of GMP compliant cytolytic NK cells, (iii) the need to activate the NK cells in order to induce NK cell mediated killing and (iv) the constraints imposed by autologous inhibitory receptor-ligand interactions. To address these issues, we determined (i) if large numbers of NK cells could be expanded from PBMC and GMP compliant cell fractions derived by elutriation, (ii) their ability to kill allogeneic and autologous tumor targets by direct cytotoxitiy and by antibody-mediated cellular cytotoxicity and (iii) defined NK cell specific receptor-ligand interactions that mediate tumor target cell killing. Methods: Human NK cells were expanded during 14 days. Expansion efficiency, NK receptor repertoire before and after expansion, expression of NK specific ligands, cytolytic activity against allogeneic and autologous tumor targets, with and without the addition of chimeric EGFR monoclonal antibody, were investigated. Results: Cell expansion shifted the NK cell receptor repertoire towards activation and resulted in cytotoxicity against various allogeneic tumor cell lines and autologous gastric cancer cells, while sparing normal PBMC. Blocking studies confirmed that autologous cytotoxicity is established through multiple activating receptor-ligand interactions. Importantly, expanded NK cells also mediated ADCC in an autologous and allogeneic setting by antibodies that are currently being used to treat patients with select solid tumors. Conclusion: These data demonstrate that large numbers of cytolytic NK cells can be generated from PBMC and lymphocyte-enriched fractions obtained by GMP compliant counter current elutriation from PBMC, establishing the preclinical evidence necessary to support clinical trials utilizing autologous expanded NK cells, both directly and in combination with monoclonal antibodies in future cell-based immunotherapy in select solid tumors. © 2010 Voskens et al; licensee BioMed Central Ltd.
Source Title: Journal of Experimental and Clinical Cancer Research
URI: https://scholarbank.nus.edu.sg/handle/10635/178196
ISSN: 1756-9966
DOI: 10.1186/1756-9966-29-134
Rights: Attribution 4.0 International
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