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Published in: BMC Immunology 1/2009

Open Access 01-12-2009 | Research article

Control of CD56 expression and tumor cell cytotoxicity in human Vγ2Vδ2 T cells

Authors: Elizabeth M Urban, Haishan Li, Cheryl Armstrong, Chiara Focaccetti, Cristiana Cairo, C David Pauza

Published in: BMC Immunology | Issue 1/2009

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Abstract

Background

In lymphocyte subsets, expression of CD56 (neural cell adhesion molecule-1) correlates with cytotoxic effector activity. For cells bearing the Vγ2Vδ2 T cell receptor, isoprenoid pyrophosphate stimulation leads to uniform activation and proliferation, but only a fraction of cells express CD56 and display potent cytotoxic activity against tumor cells. Our goal was to show whether CD56 expression was regulated stochastically, similar to conventional activation antigens, or whether CD56 defined a lineage of cells committed to the cytotoxic phenotype.

Results

Tracking individual cell clones defined by their Vγ2 chain CDR3 region sequences, we found that CD56 was expressed on precursor cytotoxic T cells already present in the population irrespective of their capacity to proliferate after antigen stimulation. Public T cell receptor sequences found in the CD56+ subset from one individual might appear in the CD56- subset of another donor. The commitment of individual clones to CD56+ or CD56- lineages was stable for each donor over a 1 year interval.

Conclusion

The ability to express CD56 was not predicted by TCR sequence or by the strength of signal received by the TCR. For γδ T cells, cytotoxic effector function is acquired when cytotoxic precursors within the population are stimulated to proliferate and express CD56. Expression of CD56 defines a committed lineage to the cytotoxic phenotype.
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Metadata
Title
Control of CD56 expression and tumor cell cytotoxicity in human Vγ2Vδ2 T cells
Authors
Elizabeth M Urban
Haishan Li
Cheryl Armstrong
Chiara Focaccetti
Cristiana Cairo
C David Pauza
Publication date
01-12-2009
Publisher
BioMed Central
Published in
BMC Immunology / Issue 1/2009
Electronic ISSN: 1471-2172
DOI
https://doi.org/10.1186/1471-2172-10-50

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