Journal article
Functional implications of T cell receptor diversity
SJ Turner, NL La Gruta, K Kedzierska, PG Thomas, PC Doherty
Current Opinion in Immunology | CURRENT BIOLOGY LTD | Published : 2009
Abstract
Naive T cells are recruited into any given host response by recognizing a spectrum of possible antigens with 'sufficient' avidity. Does selecting a more functionally diverse array give better immune control? Perhaps low avidity 'killers' that 'kiss and run' operate optimally to eliminate virus-infected targets, while high avidity 'helpers' that stay faithfully in place produce more cytokine. Recent findings indeed suggest that the selection of a broad T cell receptor repertoire is characteristic of the initial phase following antigen contact, while continued exposure leads to further cycles of division and the progressive numerical dominance of 'best-fit' clonotypes. Here, we review recent a..
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Awarded by National Institutes of Health
Funding Acknowledgements
This work was supported by NHMRC program grant; 299907 and by NIH grant AI170251 awarded to PCD; an NHMRC project grant #508929 and Pfizer (Australia) Senior Research Fellowship awarded to SJT; an NHMRC RD Wright Fellowship awarded to NLG and KK.