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CD27 is required for generation and long-term maintenance of T cell immunity.

J Hendriks ,
L A Gravestein ,
K Tesselaar ,
R A van Lier ,
T N Schumacher ,
J Borst

Abstract

The Traf-linked tumor necrosis factor receptor family member CD27 is known as a T cell costimulatory molecule. We generated CD27-/- mice and found that CD27 makes essential contributions to mature CD4+ and CD8+ T cell function: CD27 supported antigen-specific expansion (but not effector cell maturation) of naïve T cells, independent of the cell cycle-promoting activities of CD28 and interleukin 2. Primary CD4+ and CD8+ T cell responses to influenza virus were impaired in CD27-/- mice. Effects of deleting the gene encoding CD27 were most profound on T cell memory, reflected by delayed response kinetics and reduction of CD8+ virus-specific T cell numbers to the level seen in the primary response. This demonstrates the requirement for a costimulatory receptor in the generation of T cell memory.

More about this publication

Nature immunology

Volume 1
Issue nr. 5
Pages 433-40
Publication date 01-11-2000

Full text links

Publisher website (DOI) 10.1038/80877
Europe PubMed Central 11062504
Pubmed 11062504

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