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CD27 promotes survival of activated T cells and complements CD28 in generation and establishment of the effector T cell pool.

Jenny Hendriks ,
Yanling Xiao ,
Jannie Borst

Abstract

CD27, like CD28, acts in concert with the T cell receptor to support T cell expansion. Using CD27(-/-) mice, we have shown earlier that CD27 determines the magnitude of primary and memory T cell responses to influenza virus. Here, we have examined the relative contributions of CD27 and CD28 to generation of the virus-specific effector T cell pool and its establishment at the site of infection (the lung), using CD27(-/-), CD28(-/-), and CD27/CD28(-/-) mice. We find that primary and memory CD8+ T cell responses to influenza virus are dependent on the collective contribution of both receptors. In the primary response, CD27 and CD28 impact to a similar extent on expansion of virus-specific T cells in draining lymph nodes. CD27 is the principle determinant for accumulation of virus-specific T cells in the lung because it can sustain this response in CD28(-/-) mice. Unlike CD28, CD27 does not affect cell cycle activity, but promotes survival of activated T cells throughout successive rounds of division at the site of priming and may do so at the site of infection as well. CD27 was found to rescue CD28(-/-) T cells from death at the onset of division, explaining its capacity to support a T cell response in absence of CD28.

More about this publication

The Journal of experimental medicine

Volume 198
Issue nr. 9
Pages 1369-80
Publication date 03-11-2003

Full text links

Publisher website (DOI) 10.1084/jem.20030916
Europe PubMed Central 14581610
Pubmed 14581610

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