Expansion and function of CD8+ T cells expressing Ly49 inhibitory receptors specific for MHC class I molecules.

نویسندگان

  • Nicolas Anfossi
  • Scott H Robbins
  • Sophie Ugolini
  • Philippe Georgel
  • Kasper Hoebe
  • Cécile Bouneaud
  • Catherine Ronet
  • Arthur Kaser
  • Catherine B DiCioccio
  • Elena Tomasello
  • Richard S Blumberg
  • Bruce Beutler
  • Steven L Reiner
  • Lena Alexopoulou
  • Olivier Lantz
  • David H Raulet
  • Laurent Brossay
  • Eric Vivier
چکیده

MHC class I-specific Ly49 inhibitory receptors regulate NK cell activation, thereby preventing autologous damage to normal cells. Ly49 receptors are also expressed on a subset of CD8+ T cells whose origin and function remain unknown. We report here that, despite their phenotypic and cytolytic similarities, Ly49+CD8+ T cells and conventional Ly49-CD44high memory-phenotype CD8+ T cells present strikingly distinct features. First, under steady state conditions Ly49+CD8+ T cells are poor cytokine producers (TNF-alpha and IFN-gamma) upon TCR triggering. Second, Ly49+CD8+ T cells are not induced upon various settings of Ag immunization or microbial challenge. However, Ly49 can be induced on a fraction of self-specific CD8+ T cells if CD4+ T cells are present. Finally, the size of the Ly49+CD8+ T cell subset is selectively reduced in the absence of STAT1. These results indicate that Ly49 expression is associated with a differentiation program of cytolytic CD8+ T cells triggered upon chronic antigenic exposure. They further suggest that the size of the Ly49+CD8+ T cell subset marks a history of CD8+ T cell activation that might preferentially result from endogenous inducers of inflammation rather than from microbial infections.

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عنوان ژورنال:
  • Journal of immunology

دوره 173 6  شماره 

صفحات  -

تاریخ انتشار 2004