An optimal CD8+ T cell response requires signals from the T cell receptor (TCR), co-stimulatory molecules, and cytokines. In most cases, the relative contribution of these signals to CD8+ T cell proliferation, accumulation, effector function, and differentiation to memory is unknown. Recent work (Boyman, O., M. Kovar, M.P. Rubinstein, C.D. Surh, and J. Sprent. 2006. Science. 311:1924–1927; Kamimura, D., Y. Sawa, M. Sato, E. Agung, T. Hirano, and M. Murakami. 2006. J. Immunol. 177:306–314) has shown that anti–interleukin (IL) 2 monoclonal antibodies that are neutralizing in vitro enhance the potency of IL-2 in vivo. We investigated the role of IL-2 signals in driving CD8+ T cell proliferation in the absence of TCR stimulation by foreign antigen. IL-2 signals induced rapid activation of signal transducer and activator of transcription 5 in all CD8+ T cells, both naive and memory phenotype, and promoted the differentiation of naive CD8+ T cells into effector cells. IL-2–anti–IL-2 complexes induced proliferation of naive CD8+ T cells in an environment with limited access to self–major histocompatibility complex (MHC) and when competition for self-MHC ligands was severe. After transfer into wild-type animals, IL-2–activated CD8+ T cells attained and maintained a central memory phenotype and protected against lethal bacterial infection. IL-2–anti–IL-2 complex–driven memory-like CD8+ T cells had incomplete cellular fitness compared with antigen-driven memory cells regarding homeostatic turnover and cytokine production. These results suggest that intense IL-2 signals, with limited contribution from the TCR, program the differentiation of protective memory-like CD8+ cells but are insufficient to guarantee overall cellular fitness.
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6 August 2007
Article|
July 30 2007
Naive CD8+ T cells differentiate into protective memory-like cells after IL-2–anti–IL-2 complex treatment in vivo
Daisuke Kamimura,
Daisuke Kamimura
Department of Immunology and Howard Hughes Medical Institute, University of Washington, Seattle, WA 98195
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Michael J. Bevan
Michael J. Bevan
Department of Immunology and Howard Hughes Medical Institute, University of Washington, Seattle, WA 98195
Search for other works by this author on:
Daisuke Kamimura
Department of Immunology and Howard Hughes Medical Institute, University of Washington, Seattle, WA 98195
Michael J. Bevan
Department of Immunology and Howard Hughes Medical Institute, University of Washington, Seattle, WA 98195
CORRESPONDENCE Michael J. Bevan: [email protected]
Abbreviations used: C57BL/6, B6; HP, homeostatic pro liferation; LM-OVA, Listeria monocytogenes–expressing soluble OVA.
Received:
March 16 2007
Accepted:
July 05 2007
Online ISSN: 1540-9538
Print ISSN: 0022-1007
The Rockefeller University Press
2007
J Exp Med (2007) 204 (8): 1803–1812.
Article history
Received:
March 16 2007
Accepted:
July 05 2007
Citation
Daisuke Kamimura, Michael J. Bevan; Naive CD8+ T cells differentiate into protective memory-like cells after IL-2–anti–IL-2 complex treatment in vivo . J Exp Med 6 August 2007; 204 (8): 1803–1812. doi: https://doi.org/10.1084/jem.20070543
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