CD9-mediated costimulation of TCR-triggered naive T cells leads to activation followed by apoptosis.


Journal article


X. Tai, K. Toyooka, Y. Yashiro, R. Abe, C. S. Park, T. Hamaoka, M. Kobayashi, S. Neben, H. Fujiwara
Journal of immunology, 1997

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APA   Click to copy
Tai, X., Toyooka, K., Yashiro, Y., Abe, R., Park, C. S., Hamaoka, T., … Fujiwara, H. (1997). CD9-mediated costimulation of TCR-triggered naive T cells leads to activation followed by apoptosis. Journal of Immunology.


Chicago/Turabian   Click to copy
Tai, X., K. Toyooka, Y. Yashiro, R. Abe, C. S. Park, T. Hamaoka, M. Kobayashi, S. Neben, and H. Fujiwara. “CD9-Mediated Costimulation of TCR-Triggered Naive T Cells Leads to Activation Followed by Apoptosis.” Journal of immunology (1997).


MLA   Click to copy
Tai, X., et al. “CD9-Mediated Costimulation of TCR-Triggered Naive T Cells Leads to Activation Followed by Apoptosis.” Journal of Immunology, 1997.


BibTeX   Click to copy

@article{x1997a,
  title = {CD9-mediated costimulation of TCR-triggered naive T cells leads to activation followed by apoptosis.},
  year = {1997},
  journal = {Journal of immunology},
  author = {Tai, X. and Toyooka, K. and Yashiro, Y. and Abe, R. and Park, C. S. and Hamaoka, T. and Kobayashi, M. and Neben, S. and Fujiwara, H.}
}

Abstract

The induction of full activation or death in TCR-triggered T cells depends largely on whether appropriate costimulatory signals are provided. In this study, we show that the costimulation of CD9 on naive T cells during TCR stimulation results in transient, albeit potent, activation followed by apoptosis, rather than full activation. Anti-CD9 mAb synergized with suboptimal doses of anti-CD3 mAb in inducing T cell activation. [3H]TdR incorporation determined 2 days after CD9 costimulation was as potent as that induced by CD28 costimulation. In contrast to progressive T cell proliferation induced by CD28 costimulation, CD9 costimulation led to the induction of apoptosis of once-activated T cells. Although IL-2R expression was induced significantly earlier and to a greater degree after CD9 costimulation than after CD28 costimulation, CD9 costimulation only transiently produced a small amount of IL-2 and induced apparently low levels of bcl-xL compared with those observed in CD28 costimulation. Addition of rIL-2 to cultures of CD9 costimulation induced strikingly enhanced expression of bcl proteins, especially of bcl-xL, and protected TCR-stimulated T cells from apoptosis. These data indicate that CD9-mediated costimulation of TCR-triggered naive T cells leads to activation followed by apoptosis as the result of failure to generate a positive signal for sufficient levels of IL-2 production.



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