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Characterization of CD28CD4 T cells in living kidney transplant patients with long-term allograft acceptance |
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| Authors: | Masashi Kato Tetsuya Matsuguchi Yoshinari Ono Ryohei Hattori Shinichi Ohshima Yasunobu Yoshikai |
| Affiliation: | a Department of Urology (M.K., Y.O., R.H., S.O.), Nagoya University School of Medicine, Nagoya, Japan b Laboratory of Host Defense and Germfree Life, Institute for Disease Mechanism and Control (T.M., Y.Y.), Nagoya University School of Medicine, Nagoya, Japan |
| Abstract: | CD28−CD4+ T-cell subpopulation is expanded in kidney allograft patients with long graft survival. To seek for the roles of CD28−CD4+ T cells in the long-term acceptance of kidney allografts, we characterized this population by analyzing cell surface molecules, TCR Vβ repertoire, mixed lymphocyte reaction (MLR), and cytokine production. The number of CD28−CD4+ T cells increased correlatively with time after transplantation in this group of patients. The CD28−CD4+ T cells did not express detectable levels of CD25, CD69, V24, or CTLA-4 but expressed heterogeneous amounts of CD45 RA on the surface. Freshly sorted CD28−CD4+ T cells revealed a restricted Vβ repertoire, whereas the Vβ usage of CD28+CD4+ T cells from the same patients was much diversified. Expression levels of TGF-β and IFNγ gene were significantly higher in the CD28− CD4+ T cells than in the CD28+CD4+ T cells from the kidney allograft patients. These findings suggest that an oligoclonal CD28− CD4+ T-cell population is continuously activated in patients with long allograft survival, which may be linked with the long-term acceptance. |
| Keywords: | human T lymphocytes transplantation cell surface molecules |
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