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- W3021575480 abstract "Abstract Background CD8 + CD28 − T suppressor (Ts) cells play critical role in transplant tolerance. Our previous study has generated CD8 + CD28 − Ts cells in vitro which exert robust allospecific suppressive capacity in vitro. Results CD8 + CD28 − Ts cells were expanded by stimulating human CD8 + T cells with allogeneic antigen presenting cells in the presence of the common gamma chain cytokines IL-2, IL-7 and IL-15 in vitro, and were further verified in vitro through day 7 to 11 for their persistency of the allospecific suppressive capacity. When CD8 + CD28 − Ts cells were adoptively transferred into NOG mice, their capacity to inhibit CD4 + T cell proliferation in allospecific manner remained potent on 11 days after their injection. The mechanisms for expansion of CD8 + CD28 − Ts cells by the common gamma chain cytokines were investigated. These included promoting CD8 + CD28 − T cells proliferation, converting CD8 + CD28 + T cells to CD8 + CD28 − T cells and decreasing CD8 + CD28 − T cell death. Furthermore, the expanded CD8 + CD28 − Ts cells showed upregulation of the co-inhibitory molecule Tim-3 and down-regulation of the cytotoxic molecule granzyme B. Conclusions In summary, these results demonstrated that the in vitro-expanded human CD8 + CD28 − T cells retained potent allospecific suppressive capacity in vivo and depicted multiple mechanisms for the expansion of Ts cells, which might promote further bench to clinic research." @default.
- W3021575480 created "2020-05-13" @default.
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- W3021575480 date "2020-04-29" @default.
- W3021575480 modified "2023-10-14" @default.
- W3021575480 title "Human CD8+CD28− T suppressor cells expanded by common gamma chain (γc) cytokines retain steady allospecific suppressive capacity in vivo" @default.
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- W3021575480 doi "https://doi.org/10.1186/s12865-020-00354-z" @default.
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