周边公差
抗原
过继性细胞移植
免疫耐受
免疫学
传出的
生物
抗原提呈细胞
免疫系统
CD8型
T细胞
迟发型超敏反应
人口
细胞毒性T细胞
巨噬细胞
体外
医学
神经科学
生物化学
传入的
环境卫生
作者
Hsi‐Hsien Lin,Douglas E. Faunce,Martin Stacey,Ania Terajewicz,Takahiko Nakamura,Jie Zhang-Hoover,Marilyn Kerley,Michael L. Mucenski,Siamon Gordon,Joan Stein‐Streilein
摘要
We show that the mouse macrophage-restricted F4/80 protein is not required for the development and distribution of tissue macrophages but is involved in the generation of antigen-specific efferent regulatory T (T reg) cells that suppress antigen-specific immunity. In the in vivo anterior chamber (a.c.)–associated immune deviation (ACAID) model of peripheral tolerance, a.c. inoculation of antigen into F4/80−/− mice was unable to induce efferent T reg cells and suppress delayed-type hypersensitivity (DTH) responses. Moreover, the use of anti-F4/80 mAb and F4/80−/− APCs in an in vitro ACAID model showed that all APC cells in the culture must be able to express F4/80 protein if efferent T reg cells were to be generated. In a low-dose oral tolerance model, WT but not F4/80−/− mice generated an efferent CD8+ T reg cell population that suppressed an antigen-specific DTH response. Peripheral tolerance was restored in F4/80−/− mice by adoptive transfer of F4/80+ APCs in both peripheral tolerance models, indicating a central role for the F4/80 molecule in the generation of efferent CD8+ T reg cells.
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