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CD28 controls the development of innate-like CD8+ T cells by promoting the functional maturation of NKT cells

机译:innate-like CD8 + CD28控制发展T细胞通过促进的功能成熟NKT细胞

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摘要

NK T cells(NKT cells) share functional characteristics and homing properties that are distinct from conventional T cells. In this study, we investigated the contribution of CD28 in the functional development of γδ NKT and αβ NKT cells in mice. We show that CD28 promotes the thymic maturation of promyelocytic leukemia zinc finger+ IL-4+ NKT cells and upregulation of LFA-1 expression on NKT cells. We demonstrate that the developmental defect of γδ NKT cells in CD28-deficient mice is cell autonomous. Moreover, we show in both wild-type C57BL/6 mice and in downstream of tyrosine kinase-1 transgenic mice, a mouse model with increased numbers of γδ NKT cells, that CD28-mediated regulation of thymic IL-4+ NKT cells promotes the differentiation of eomesodermin+ CD44high innate-like CD8+ T cells. These findings reveal a previously unappreciated mechanism by which CD28 controls NKT-cell homeostasis and the size of the innate-like CD8+ T-cell pool.
机译:NK T细胞(NKT细胞)分享功能特点和导航属性有别于传统的T细胞。研究中,我们调查了CD28的贡献功能开发的γδNKT和αβNKT细胞在小鼠体内。胸腺成熟的早幼粒细胞白血病锌手指+ il - 4 + NKT细胞和LFA-1 upregulationNKT细胞上表达。发育缺陷的γδNKT细胞CD28-deficient小鼠细胞自动。我们将展示在野生型C57BL / 6小鼠和下游的酪氨酸激酶1转基因小鼠,与数量的增加小鼠模型γδNKT胸腺细胞,CD28-mediated监管il - 4 + NKT细胞促进分化的eomesodermin + CD44high innate-like CD8 + T细胞。这些发现揭示了先前的赏识机制nkt CD28控制体内平衡和innate-like CD8 +的大小t细胞池。

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