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首页> 外文期刊>PLoS One >Tumor-infiltrating CD62L + PD-1 - CD8 T cells retain proliferative potential via Bcl6 expression and replenish effector T cells within the tumor
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Tumor-infiltrating CD62L + PD-1 - CD8 T cells retain proliferative potential via Bcl6 expression and replenish effector T cells within the tumor

机译:肿瘤浸润的CD62L + PD-1 - CD8 T细胞通过BCl6表达保留增殖潜力,并在肿瘤内补充效应T细胞

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摘要

Tumor antigen–primed CD8 T cells differentiate into effector T cells that kill tumor cells rapidly, whereas durable responses of CD8 T cells are required to cope with long-lasting tumor growth. However, it is not well known how persisting CD8 T cells are generated. In this study, we analyzed CD8 T cells primed by antigens in tumor-draining lymph nodes and found that CD8 T cells first differentiated into a CD62L-intermediate (CD62L int ) stage upon antigen stimulation. These cells gave rise to tumor-infiltrating CD62L - CD44 high Bcl6 - effector T cells and CD62L + CD44 high Bcl6 + memory-like T cells. Memory-like T cells within the tumor expressed CD127, CXCR3 and had the potential to proliferate significantly when they were transferred into tumor-bearing mice. Bcl6 expression in these T cells was critical because Bcl6 -/- CD62L + CD44 high CD8T cells within the tumor were defective in expansion after secondary transfer. Taken together, our findings show that CD62L + CD44 high Bcl6 + cells are generated from highly proliferating CD62L int T cells and retain high proliferative potential, which contributes to replenishment of effector T cells within the tumor.
机译:肿瘤抗原 - 引发的CD8 T细胞分化为迅速杀死肿瘤细胞的效应T细胞,而CD8 T细胞的耐用反应需要应对持久的肿瘤生长。然而,尚不为众所周知,如何持久地产生CD8 T细胞。在该研究中,我们分析了肿瘤排水淋巴结中的抗原引发的CD8 T细胞,发现CD8 T细胞首先在抗原刺激时分化成CD62L-中间体(CD62L int)阶段。这些细胞产生肿瘤浸润的CD62L - CD44高BCl6 - 效应T细胞和CD62L + CD44高Bcl6 +记忆样T细胞。肿瘤内的记忆样T细胞表达CD127,CXCR3,并且当它们转移到肿瘤的小鼠中时具有显着促进的可能性。这些T细胞中的Bcl6表达至关重要,因为在肿瘤内的BCl6 - / - CD62L + CD44高CD8T细胞在二次转移后膨胀差异有缺陷。我们的研究结果表明,CD62L + CD44高Bcl6 +细胞由高增殖的CD62L型T细胞产生并保留高增殖潜力,这有助于补充肿瘤内的效应T细胞。

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