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T-Bet and Eomes Regulate the Balance between the Effector/Central Memory T Cells versus Memory Stem Like T Cells

机译:T-Bet和Eomes调节效应子/中央记忆T细胞与记忆干样T细胞之间的平衡

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摘要

Memory T cells are composed of effector, central, and memory stem cells. Previous studies have implicated that both T-bet and Eomes are involved in the generation of effector and central memory CD8 T cells. The exact role of these transcription factors in shaping the memory T cell pool is not well understood, particularly with memory stem T cells. Here, we demonstrate that both T-bet or Eomes are required for elimination of established tumors by adoptively transferred CD8 T cells. We also examined the role of T-bet and Eomes in the generation of tumor-specific memory T cell subsets upon adoptive transfer. We showed that combined T-bet and Eomes deficiency resulted in a severe reduction in the number of effector/central memory T cells but an increase in the percentage of CD62LhighCD44low Sca-1+ T cells which were similar to the phenotype of memory stem T cells. Despite preserving large numbers of phenotypic memory stem T cells, the lack of both of T-bet and Eomes resulted in a profound defect in antitumor memory responses, suggesting T-bet and Eomes are crucial for the antitumor function of these memory T cells. Our study establishes that T-bet and Eomes cooperate to promote the phenotype of effector/central memory CD8 T cell versus that of memory stem like T cells.
机译:记忆T细胞由效应干细胞,中央干细胞和记忆干细胞组成。先前的研究暗示T-bet和Eomes均参与效应子和中央记忆CD8 T细胞的产生。这些转录因子在塑造记忆T细胞库中的确切作用尚不清楚,特别是对于记忆干T细胞。在这里,我们证明通过过继转移的CD8 T细胞消除既定的肿瘤需要T-bet或Eomes。我们还研究了过继转移后T-bet和Eomes在肿瘤特异性记忆T细胞亚群生成中的作用。我们发现,T-bet和Eomes缺乏症共同导致效应子/中央记忆T细胞数量的严重减少,但CD62L high CD44 low 的百分比增加Sca-1 + T细胞与记忆干T细胞的表型相似。尽管保留了大量的表型记忆干T细胞,但T-bet和Eomes的缺乏导致抗肿瘤记忆反应的严重缺陷,这表明T-bet和Eomes对于这些记忆T细胞的抗肿瘤功能至关重要。我们的研究建立了T-bet和Eomes共同促进效应子/中央记忆CD8 T细胞表型与记忆干细胞像T细胞一样的表型。

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