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首页> 外文期刊>Journal of cellular and molecular medicine. >Down‐regulation of EOMES drives T‐cell exhaustion via abolishing EOMES‐mediated repression of inhibitory receptors of T cells in liver cancer
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Down‐regulation of EOMES drives T‐cell exhaustion via abolishing EOMES‐mediated repression of inhibitory receptors of T cells in liver cancer

机译:eomes的下调通过废除浓度介导的T细胞耗尽来介导肝癌中T细胞抑制剂的抑制剂抑制

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摘要

T‐cell exhaustion is one of the hallmarks in cancer, but the mechanisms underlying T‐cell dysregulation remains unclear. Here, we reported that down‐regulation of transcription factor EOMES contributed to increased levels of inhibitory receptors in T cell among the tumour tissues and resulted in the poor prognosis of hepatocellular carcinoma (HCC). By analysing the correlation between EOMES in tumour‐infiltrating T cells and the clinical features, we demonstrated that the EOMES was related to the advanced stage and poor prognosis of HCC. Further mechanistic studies revealed that the EOMES mainly expressed in the CD8 T cells and were down‐regulated in tumour samples. Moreover, we demonstrated that the EOMES directly bound at the transcriptional regulatory regions of the key inhibitory factors including PD‐1, CTAL‐4 and CD39, and lower levels of EOMES contributed to overexpression of these factors in T cells. Together, our studies provide new insight into the transcriptional deregulation of the inhibitory receptors on T cells during the tumorigenesis.
机译:T细胞疲惫是癌症的标志之一,但T细胞失调的机制仍然尚不清楚。在这里,我们报道了转录因子浓度的下调导致肿瘤组织中T细胞中的抑制作用水平增加,导致肝细胞癌(HCC)的预后差。通过分析肿瘤渗透T细胞和临床特征的浓度与临床特征之间的相关性,综合症素与HCC的先进阶段和差的预后有关。进一步的机械研究表明,煤矿主要在CD8 T细胞中表达并在肿瘤样品中下调。此外,我们证明了在包括PD-1,CTAL-4和CD39的关键抑制因子的转录调节区域的eOME,以及较低水平的浓度导致T细胞中这些因素的过度表达。我们的研究在一起,为在肿瘤发生期间对T细胞上的抑制性受体的转录放松作用进行了新的洞察。

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