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Transcriptional regulation and T cell exhaustion

机译:转录调控和T细胞衰竭

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PURPOSE OF REVIEW: This review highlights the control of transcriptional networks, including induction of inhibitory receptors, by T cell-specific transcription factors in exhausted T cells that accumulate in chronic viral infections including HIV. RECENT FINDINGS: Transcriptional profiling has established distinct molecular phenotypes for exhausted CD4+ and CD8+ T cells in chronic viral infection models. There exists a subset of transcription factors associated with exhaustion, notably Blimp-1, basic leucine zipper transcription factor, ATF-like and Helios. Epigenetic phenomena are likely important in regulating gene expression networks during exhaustion as illustrated by programmed death 1 promoter methylation patterns. SUMMARY: Following chronic viral infections, CD4 and CD8 T cells defined functionally and phenotypically as exhausted have distinct transcriptional profiles. These studies have identified a core set of transcription factors that have been implicated in promoting exhaustion. However, no single factor appears to be an exhaustion determining factor, suggesting that T cell exhaustion reflects a combinatorial mechanism with multiple transcription factors interacting to influence the development of functionally exhausted T cells as well as different T effector populations.
机译:综述的目的:这篇综述强调了在疲惫的T细胞中积累的T细胞特异性转录因子对转录网络的控制,包括抑制性受体的诱导,这些T细胞在包括HIV在内的慢性病毒感染中积累。最近的发现:转录谱分析为慢性病毒感染模型中的疲惫的CD4 +和CD8 + T细胞建立了独特的分子表型。存在与疲劳相关的转录因子子集,尤其是Blimp-1,碱性亮氨酸拉链转录因子,ATF样和Helios。表观遗传现象可能在精疲力竭中调节基因表达网络中很重要,如程序性死亡1启动子甲基化模式所示。摘要:在慢性病毒感染后,功能和表型定义为疲惫的CD4和CD8 T细胞具有独特的转录谱。这些研究已经确定了一组核心转录因子,这些因子与促进力竭有关。但是,没有一个单一的因素似乎是衰竭的决定因素,这表明T细胞的衰竭反映了多种转录因子相互作用的组合机制,这些转录因子相互作用以影响功能衰竭的T细胞以及不同的T效应子群体的发育。

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