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Gene Deregulation and Chronic Activation in Natural Killer Cells Deficient in the Transcription Factor ETS1

机译:缺乏转录因子ETS1的自然杀伤细胞中的基因调控和慢性激活。

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摘要

Multiple transcription factors guide the development of mature functional natural killer (NK) cells, yet little is known about their function. We used global gene expression and genome-wide binding analyses combined with developmental and functional studies to unveil three roles for the ETS1 transcription factor in NK cells. ETS1 functions at the earliest stages of NK cell development to promote expression of critical transcriptional regulators including T-BET and ID2, NK cell receptors (NKRs) including NKp46, Ly49H, and Ly49D, and signaling molecules essential for NKR function. As a consequence, Ets1 -/- NK cells fail to degranulate after stimulation through activating NKRs. Nonetheless, these cells are hyperresponsive to cytokines and have characteristics of chronic stimulation including increased expression of inhibitory NKRs and multiple activation-associated genes. Therefore, ETS1 regulates a broad gene expression program in NK cells that promotes target cell recognition while limiting cytokine-driven activation.
机译:多种转录因子指导成熟的功能性自然杀伤(NK)细胞的发展,但对其功能知之甚少。我们使用了全局基因表达和全基因组结合分析以及发展和功能研究,揭示了ET细胞在NK细胞中的三个作用。 ETS1在NK细胞发育的最早阶段起作用,以促进关键转录调节因子(包括T-BET和ID2),包括NKp46,Ly49H和Ly49D在内的NK细胞受体(NKR)的表达,以及对NKR功能至关重要的信号分子。结果,在通过激活NKRs刺激后,Ets1-/-NK细胞不能脱粒。但是,这些细胞对细胞因子具有高反应性,并具有慢性刺激的特征,包括抑制性NKRs的表达增加以及与多种激活相关的基因。因此,ETS1调节NK细胞中广泛的基因表达程序,该程序可促进靶细胞识别,同时限制细胞因子驱动的激活。

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