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首页> 外文期刊>Nature immunology >Safeguard function of PU.1 shapes the inflammatory epigenome of neutrophils
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Safeguard function of PU.1 shapes the inflammatory epigenome of neutrophils

机译:PU.1的保障功能塑造中性粒细胞的炎症外观蛋白酶

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摘要

Neutrophils are essential first-line defense cells against invading pathogens, yet when inappropriately activated, their strong immune response can cause collateral tissue damage and contributes to immunological diseases. However, whether neutrophils can intrinsically titrate their immune response remains unknown. Here we conditionally deleted the Spi1 gene, which encodes the myeloid transcription factor PU.1, from neutrophils of mice undergoing fungal infection and then performed comprehensive epigenomic profiling. We found that as well as providing the transcriptional prerequisite for eradicating pathogens, the predominant function of PU.1 was to restrain the neutrophil defense by broadly inhibiting the accessibility of enhancers via the recruitment of histone deacetylase 1. Such epigenetic modifications impeded the immunostimulatory AP-1 transcription factor JUNB from entering chromatin and activating its targets. Thus, neutrophils rely on a PU.1-installed inhibitor program to safeguard their epigenome from undergoing uncontrolled activation, protecting the host against an exorbitant innate immune response.
机译:中性粒细胞是必不可少的一线防御细胞反对入侵病原体,但在不恰当的激活时,它们的强烈免疫反应会导致抵押组织损伤并导致免疫疾病。然而,中性粒细胞是否可以本质上滴定其免疫反应仍然未知。在这里,我们有条件地删除了编码髓样转录因子PU.1的SPI1基因,从遭受真菌感染的小鼠中性粒细胞,然后进行全面的表观型分析。我们发现,除了通过募集组蛋白脱乙酰化酶1.募集组蛋白脱乙酰化酶1,PU.1的主要功能是通过募集抑制增强剂的可及性来抑制中性粒细胞防御。这种表观遗传修饰阻碍了免疫刺激剂1转录因子junb进入染色质并激活其目标。因此,嗜中性粒细胞依赖于PU.1安装的抑制剂计划,以保护其外延蛋白组经受不受控制的活化,保护宿主免受过高的先天免疫应答。

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