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Cytoplasmic‐translocated Ku70 senses intracellular DNA and mediates interferon‐lambda1 induction

机译:细胞质翻译Ku70感测细胞内DNA介质干扰素 - λ1诱导

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摘要

We have previously identified that human Ku70, a nuclear protein, serves as a cytosolic DNA sensor. Upon transfection with DNA or infection with DNA virus, Ku70 translocates from the nucleus into the cytoplasm and then predominately induces interferon lambda1 (IFN‐λ1) rather than IFN‐alpha or IFN‐beta, through a STING‐dependent signalling pathway. However, a detailed mechanism for Ku70 cytoplasmic translocation and its correlation with IFN‐λ1 induction have not been fully elucidated. Here, we observed that cytoplasmic translocation of Ku70 only occurred in DNA‐triggered IFN‐λ1‐inducible cells. Additionally, infection by Herpes simplex virus type‐1 (HSV‐1), a DNA virus, induces cytoplasmic translocation of Ku70 and IFN‐λ1 induction in a strain‐dependent manner: the translocation and IFN‐λ1 induction were detected upon infection by HSV‐1 McKrae, but not MacIntyre, strain. A kinetic analysis indicated that cytoplasmic translocation of Ku70 was initiated right after DNA transfection and was peaked at 6 hr after DNA stimulation. Furthermore, treatment with leptomycin B, a nuclear export inhibitor, inhibited both Ku70 translocation and IFN‐λ1 induction, suggesting that Ku70 translocation is an essential and early event for its cytosolic DNA sensing. We further confirmed that enhancing the acetylation status of the cells promotes Ku70’s cytoplasmic accumulation, and therefore increases DNA‐mediated IFN‐λ1 induction. These findings provide insights into the molecular mechanism by which the versatile sensor detects pathogenic DNA in a localization‐dependent manner.
机译:之前我们已经确定了人类的KU70,核蛋白,作为一种胞质DNA传感器。当与DNA转染或感染的DNA病毒,从细胞核进入细胞质KU70易位,然后主要诱导干扰素lambda1(IFN-λ1),而不是IFN-α或IFN-β,通过刺依赖性信号转导途径。然而,KU70细胞质迁移及其与IFN-λ1诱导相关的详细机制尚未完全阐明。在这里,我们观察到,KU70的细胞质迁移仅发生在DNA触发的IFN-λ1诱导细胞。此外,感染单纯疱疹病毒1型(HSV-1),一种DNA病毒,诱导KU70和IFN-λ1诱导细胞质易位的应变依赖性的方式:由HSV感染时被检测出的移位和IFN-λ1感应-1 McKrae,但不麦金太尔,应变。动力学分析表明,KU70的细胞质易位DNA转染后右发起并在DNA刺激后6小时达到峰值被。此外,细霉素B,核输出抑制剂的治疗,抑制了KU70易位和IFN-λ1诱导,这表明KU70易位是其胞质DNA感测的基本和早期事件。我们进一步证实,增强细胞的乙酰化状态促进KU70的细胞质中的积累,并因此增加DNA介导的IFN-λ1诱导。这些发现提供了见解,通过该多功能传感器检测在定位依赖性方式致病的DNA的分子机制。

著录项

  • 期刊名称 Immunology
  • 作者单位
  • 年(卷),期 2021(163),3
  • 年度 2021
  • 页码 323–337
  • 总页数 15
  • 原文格式 PDF
  • 正文语种
  • 中图分类 免疫学;
  • 关键词

    机译:乙酰化;细胞溶质DNA传感器;IFN-λ1;ku70;易位;

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