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FACT is a sensor of DNA torsional stress in eukaryotic cells

机译:事实是真核细胞中DNA扭转应激的传感器

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摘要

Transitions of B-DNA to alternative DNA structures (ADS) can be triggered by negative torsional strain, which occurs during replication and transcription, and may lead to genomic instability. However, how ADS are recognized in cells is unclear. We found that the binding of candidate anticancer drug, curaxin, to cellular DNA results in uncoiling of nucleosomal DNA, accumulation of negative supercoiling and conversion of multiple regions of genomic DNA into left-handed Z-form. Histone chaperone FACT binds rapidly to the same regions via the SSRP1 subunit in curaxin-treated cells. In vitro binding of purified SSRP1 or its isolated CID domain to a methylated DNA fragment containing alternating purine/pyrimidines, which is prone to Z-DNA transition, is much stronger than to other types of DNA. We propose that FACT can recognize and bind Z-DNA or DNA in transition from a B to Z form. Binding of FACT to these genomic regions triggers a p53 response. Furthermore, FACT has been shown to bind to other types of ADS through a different structural domain, which also leads to p53 activation. Thus, we propose that FACT acts as a sensor of ADS formation in cells. Recognition of ADS by FACT followed by a p53 response may explain the role of FACT in DNA damage prevention.
机译:B-DNA转变为替代DNA结构(ADS)可以通过阴性扭转应变引发,在复制和转录期间发生,并且可能导致基因组不稳定性。但是,在细胞中如何识别广告是不清楚的。我们发现候选抗癌药物,曲突与细胞DNA的结合导致细胞DNA的未磁性DNA,将阴性超咖啡的积累和基因组DNA的多个区域转化为左手Z形式。组蛋白伴侣的事实通过Cuxin处理细胞中的SSRP1亚基迅速结合到相同的区域。将纯化的SSRP1或其分离的CID结构域的体外结合到含有交替嘌呤/嘧啶的甲基化DNA片段,其易于Z-DNA转变,比其他类型的DNA更强大。我们提出该事实可以识别和结合Z-DNA或DNA在从B到Z形式转变。对这些基因组区域的事实结合触发了p53的反应。此外,已经证明了事实是通过不同的结构结构域与其他类型的ADS结合,这也导致P53激活。因此,我们提出了该事实作为细胞中ADS形成的传感器。事实上识别广告,其次是P53响应可以解释事实在DNA损伤预防中的作用。

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  • 来源
    《Nucleic Acids Research》 |2017年第4期|共21页
  • 作者单位

    Roswell Pk Canc Inst Dept Cell Stress Biol Elm &

    Carlton St Buffalo NY 14127 USA;

    Roswell Pk Canc Inst Dept Cell Stress Biol Elm &

    Carlton St Buffalo NY 14127 USA;

    Roswell Pk Canc Inst Dept Cell Stress Biol Elm &

    Carlton St Buffalo NY 14127 USA;

    Univ Haifa Dept Evolutionary &

    Environm Biol Tauber Bioinformat Res Ctr IL-31905 Haifa Israel;

    Blokhin Canc Res Ctr RAMS Inst Carcinogenesis Dept Chem Carcinogenesis Moscow 115478 Russia;

    Blokhin Canc Res Ctr RAMS Inst Carcinogenesis Dept Chem Carcinogenesis Moscow 115478 Russia;

    Blokhin Canc Res Ctr RAMS Inst Carcinogenesis Dept Chem Carcinogenesis Moscow 115478 Russia;

    Blokhin Canc Res Ctr RAMS Inst Carcinogenesis Dept Chem Carcinogenesis Moscow 115478 Russia;

    Roswell Pk Canc Inst Dept Cell Stress Biol Elm &

    Carlton St Buffalo NY 14127 USA;

    Ariel Univ Dept Mol Biol IL-40700 Ariel Israel;

    Roswell Pk Canc Inst Dept Bioinformat Elm &

    Carlton St Buffalo NY 14127 USA;

    Roswell Pk Canc Inst Dept Bioinformat Elm &

    Carlton St Buffalo NY 14127 USA;

    Blokhin Canc Res Ctr RAMS Inst Carcinogenesis Dept Chem Carcinogenesis Moscow 115478 Russia;

    Univ Texas Dallas Dept Mol &

    Cell Biol 800 W Campbell Rd Richardson TX 75080 USA;

    Roswell Pk Canc Inst Dept Cell Stress Biol Elm &

    Carlton St Buffalo NY 14127 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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