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Structure-specific endonuclease activity of SNM1A enables processing of a DNA interstrand crosslink

机译:SNM1A的结构特异性内切核酸酶活性能够处理DNA Interstrand Crosslink

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摘要

DNA interstrand crosslinks (ICLs) covalently join opposing strands, blocking both replication and transcription, therefore making ICL-inducing compounds highly toxic and ideal anti-cancer agents. While incisions surrounding the ICL are required to remove damaged DNA, it is currently unclear which endonucleases are needed for this key event. SNM1A has been shown to play an important function in human ICL repair, however its suggested role has been limited to exonuclease activity and not strand incision. Here we show that SNM1A has endonuclease activity, having the ability to cleave DNA structures that arise during the initiation of ICL repair. In particular, this endonuclease activity cleaves singlestranded DNA. Given that unpaired DNA regions occur 5' to an ICL, these findings suggest SNM1A may act as either an endonuclease and/or exonuclease during ICL repair. This finding is significant as it expands the potential role of SNM1A in ICL repair.
机译:DNA Interstrand Crosslinks(ICL)共价加入相对的链,阻断复制和转录,因此使ICL诱导的化合物具有高毒性和理想的抗癌剂。 虽然ICL周围的切口需要去除受损的DNA,但目前不清楚该关键事件需要哪种内切核酸酶。 SNM1A已被证明可以在人类ICL修复中发挥重要功能,但其建议的作用仅限于外切核酸酶活性而不是绞喉切口。 在这里,我们表明SNM1A具有内切核酸酶活性,能够能够切割在ICL修复期间产生的DNA结构。 特别是,这种内切核酸酶活性切割单表单集的DNA。 鉴于未配对的DNA区域发生5'到ICL,这些发现表明SNM1A可以在ICL修复期间用作内切核酸酶和/或外切核酸酶。 这一发现很重要,因为它扩大了SNM1A在ICL修复中的潜在作用。

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  • 来源
    《Nucleic Acids Research》 |2018年第17期|共10页
  • 作者单位

    McMaster Univ Fac Hlth Sci Dept Biochem &

    Biomed Sci Hamilton ON L8N 3Z5 Canada;

    Western Univ Schulich Sch Med &

    Dent Dept Biochem London ON N6A 5C1 Canada;

    McMaster Univ Fac Hlth Sci Dept Biochem &

    Biomed Sci Hamilton ON L8N 3Z5 Canada;

    McMaster Univ Fac Hlth Sci Dept Biochem &

    Biomed Sci Hamilton ON L8N 3Z5 Canada;

    McMaster Univ Fac Hlth Sci Dept Biochem &

    Biomed Sci Hamilton ON L8N 3Z5 Canada;

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