首页> 外文OA文献 >Initiation of DNA interstrand cross-link repair in humans: the nucleotide excision repair system makes dual incisions 5' to the cross-linked base and removes a 22- to 28-nucleotide-long damage-free strand.
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Initiation of DNA interstrand cross-link repair in humans: the nucleotide excision repair system makes dual incisions 5' to the cross-linked base and removes a 22- to 28-nucleotide-long damage-free strand.

机译:在人类中启动DNA链间交联修复:核苷酸切除修复系统在交联碱基的5'处形成双切口,并去除了22至28个核苷酸长的无损伤链。

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摘要

Most DNA repair mechanisms rely on the redundant information inherent to the duplex to remove damaged nucleotides and replace them with normal ones, using the complementary strand as a template. Interstrand cross-links pose a unique challenge to the DNA repair machinery because both strands are damaged. To study the repair of interstrand cross-links by mammalian cells, we tested the activities of cell extracts of wild-type or excision repair-defective rodent cell lines and of purified human excision nuclease on a duplex with a site-specific cross-link. We found that in contrast to monoadducts, which are removed by dual incisions bracketing the lesion, the cross-link causes dual incisions, both 5' to the cross-link in one of the two strands. The net result is the generation of a 22- to 28-nucleotide-long gap immediately 5' to the cross-link. This gap may act as a recombinogenic signal to initiate cross-link removal.
机译:大多数DNA修复机制都依赖于双链体固有的冗余信息,以互补链为模板,去除受损的核苷酸并将其替换为正常的核苷酸。链间交联对DNA修复机制提出了独特的挑战,因为两条链均被破坏。为了研究哺乳动物细胞对链间交联的修复,我们在具有位点特异性交联的双链体上测试了野生型或切除修复缺陷型啮齿动物细胞系和纯化的人类切除核酸酶的细胞提取物的活性。我们发现,与单加合物不同,该双加合物通过括号内的病灶的双切口去除,交联导致双切口,两个链中的5'均与交联成一条。最终结果是在交联处紧靠5'端产生了22至28个核苷酸长的缺口。该间隙可以充当重组信号以启动交联去除。

著录项

  • 作者

    Bessho, T; Mu, D; Sancar, A;

  • 作者单位
  • 年度 1997
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  • 原文格式 PDF
  • 正文语种 en
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