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A Broad-Spectrum Inhibitor of CRISPR-Cas9

机译:CRISPR-CAS9的广谱抑制剂

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摘要

CRISPR-Cas9 proteins function within bacterial immune systems to target and destroy invasive DNA and have been harnessed as a robust technology for genome editing. Small bacteriophage-encoded anti-CRISPR proteins (Acrs) can inactivate Cas9, providing an efficient off switch for Cas9-based applications. Here, we show that two Acrs, AcrIIC1 and AcrIIC3, inhibit Cas9 by distinct strategies. AcrIIC1 is a broad-spectrum Cas9 inhibitor that prevents DNA cutting by multiple divergent Cas9 orthologs through direct binding to the conserved HNH catalytic domain of Cas9. A crystal structure of an AcrIIC1-Cas9 HNH domain complex shows how AcrIIC1 traps Cas9 in a DNA-bound but catalytically inactive state. By contrast, AcrIIC3 blocks activity of a single Cas9 ortholog and induces Cas9 dimerization while preventing binding to the target DNA. These two orthogonal mechanisms allow for separate control of Cas9 target binding and cleavage and suggest applications to allow DNA binding while preventing DNA cutting by Cas9.
机译:CRISPR-CAS9蛋白质在细菌免疫系统内靶向并破坏侵入性DNA,并被利用作为基因组编辑的稳健技术。小型噬菌体编码的防克隆蛋白(ACRS)可以灭活CAS9,为Cas9的应用提供有效的开关。在这里,我们展示了两种ACRS,Acriic1和Acriic3,通过独特的策略来抑制Cas9。 Acriic1是一种广谱Cas9抑制剂,可防止通过与Cas9的保守HNH催化结构域的直接结合直接结合多次发散Cas9矫正剂的DNA切割。 ACRIIC1-CAS9 HNH结构域复合物的晶体结构显示了acriic1陷阱Cas9在DNA结合但催化惰性状态下。相反,acriic3阻断单个Cas9 Ortholog的活性,并诱导Cas9二聚化,同时防止与靶DNA结合。这两个正交机制允许单独控制Cas9靶结合和切割,并表明应用以允许DNA结合,同时防止Cas9切割的DNA切割。

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  • 来源
    《Cell》 |2017年第6期|共10页
  • 作者

    Harrington Lucas B.; Doxzen Kevin W.; Ma Enbo; Liu Jun-Jie; Knott Gavin J.; Edraki Alireza; Garcia Bianca; Amrani Nadia; Chen Janice S.; Cofsky Joshua C.; Kranzusch Philip J.; Sontheimer Erik J.; Davidson Alan R.; Maxwell Karen L.; Doudna Jennifer A.;

  • 作者单位

    Univ Calif Berkeley Dept Mol &

    Cell Biol 229 Stanley Hall Berkeley CA 94720 USA;

    Univ Calif Berkeley Biophys Grad Grp Berkeley CA 94720 USA;

    Univ Calif Berkeley Dept Mol &

    Cell Biol 229 Stanley Hall Berkeley CA 94720 USA;

    Univ Calif Berkeley Dept Mol &

    Cell Biol 229 Stanley Hall Berkeley CA 94720 USA;

    Univ Calif Berkeley Dept Mol &

    Cell Biol 229 Stanley Hall Berkeley CA 94720 USA;

    Univ Massachusetts Sch Med RNA Therapeut Inst Program Mol Med Worcester MA 01605 USA;

    Univ Toronto Dept Biochem Toronto ON M5S 1A8 Canada;

    Univ Massachusetts Sch Med RNA Therapeut Inst Program Mol Med Worcester MA 01605 USA;

    Univ Calif Berkeley Dept Mol &

    Cell Biol 229 Stanley Hall Berkeley CA 94720 USA;

    Univ Calif Berkeley Dept Mol &

    Cell Biol 229 Stanley Hall Berkeley CA 94720 USA;

    Harvard Med Sch Dept Microbiol &

    Immunobiol Boston MA 02115 USA;

    Univ Massachusetts Sch Med RNA Therapeut Inst Program Mol Med Worcester MA 01605 USA;

    Univ Toronto Dept Biochem Toronto ON M5S 1A8 Canada;

    Univ Toronto Dept Biochem Toronto ON M5S 1A8 Canada;

    Univ Calif Berkeley Dept Mol &

    Cell Biol 229 Stanley Hall Berkeley CA 94720 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
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