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Cas4-Cas1 fusions drive efficient PAM selection and control CRISPR adaptation

机译:CAS4-CAS1融合驾驶高效PAM选择和控制CRISPR适应

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摘要

Microbes have the unique ability to acquire immunological memories from mobile genetic invaders to protect themselves from predation. To confer CRISPR resistance, new spacers need to be compatible with a targeting requirement in the invader's DNA called the protospacer adjacent motif (PAM). Many CRISPR systems encode Cas4 proteins to ensure new spacers are integrated that meet this targeting prerequisite. Here we report that a gene fusion between cas4 and cas1 from the Geobacter sulfurreducens I-U CRISPR-Cas system is capable of introducing functional spacers carrying interference proficient TTN PAM sequences at much higher frequencies than unfused Cas4 adaptation modules. Mutations of Cas4-domain catalytic residues resulted in dramatically decreased naive and primed spacer acquisition, and a loss of PAM selectivity showing that the Cas4 domain controls Cas1 activity. We propose the fusion gene evolved to drive the acquisition of only PAM-compatible spacers to optimize CRISPR interference.
机译:微生物具有从移动遗传入侵者获得免疫记忆的独特能力,以保护自己免受捕食。为了赋予Crispr抗性,新的垫片需要与入侵者DNA中的靶向要求相容,称为Protospacer相邻的主题(PAM)。许多CRISPR系统编码CAS4蛋白质以确保集成了新的垫片,以满足该靶向先决条件。在这里,我们认为Cas4和Cas1之间的基因融合来自Geobacter SulfurredeCens I-U CRISPR-CAS系统的功能能够引入携带干扰熟练TTN PAM序列的功能间隔,而不是未使用的CAS4适配模块的频率。 Cas4-结构域催化残基的突变导致显着降低的幼稚和灌注间隔物采集,以及损失的PAM选择性,显示CAS4结构域对Cas1活性进行控制。我们提出了融合基因演变,以驱动仅采集的普遍兼容的垫片以优化Crispr的干扰。

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  • 来源
    《Nucleic Acids Research》 |2019年第10期|共8页
  • 作者单位

    Delft Univ Technol Dept Bionanosci Kavli Inst Nanosci Maasweg 9 NL-2629 HZ Delft Netherlands;

    Delft Univ Technol Dept Bionanosci Kavli Inst Nanosci Maasweg 9 NL-2629 HZ Delft Netherlands;

    Delft Univ Technol Dept Bionanosci Kavli Inst Nanosci Maasweg 9 NL-2629 HZ Delft Netherlands;

    Delft Univ Technol Dept Bionanosci Kavli Inst Nanosci Maasweg 9 NL-2629 HZ Delft Netherlands;

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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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