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Systematic discovery of natural CRISPR-Cas12a inhibitors

机译:天然CRISPR-Cas12a抑制剂的系统发现

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摘要

Cas12a (Cpf1) is a CRISPR-associated nuclease with broad utility for synthetic genome engineering, agricultural genomics, and biomedical applications. Although bacteria harboring CRISPR-Cas9 or CRISPR-Cas3 adaptive immune systems sometimes acquire mobile genetic elements encoding anti-CRISPR proteins that inhibit Cas9, Cas3, or the DNA-binding Cascade complex, no such inhibitors have been found for CRISPR-Cas12a. Here we use a comprehensive bioinformatic and experimental screening approach to identify three different inhibitors that block or diminish CRISPR-Cas12a-mediated genome editing in human cells. We also find a widespread connection between CRISPR self-targeting and inhibitor prevalence in prokaryotic genomes, suggesting a straightforward path to the discovery of many more anti-CRISPRs from the microbial world.
机译:Cas12a(Cpf1)是一种与CRISPR相关的核酸酶,在合成基因组工程,农业基因组学和生物医学应用中具有广泛的用途。尽管带有CRISPR-Cas9或CRISPR-Cas3适应性免疫系统的细菌有时会获得可移动的遗传元件,它们编码抑制Cas9,Cas3或与DNA结合的Cascade复合物的抗CRISPR蛋白,但尚未找到针对CRISPR-Cas12a的此类抑制剂。在这里,我们使用一种全面的生物信息学和实验筛选方法来鉴定三种不同的抑制剂,这些抑制剂可以阻断或减少人细胞中CRISPR-Cas12a介导的基因组编辑。我们还在原核生物基因组中发现CRISPR自我靶向与抑制剂普遍存在广泛联系,这表明从微生物界发现更多抗CRISPR的直接途径。

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