Single nucleotide substitutions effectively block Cas9 and allow for scarless genome editing in Caenorhabditis elegans

IF 3.3 3区 生物学 Genetics Pub Date : 2021-09-14 DOI:10.1101/2021.09.14.460298
J. C. Medley, Shilpa Hebbar, Joel T. Sydzyik, Anna Y. Zinovyeva
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引用次数: 6

Abstract

In Caenorhabditis elegans, germline injection of Cas9 complexes is reliably used to achieve genome editing through homology-directed repair of Cas9-generated DNA breaks. To prevent Cas9 from targeting repaired DNA, additional blocking mutations are often incorporated into homologous repair templates. Cas9 can be blocked either by mutating the PAM sequence that is essential for Cas9 activity or by mutating the guide sequence that targets Cas9 to a specific genomic location. However, it is unclear how many nucleotides within the guide sequence should be mutated, since Cas9 can recognize “off-target” sequences that are imperfectly paired to its guide. In this study, we examined whether single-nucleotide substitutions within the guide sequence are sufficient to block Cas9 and allow for efficient genome editing. We show that a single mismatch within the guide sequence effectively blocks Cas9 and allows for recovery of edited animals. Surprisingly, we found that a low rate of edited animals can be recovered without introducing any blocking mutations, suggesting a temporal block to Cas9 activity in C. elegans. Furthermore, we show that the maternal genome of hermaphrodite animals is preferentially edited over the paternal genome. We demonstrate that maternally provided haplotypes can be selected using balancer chromosomes and propose a method of mutant isolation that greatly reduces screening efforts post-injection. Collectively, our findings expand the repertoire of genome editing strategies in C. elegans and demonstrate that extraneous blocking mutations are not required to recover edited animals when the desired mutation is located within the guide sequence.
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在秀丽隐杆线虫中,单核苷酸替换有效地阻断Cas9并允许无疤痕的基因组编辑
在秀丽隐杆线虫中,通过同源定向修复Cas9产生的DNA断裂,可靠地使用Cas9复合物的种系注射来实现基因组编辑。为了防止Cas9靶向修复的DNA,通常在同源修复模板中加入额外的阻断突变。可以通过突变对Cas9活性至关重要的PAM序列或通过将靶向Cas9的引导序列突变到特定的基因组位置来阻断Cas9。然而,目前尚不清楚引导序列中有多少核苷酸应该发生突变,因为Cas9可以识别与其引导序列不完全配对的“脱靶”序列。在这项研究中,我们检查了引导序列中的单核苷酸取代是否足以阻断Cas9并允许有效的基因组编辑。我们表明,引导序列中的单一失配有效地阻断了Cas9,并允许恢复编辑的动物。令人惊讶的是,我们发现,在不引入任何阻断突变的情况下,可以恢复低比率的编辑动物,这表明秀丽隐杆线虫的Cas9活性存在时间阻断。此外,我们还表明,雌雄同体动物的母体基因组优先于父系基因组进行编辑。我们证明,可以使用平衡染色体选择母体提供的单倍型,并提出了一种突变分离方法,大大减少了注射后的筛选工作。总之,我们的发现扩展了秀丽隐杆线虫基因组编辑策略的范围,并证明当所需突变位于指导序列内时,不需要额外的阻断突变来恢复编辑过的动物。
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来源期刊
Genetics
Genetics 生物-遗传学
CiteScore
6.20
自引率
6.10%
发文量
177
期刊介绍: GENETICS is published by the Genetics Society of America, a scholarly society that seeks to deepen our understanding of the living world by advancing our understanding of genetics. Since 1916, GENETICS has published high-quality, original research presenting novel findings bearing on genetics and genomics. The journal publishes empirical studies of organisms ranging from microbes to humans, as well as theoretical work. While it has an illustrious history, GENETICS has changed along with the communities it serves: it is not your mentor''s journal. The editors make decisions quickly – in around 30 days – without sacrificing the excellence and scholarship for which the journal has long been known. GENETICS is a peer reviewed, peer-edited journal, with an international reach and increasing visibility and impact. All editorial decisions are made through collaboration of at least two editors who are practicing scientists. GENETICS is constantly innovating: expanded types of content include Reviews, Commentary (current issues of interest to geneticists), Perspectives (historical), Primers (to introduce primary literature into the classroom), Toolbox Reviews, plus YeastBook, FlyBook, and WormBook (coming spring 2016). For particularly time-sensitive results, we publish Communications. As part of our mission to serve our communities, we''ve published thematic collections, including Genomic Selection, Multiparental Populations, Mouse Collaborative Cross, and the Genetics of Sex.
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