Recent application of CRISPR-Cas12 and OMEGA system for genome editing

清脆的 基因组编辑 Cas9 生物 计算生物学 基因 基因组 遗传学
作者
Isabel Wen Badon,Yeounsun Oh,Ho-Joong Kim,Seung Hwan Lee
出处
期刊:Molecular Therapy [Elsevier]
卷期号:32 (1): 32-43 被引量:1
标识
DOI:10.1016/j.ymthe.2023.11.013
摘要

In 2012, it was discovered that precise gene editing could be induced in target DNA using the reprogrammable characteristics of the CRISPR system. Since then, several studies have investigated the potential of the CRISPR system to edit various biological organisms. For the typical CRISPR system obtained from bacteria and archaea, many application studies have been conducted and have spread to various fields. To date, orthologs with various characteristics other than CRISPR-Cas9 have been discovered and are being intensively studied in the field of gene editing. CRISPR-Cas12 and its varied orthologs are representative examples of genome editing tools and have superior properties in terms of in vivo target gene editing compared with Cas9. Recently, TnpB and Fanzor of the OMEGA (obligate mobile element guided activity) system were identified to be the ancestor of CRISPR-Cas12 on the basis of phylogenetic analysis. Notably, the compact sizes of Cas12 and OMEGA endonucleases allow adeno-associated virus (AAV) delivery; hence, they are set to challenge Cas9 for in vivo gene therapy. This review is focused on these RNA-guided reprogrammable endonucleases: their structure, biochemistry, off-target effects, and applications in therapeutic gene editing.
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