The delivery challenge: fulfilling the promise of therapeutic genome editing

基因组编辑 计算生物学 遗传增强 核酸酶 免疫原性 基因传递 基因 基因组 基因组工程 生物 遗传学 免疫系统
作者
Joost van Haasteren,Jie Li,Olivia J. Scheideler,Niren Murthy,David V. Schaffer
出处
期刊:Nature Biotechnology [Springer Nature]
卷期号:38 (7): 845-855 被引量:190
标识
DOI:10.1038/s41587-020-0565-5
摘要

Genome editing has the potential to treat an extensive range of incurable monogenic and complex diseases. In particular, advances in sequence-specific nuclease technologies have dramatically accelerated the development of therapeutic genome editing strategies that are based on either the knockout of disease-causing genes or the repair of endogenous mutated genes. These technologies are progressing into human clinical trials. However, challenges remain before the therapeutic potential of genome editing can be fully realized. Delivery technologies that have serendipitously been developed over the past couple decades in the protein and nucleic acid delivery fields have been crucial to genome editing success to date, including adeno-associated viral and lentiviral vectors for gene therapy and lipid nanoparticle and other non-viral vectors for nucleic acid and protein delivery. However, the efficiency and tissue targeting capabilities of these vehicles must be further improved. In addition, the genome editing enzymes themselves need to be optimized, and challenges regarding their editing efficiency, specificity and immunogenicity must be addressed. Emerging protein engineering and synthetic chemistry approaches can offer solutions and enable the development of safe and efficacious clinical genome editing.
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