In vivo liver targeted genome editing as therapeutic approach: progresses and challenges.

IF 4.9 Q1 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Frontiers in genome editing Pub Date : 2024-08-23 eCollection Date: 2024-01-01 DOI:10.3389/fgeed.2024.1458037
Chiara Simoni, Elena Barbon, Andrés F Muro, Alessio Cantore
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Abstract

The liver is an essential organ of the body that performs several vital functions, including the metabolism of biomolecules, foreign substances, and toxins, and the production of plasma proteins, such as coagulation factors. There are hundreds of genetic disorders affecting liver functions and, for many of them, the only curative option is orthotopic liver transplantation, which nevertheless entails many risks and long-term complications. Some peculiar features of the liver, such as its large blood flow supply and the tolerogenic immune environment, make it an attractive target for in vivo gene therapy approaches. In recent years, several genome-editing tools mainly based on the clustered regularly interspaced short palindromic repeats associated protein 9 (CRISPR-Cas9) system have been successfully exploited in the context of liver-directed preclinical or clinical therapeutic applications. These include gene knock-out, knock-in, activation, interference, or base and prime editing approaches. Despite many achievements, important challenges still need to be addressed to broaden clinical applications, such as the optimization of the delivery methods, the improvement of the editing efficiency, and the risk of on-target or off-target unwanted effects and chromosomal rearrangements. In this review, we highlight the latest progress in the development of in vivo liver-targeted genome editing approaches for the treatment of genetic disorders. We describe the technological advancements that are currently under investigation, the challenges to overcome for clinical applicability, and the future perspectives of this technology.

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作为治疗方法的体内肝脏靶向基因组编辑:进展与挑战。
肝脏是人体的重要器官,具有多种重要功能,包括代谢生物大分子、外来物质和毒素,以及生成凝血因子等血浆蛋白。影响肝脏功能的遗传性疾病有数百种,其中许多疾病的唯一治疗方法是肝移植,但肝移植存在许多风险和长期并发症。肝脏的一些特殊功能,如大量血流供应和耐受性免疫环境,使其成为体内基因治疗方法的一个有吸引力的靶点。近年来,几种主要基于聚类规则间隔短回文重复序列相关蛋白9(CRISPR-Cas9)系统的基因组编辑工具已成功应用于肝脏定向临床前或临床治疗。这些方法包括基因敲除、敲入、激活、干扰或碱基和质粒编辑方法。尽管取得了许多成就,但要扩大临床应用,仍需应对一些重要挑战,如优化传递方法、提高编辑效率、靶上或靶下意外效应和染色体重排的风险等。在本综述中,我们将重点介绍用于治疗遗传疾病的体内肝脏靶向基因组编辑方法的最新进展。我们介绍了目前正在研究的技术进展、临床应用需要克服的挑战以及这项技术的未来前景。
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来源期刊
CiteScore
7.00
自引率
0.00%
发文量
0
审稿时长
13 weeks
期刊最新文献
Knockout mutation in TaD27 enhances number of productive tillers in hexaploid wheat. Targeting DLBCL by mutation-specific disruption of cancer-driving oncogenes. The potential of HBV cure: an overview of CRISPR-mediated HBV gene disruption. Use of paired Cas9-NG nickase and truncated sgRNAs for single-nucleotide microbial genome editing. Making gene editing accessible in resource limited environments: recommendations to guide a first-time user.
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