Long sequence insertion via CRISPR/Cas gene-editing with transposase, recombinase, and integrase

IF 4.7 3区工程技术 Q2 ENGINEERING, BIOMEDICAL

Current Opinion in Biomedical Engineering Pub Date : 2023-07-22 DOI:10.1016/j.cobme.2023.100491

Xiaotong Wang , Guangxue Xu , William A. Johnson , Yuanhao Qu , Di Yin , Nurupa Ramkissoon , Hong Xiang , Le Cong

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引用次数: 0

Abstract

CRISPR/Cas-based gene-editing technologies have emerged as one of the most transformative tools in genome science over the past decade, providing unprecedented possibilities for both fundamental and translational research. Following the initial wave of innovations for gene knock-out, epigenetic/RNA modulation, and nickase-mediated base-editing, recent efforts have pivoted towards long-sequence gene editing—specifically, the insertion of large fragments (>1 kb) into the endogenous genome. In this review, we survey the development of these CRISPR/Cas-based sequence insertion methodologies in conjunction with the emergence of novel families of editing enzymes, such as transposases, single-stranded DNA-annealing proteins, recombinases, and integrases. Despite facing a number of challenges, this field continues to evolve rapidly and holds the potential to catalyze a new wave of revolutionary biomedical applications.

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利用转座酶、重组酶和整合酶进行CRISPR/Cas基因编辑的长序列插入

在过去的十年里，基于CRISPR/ cas的基因编辑技术已经成为基因组科学中最具变革性的工具之一，为基础研究和转化研究提供了前所未有的可能性。继基因敲除、表观遗传/RNA调节和镍酶介导的碱基编辑的最初创新浪潮之后，最近的努力转向了长序列基因编辑，特别是将大片段(1kb)插入内源基因组。在这篇综述中，我们调查了这些基于CRISPR/ cas的序列插入方法的发展，并结合了新的编辑酶家族的出现，如转座酶、单链dna退火蛋白、重组酶和整合酶。尽管面临着许多挑战，但这一领域继续迅速发展，并有可能催化一波新的革命性生物医学应用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Current Opinion in Biomedical Engineering Medicine-Medicine (miscellaneous)

CiteScore

8.60

自引率

2.60%

发文量