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在人类细胞和小鼠原代成肌细胞中精确的碱基编辑而无非预期的插入缺失。

Precise base editing without unintended indels in human cells and mouse primary myoblasts.

机构信息

Department of Physiology, Korea University College of Medicine, Seoul, 02841, Republic of Korea.

Department of Medicine, Korea University College of Medicine, Seoul, 02841, Republic of Korea.

出版信息

Exp Mol Med. 2023 Dec;55(12):2586-2595. doi: 10.1038/s12276-023-01128-4. Epub 2023 Dec 1.

Abstract

Base editors are powerful tools for making precise single-nucleotide changes in the genome. However, they can lead to unintended insertions and deletions at the target sites, which is a significant limitation for clinical applications. In this study, we aimed to eliminate unwanted indels at the target sites caused by various evolved base editors. Accordingly, we applied dead Cas9 instead of nickase Cas9 in the base editors to induce accurate substitutions without indels. Additionally, we tested the use of chromatin-modulating peptides in the base editors to improve nucleotide conversion efficiency. We found that using both dead Cas9 and chromatin-modulating peptides in base editing improved the nucleotide substitution efficiency without unintended indel mutations at the desired target sites in human cell lines and mouse primary myoblasts. Furthermore, the proposed scheme had fewer off-target effects than conventional base editors at the DNA level. These results indicate that the suggested approach is promising for the development of more accurate and safer base editing techniques for use in clinical applications.

摘要

碱基编辑器是在基因组中进行精确单核苷酸突变的强大工具。然而,它们会在靶位点导致非预期的插入和缺失,这对临床应用来说是一个重大的限制。在这项研究中,我们旨在消除各种进化碱基编辑器在靶位点引起的不需要的插入缺失。为此,我们在碱基编辑器中应用了失活 Cas9 而非切口 Cas9,以诱导无插入缺失的精确替换。此外,我们还测试了在碱基编辑器中使用染色质调节肽来提高核苷酸转化效率。我们发现,在人类细胞系和小鼠原代成肌细胞中,使用失活 Cas9 和染色质调节肽的碱基编辑都可以提高核苷酸替换效率,而不会在所需靶位点产生非预期的插入缺失突变。此外,与传统碱基编辑器相比,该方案在 DNA 水平上的脱靶效应更少。这些结果表明,该方案有望为开发更精确和更安全的碱基编辑技术,应用于临床应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/74f1/10766602/45ae3c7796ac/12276_2023_1128_Fig1_HTML.jpg

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