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基于CRISPR技术在原代人B细胞和淋巴瘤细胞系中进行基因敲入的策略。

Strategies for CRISPR-based knock-ins in primary human B cells and lymphoma cell lines.

作者信息

Lund Sophie, Gong Chun, Yu Xin, Staudt Louis M, Hodson Daniel J, Scheich Sebastian

机构信息

Goethe University Frankfurt, University Hospital, Frankfurt am Main, Germany.

University Cancer Center (UCT) Frankfurt, University Hospital, Goethe University, Frankfurt am Main, Germany.

出版信息

Front Immunol. 2025 May 16;16:1589729. doi: 10.3389/fimmu.2025.1589729. eCollection 2025.

Abstract

Since its advent about ten years ago, the CRISPR-Cas9 system has been frequently used in biomedical applications. It has advanced various fields, and CRISPR-Cas9-based therapeutics have shown promising results in the treatment of specific hematological diseases. Furthermore, CRISPR gene editing technologies have revolutionized cancer research by enabling a broad range of genetic perturbations, including genetic knockouts and precise single nucleotide changes. This perspective focuses on the state-of-the-art methodology of CRISPR knock-ins to engineer immune cells. Since this technique relies on homology-directed repair (HDR) of double-strand breaks (DSBs) induced by the Cas9 enzyme, it can be used to introduce specific mutations into the target genome. Therefore, this methodology offers a valuable opportunity to functionally study specific mutations and to uncover their impacts not only on overall cell functions but also on the mechanisms behind cancer-related alterations in common signaling pathways. This article highlights CRISPR knock-in strategies, protocols, and applications in cancer and immune research, with a focus on diffuse large B cell lymphoma.

摘要

大约十年前CRISPR-Cas9系统问世以来,它在生物医学应用中得到了频繁使用。它推动了各个领域的发展,基于CRISPR-Cas9的疗法在治疗特定血液疾病方面已显示出有前景的结果。此外,CRISPR基因编辑技术通过实现广泛的基因扰动,包括基因敲除和精确的单核苷酸变化,彻底改变了癌症研究。这篇综述聚焦于用于改造免疫细胞的CRISPR基因敲入的最新方法。由于该技术依赖于Cas9酶诱导的双链断裂(DSB)的同源定向修复(HDR),它可用于将特定突变引入目标基因组。因此,这种方法为功能研究特定突变以及揭示它们不仅对整体细胞功能而且对常见信号通路中癌症相关改变背后的机制的影响提供了宝贵机会。本文重点介绍CRISPR基因敲入策略、方案及其在癌症和免疫研究中的应用,尤其关注弥漫性大B细胞淋巴瘤。

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