通过 CRISPR/Cas 精确碱基编辑技术靶向胶质瘤中的 IDH1 R132H 突变。

IF 3.7 Q1 CLINICAL NEUROLOGY

Neuro-oncology advances Pub Date : 2024-11-02 eCollection Date: 2024-01-01 DOI:10.1093/noajnl/vdae182

Remi Weber, Flavio Vasella, Artsiom Klimko, Manuela Silginer, Martine Lamfers, Marian Christoph Neidert, Luca Regli, Gerald Schwank, Michael Weller

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引用次数: 0

摘要

背景：胶质瘤是最常见的恶性原发性脑肿瘤，但缺乏根治性治疗方法。了解胶质瘤特异性分子改变对开发新型疗法至关重要。其中，异柠檬酸脱氢酶 1 基因突变（IDH1 R132H）尽管发生早且表达广泛，但其生物学后果仍无定论：因此，我们采用了CRISPR/Cas腺嘌呤碱基编辑器来校正IDH1 R132H基因突变：结果：在原发性患者衍生细胞模型中成功纠正了IDH1 R132H突变，从而降低了IDH1 R132H蛋白水平，减少了2-羟基戊二酸的产生，但却增加了增殖。利用双腺相关病毒分裂内含子系统成功地在体外和体内传递了基础编辑物：综上所述，我们的研究为针对 IDH1 R132H 突变的精确基因干预提供了一种策略，从而可以开发精确的模型来研究其对胶质瘤生物学的影响，并作为体内基因治疗的框架。

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Targeting the IDH1 ^R132H mutation in gliomas by CRISPR/Cas precision base editing.

Background: Gliomas, the most frequent malignant primary brain tumors, lack curative treatments. Understanding glioma-specific molecular alterations is crucial to develop novel therapies. Among them, the biological consequences of the isocitrate dehydrogenase 1 gene mutation (IDH1 ^R132H) remain inconclusive despite its early occurrence and widespread expression.

Methods: We thus employed CRISPR/Cas adenine base editors, which allow precise base pair alterations with minimal undesirable effects, to correct the IDH1 ^R132H mutation.

Results: Successful correction of the IDH1 ^R132H mutation in primary patient-derived cell models led to reduced IDH1 ^R132H protein levels and decreased production of 2-hydroxyglutarate, but increased proliferation. A dual adeno-associated virus split intein system was used to successfully deliver the base editor in vitro and in vivo.

Conclusions: Taken together, our study provides a strategy for a precise genetic intervention to target the IDH1 ^R132H mutation, enabling the development of accurate models to study its impact on glioma biology and serving as a framework for an in vivo gene therapy.

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来源期刊

Neuro-oncology advances

CiteScore

6.20

自引率

0.00%

发文量

审稿时长

12 weeks