Identification of selective and non-selective C9ORF72 targeting in vivo active siRNAs

IF 6.5 2区医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL

Molecular Therapy. Nucleic Acids Pub Date : 2024-07-31 DOI:10.1016/j.omtn.2024.102291

James W. Gilbert, Zachary Kennedy, Bruno Godinho, Ashley Summers, Alexandra Weiss, Dimas Echeverria, Brianna Bramato, Nicholas McHugh, David Cooper, Ken Yamada, Matthew Hassler, Hélène Tran, Fen Biao Gao, Robert H. Brown Jr., Anastasia Khvorova

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引用次数: 0

Abstract

A hexanucleotide (GC) repeat expansion (HRE) within intron one of is the leading genetic cause of amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD). haploinsufficiency, formation of RNA foci, and production of dipeptide repeat (DPR) proteins have been proposed as mechanisms of disease. Here, we report the first example of disease-modifying siRNAs for driven ALS/FTD. Using a combination of reporter assay and primary cortical neurons derived from a C9-ALS/FTD mouse model, we screened a panel of more than 150 fully chemically stabilized siRNAs targeting different transcriptional variants. We demonstrate the lack of correlation between siRNA efficacy in reporter assay versus native environment; repeat-containing mRNA variants are found to preferentially localize to the nucleus, and thus mRNA accessibility and intracellular localization have a dominant impact on functional RNAi. Using a C9-ALS/FTD mouse model, we demonstrate that divalent siRNAs targeting mRNA variants specifically or non-selectively reduce the expression of mRNA and significantly reduce DPR proteins. Interestingly, siRNA silencing all mRNA transcripts was more effective in removing intranuclear mRNA aggregates than targeting only HRE-containing mRNA transcripts. Combined, these data support RNAi-based degradation of as a potential therapeutic paradigm.

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鉴定选择性和非选择性 C9ORF72 靶向体内活性 siRNA

肌萎缩性脊髓侧索硬化症（ALS）和额颞叶痴呆症（FTD）的主要遗传病因是肌萎缩性脊髓侧索硬化症（ALS）和额颞叶痴呆症（FTD）内含子一的六核苷酸（GC）重复扩增（HRE）。在此，我们首次报道了用于驱动 ALS/FTD 的可改变疾病的 siRNA。我们结合使用报告分析法和从 C9-ALS/FTD 小鼠模型中提取的原发性皮层神经元，筛选出了 150 多种针对不同转录变体的完全化学稳定 siRNA。我们证明了 siRNA 在报告检测中的功效与原生环境之间缺乏相关性；含重复的 mRNA 变体被发现优先定位于细胞核，因此 mRNA 的可及性和细胞内定位对功能性 RNAi 有主要影响。我们利用 C9-ALS/FTD 小鼠模型证明，针对 mRNA 变异的二价 siRNA 可特异性或非选择性地降低 mRNA 的表达，并显著减少 DPR 蛋白。有趣的是，与只针对含 HRE 的 mRNA 转录本相比，沉默所有 mRNA 转录本的 siRNA 能更有效地清除核内 mRNA 聚集。综合来看，这些数据支持将基于 RNAi 的降解作为一种潜在的治疗范式。

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

Molecular Therapy. Nucleic Acids MEDICINE, RESEARCH & EXPERIMENTAL-

CiteScore

15.40

自引率

1.10%

发文量

336

审稿时长

20 weeks

期刊介绍： Molecular Therapy Nucleic Acids is an international, open-access journal that publishes high-quality research in nucleic-acid-based therapeutics to treat and correct genetic and acquired diseases. It is the official journal of the American Society of Gene & Cell Therapy and is built upon the success of Molecular Therapy. The journal focuses on gene- and oligonucleotide-based therapies and publishes peer-reviewed research, reviews, and commentaries. Its impact factor for 2022 is 8.8. The subject areas covered include the development of therapeutics based on nucleic acids and their derivatives, vector development for RNA-based therapeutics delivery, utilization of gene-modifying agents like Zn finger nucleases and triplex-forming oligonucleotides, pre-clinical target validation, safety and efficacy studies, and clinical trials.