ELX-02 Suppresses nonsense mutations and restores type VII collagen and laminin 332 function in recessive dystrophic and junctional epidermolysis bullosa

IF 6.5 2区医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL

Molecular Therapy. Nucleic Acids Pub Date : 2024-09-10 DOI:10.1016/j.omtn.2024.102334

Brandon Levian, Yingping Hou, Xin Tang, Liat Bainvoll, Kate Zheng, Vasu Badarinarayana, Soheil Aghamohammadzadeh, Mei Chen

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引用次数: 0

Abstract

Recessive dystrophic epidermolysis bullosa (RDEB) and junctional epidermolysis bullosa (JEB) are lethal blistering skin disorders resulting from mutations in genes coding for type VII collagen (COL7A1) and laminin 332 (LAMA3, LAMB3, or LAMC2), respectively. In RDEB, 25% of patients harbor nonsense mutations causing premature termination codons (PTCs). In JEB, a majority of mutations in LAMB3 are nonsense mutations (80%). ELX-02, an aminoglycoside analog, has demonstrated superior PTC readthrough activity and lower toxicity compared to gentamicin in various genetic disorders. This study investigated the ability of ELX-02 to suppress PTCs and promote the expression of C7 and laminin 332 in primary RDEB keratinocytes/fibroblasts and primary JEB keratinocytes harboring nonsense mutations. ELX-02 induced a dose-dependent production of C7 or laminin β3 that surpassed the results achieved with gentamicin. ELX-02 reversed RDEB and JEB cellular hypermotility and improved poor cell-substratum adhesion in JEB cells. Importantly, ELX-02-induced C7 and laminin 332 localized to the dermal-epidermal junction. This is the first study demonstrating that ELX-02 can induce PTC readthrough and restore functional C7 and laminin 332 in RDEB and JEB caused by nonsense mutations. Therefore, ELX-02 may offer a novel and safe therapy for RDEB, JEB, and other inherited skin diseases caused by nonsense mutations.

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ELX-02 抑制无义突变，恢复隐性萎缩性和交界性表皮松解症中 VII 型胶原蛋白和层粘连蛋白 332 的功能

隐性萎缩性表皮松解症（RDEB）和交界性表皮松解症（JEB）是致命的大疱性皮肤病，分别由编码 VII 型胶原蛋白（COL7A1）和层粘连蛋白 332（LAMA3、LAMB3 或 LAMC2）的基因突变引起。在 RDEB 中，25% 的患者存在无义突变，导致过早终止密码子（PTC）。在 JEB 中，LAMB3 的大多数突变是无义突变（80%）。ELX-02是一种氨基糖苷类似物，与庆大霉素相比，ELX-02在各种遗传疾病中表现出更优越的PTC读通活性和更低的毒性。本研究调查了ELX-02在原代RDEB角朊细胞/成纤维细胞和携带无义突变的原代JEB角朊细胞中抑制PTC和促进C7和层粘连蛋白332表达的能力。ELX-02 可诱导 C7 或层粘连蛋白 β3 的产生，其剂量依赖性超过庆大霉素。ELX-02逆转了RDEB和JEB细胞的过度运动性，并改善了JEB细胞中细胞与基底粘附性差的问题。重要的是，ELX-02 诱导的 C7 和层粘连蛋白 332 定位于真皮-表皮交界处。这是第一项证明ELX-02能诱导PTC读通并恢复由无义突变引起的RDEB和JEB中C7和层粘连蛋白332功能的研究。因此，ELX-02可能为无义突变引起的RDEB、JEB和其他遗传性皮肤病提供一种新颖、安全的疗法。

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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.