Dystrophin- and Utrophin-Based Therapeutic Approaches for Treatment of Duchenne Muscular Dystrophy: A Comparative Review.

IF 5.4 2区 医学 Q1 IMMUNOLOGY BioDrugs Pub Date : 2024-01-01 Epub Date: 2023-11-02 DOI:10.1007/s40259-023-00632-3
Sylwia Szwec, Zuzanna Kapłucha, Jeffrey S Chamberlain, Patryk Konieczny
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Abstract

Duchenne muscular dystrophy is a devastating disease that leads to progressive muscle loss and premature death. While medical management focuses mostly on symptomatic treatment, decades of research have resulted in first therapeutics able to restore the affected reading frame of dystrophin transcripts or induce synthesis of a truncated dystrophin protein from a vector, with other strategies based on gene therapy and cell signaling in preclinical or clinical development. Nevertheless, recent reports show that potentially therapeutic dystrophins can be immunogenic in patients. This raises the question of whether a dystrophin paralog, utrophin, could be a more suitable therapeutic protein. Here, we compare dystrophin and utrophin amino acid sequences and structures, combining published data with our extended in silico analyses. We then discuss these results in the context of therapeutic approaches for Duchenne muscular dystrophy. Specifically, we focus on strategies based on delivery of micro-dystrophin and micro-utrophin genes with recombinant adeno-associated viral vectors, exon skipping of the mutated dystrophin pre-mRNAs, reading through termination codons with small molecules that mask premature stop codons, dystrophin gene repair by clustered regularly interspaced short palindromic repeats (CRISPR)/CRISPR-associated protein 9 (CRISPR/Cas9)-mediated genetic engineering, and increasing utrophin levels. Our analyses highlight the importance of various dystrophin and utrophin domains in Duchenne muscular dystrophy treatment, providing insights into designing novel therapeutic compounds with improved efficacy and decreased immunoreactivity. While the necessary actin and β-dystroglycan binding sites are present in both proteins, important functional distinctions can be identified in these domains and some other parts of truncated dystrophins might need redesigning due to their potentially immunogenic qualities. Alternatively, therapies based on utrophins might provide a safer and more effective approach.

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肌营养不良和肌营养不良的治疗Duchenne肌营养不良方法:比较综述。
杜兴肌营养不良是一种破坏性疾病,可导致进行性肌肉损失和过早死亡。虽然医学管理主要集中在症状治疗上,但几十年的研究已经产生了第一种能够恢复肌营养不良蛋白转录物受影响的阅读框架或诱导从载体合成截短的肌营养不良蛋白质的疗法,以及基于基因治疗和细胞信号在临床前或临床开发中的其他策略。然而,最近的报道表明,潜在的治疗性肌营养不良蛋白可能对患者具有免疫原性。这就提出了一个问题,即肌营养不良蛋白副产物utrophin是否是一种更合适的治疗蛋白。在这里,我们比较了肌营养不良蛋白和utrophin的氨基酸序列和结构,结合已发表的数据和我们的扩展计算机分析。然后,我们在Duchenne肌营养不良的治疗方法的背景下讨论这些结果。具体而言,我们专注于基于用重组腺相关病毒载体递送微量肌营养不良蛋白和微量utrophin基因的策略,突变的肌营养不良素前信使核糖核酸的外显子跳跃,用小分子读取终止密码子以掩盖过早终止密码子,通过聚集的规则间隔短回文重复序列(CRISPR)/CRISPR相关蛋白9(CRISPR/Cas9)介导的基因工程和增加utrophin水平来修复肌营养不良蛋白基因。我们的分析强调了各种肌营养不良蛋白和utrophin结构域在Duchenne肌营养不良治疗中的重要性,为设计具有提高疗效和降低免疫反应性的新型治疗化合物提供了见解。虽然两种蛋白质中都存在必要的肌动蛋白和β-肌营养不良聚糖结合位点,但在这些结构域中可以发现重要的功能差异,并且由于其潜在的免疫原性,截短的肌营养不良蛋白的一些其他部分可能需要重新设计。或者,基于utrophins的治疗可能会提供一种更安全、更有效的方法。
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
BioDrugs
BioDrugs 医学-免疫学
CiteScore
12.60
自引率
2.90%
发文量
50
审稿时长
>12 weeks
期刊介绍: An essential resource for R&D professionals and clinicians with an interest in biologic therapies. BioDrugs covers the development and therapeutic application of biotechnology-based pharmaceuticals and diagnostic products for the treatment of human disease. BioDrugs offers a range of additional enhanced features designed to increase the visibility, readership and educational value of the journal’s content. Each article is accompanied by a Key Points summary, giving a time-efficient overview of the content to a wide readership. Articles may be accompanied by plain language summaries to assist patients, caregivers and others in understanding important medical advances. The journal also provides the option to include various other types of enhanced features including slide sets, videos and animations. All enhanced features are peer reviewed to the same high standard as the article itself. Peer review is conducted using Editorial Manager®, supported by a database of international experts. This database is shared with other Adis journals.
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