Comprehensive review of adverse reactions and toxicology in ASO-based therapies for Duchenne Muscular Dystrophy: From FDA-approved drugs to peptide-conjugated ASO

IF 2.9 Q2 TOXICOLOGY
Umme Sabrina Haque , Melissa Kohut , Toshifumi Yokota
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Abstract

Duchenne Muscular Dystrophy (DMD) is a devastating X-linked genetic disorder characterized by progressive muscle degeneration due to mutations in the dystrophin gene. This results in the absence or dysfunction of the dystrophin protein, leading to muscle weakness, loss of ambulation, respiratory issues, and cardiac complications, often leading to premature death. Recently, antisense oligonucleotide (ASO)-mediated exon skipping has emerged as a promising therapeutic strategy for DMD. Notably, the FDA has conditionally approved four ASO therapies for DMD, with numerous others in various stages of clinical development, indicating the growing interest and potential in this field. To enhance ASO-based therapies, researchers have explored the novel concept of conjugating peptides to the phosphorodiamidate morpholino backbone (PMO) of ASOs, leading to the development of peptide-conjugated PMOs (PPMOs). These PPMOs have demonstrated significantly improved pharmacokinetic profiles, potentially augmenting their therapeutic effectiveness. Despite the optimism surrounding ASOs and PPMOs, concerns persist regarding their efficacy and safety. To comprehensively evaluate these therapies, it is imperative to expand patient populations in clinical trials and conduct thorough investigations into the associated risks. This article provides a comprehensive review and discussion of the available data pertaining to adverse reactions and toxicology associated with FDA-approved ASO drugs for DMD. Furthermore, it offers insights into the emerging category of peptide-conjugated ASO drugs those are clinical and preclinical trials, shedding light on their potential benefits and challenges.

Abstract Image

全面回顾基于 ASO 的杜氏肌肉萎缩症疗法的不良反应和毒理学:从美国食品和药物管理局批准的药物到多肽共轭ASO
杜兴氏肌肉萎缩症(DMD)是一种毁灭性的 X 连锁遗传疾病,其特征是由于肌营养不良蛋白基因突变导致的进行性肌肉退化。这种疾病会导致肌营养不良蛋白缺失或功能障碍,从而导致肌肉无力、无法行走、呼吸困难和心脏并发症,通常会导致患者过早死亡。最近,反义寡核苷酸(ASO)介导的外显子跳越已成为一种治疗 DMD 的有前途的策略。值得注意的是,美国食品和药物管理局已经有条件地批准了四种治疗 DMD 的 ASO 疗法,还有许多其他疗法正处于不同的临床开发阶段,这表明人们对这一领域的兴趣和潜力日益增长。为了增强基于 ASO 的疗法,研究人员探索了将多肽与 ASO 的磷酰二胺吗啉基骨架(PMO)共轭的新概念,从而开发出多肽共轭 PMOs(PPMOs)。这些 PPMOs 的药代动力学特征得到了显著改善,有可能增强其治疗效果。尽管人们对 ASOs 和 PPMOs 持乐观态度,但对其疗效和安全性的担忧依然存在。为了全面评估这些疗法,必须扩大临床试验的患者群体,并对相关风险进行彻底调查。本文全面回顾和讨论了与 FDA 批准的用于治疗 DMD 的 ASO 药物相关的不良反应和毒理学方面的现有数据。此外,文章还深入探讨了正在进行临床和临床前试验的多肽共轭ASO药物这一新兴类别,揭示了其潜在的益处和挑战。
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
Current Research in Toxicology
Current Research in Toxicology Environmental Science-Health, Toxicology and Mutagenesis
CiteScore
4.70
自引率
3.00%
发文量
33
审稿时长
82 days
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