为期一年的吗啉代反义寡核苷酸治疗可改善肌营养不良症 mdx 小鼠的骨骼肌和心肌功能。

One-year treatment of morpholino antisense oligomer improves skeletal and cardiac muscle functions in dystrophic mdx mice.

机构信息

McColl-Lockwood Laboratory for Muscular Dystrophy Research, Neuromuscular/ALS Center, Department of Neurology, Carolinas Medical Center, Charlotte, North Carolina 28231, USA. bo.wu@carolinashealthcare

出版信息

Mol Ther. 2011 Mar;19(3):576-83. doi: 10.1038/mt.2010.288. Epub 2010 Dec 21.

DOI:10.1038/mt.2010.288

PMID:21179007

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3048192/

Abstract

Antisense therapy has been successful to skip targeted dystrophin exon with correction of frameshift and nonsense mutations of Duchenne muscular dystrophy (DMD). Systemic production of truncated but functional dystrophin proteins has been achieved in animal models. Furthermore, phase I/II clinical trials in United Kingdom and the Netherlands have demonstrated dystrophin induction by local and systemic administrations of antisense oligomers. However, long-term efficacy and potential toxicity remain to be determined. The present study examined 1-year systemic effect of phosphorodiamidate morpholino oligomers (PMO) treatment targeting mutated dystrophin exon 23 in mdx mice. PMO induced dystrophin expression dose-dependently and significantly improved skeletal muscle pathology and function with reduced creatine kinase (CK) levels by a regimen of 60 mg/kg biweekly administration. This regimen induced <2% dystrophin expression in the heart, but improved cardiac functions demonstrated by hemodynamics analysis. The results suggest that low levels of dystrophin induction may be able to provide detectable benefit to cardiac muscle with limited myopathy. Body weight, serum enzyme tests, and histology analysis showed no sign of toxicity in the mice treated with up to 1.5 g/kg PMO for 6 months. These results indicate that PMO could be used safely as effective drugs for long-term systemic treatment of DMD.

摘要

反义疗法已成功跳过靶向肌营养不良蛋白外显子，纠正杜氏肌营养不良症（DMD）的移码和无义突变。在动物模型中已实现截断但具有功能的肌营养不良蛋白的全身产生。此外，英国和荷兰的 I/II 期临床试验表明，通过局部和全身给予反义寡核苷酸可诱导肌营养不良蛋白。然而，长期疗效和潜在毒性仍有待确定。本研究检查了针对 mdx 小鼠突变肌营养不良蛋白外显子 23 的磷酰胺酯吗啉寡聚物（PMO）治疗的 1 年系统效应。PMO 以剂量依赖性方式诱导肌营养不良蛋白表达，并通过每两周 60mg/kg 的方案显著改善骨骼肌病理学和功能，同时降低肌酸激酶（CK）水平。该方案诱导心脏中的肌营养不良蛋白表达<2%，但通过血液动力学分析显示心脏功能得到改善。结果表明，低水平的肌营养不良蛋白诱导可能能够为心肌提供可检测的益处，而肌病有限。在 6 个月内用高达 1.5g/kg PMO 治疗的小鼠中，体重、血清酶试验和组织学分析均未显示出毒性迹象。这些结果表明，PMO 可用作安全有效的药物，用于 DMD 的长期系统治疗。

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本文引用的文献

AAV-directed muscular dystrophy gene therapy.AAV 靶向肌肉营养不良基因治疗。

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