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衣壳修饰的腺病毒载体用于改善肌肉定向基因治疗。

Capsid-modified adenoviral vectors for improved muscle-directed gene therapy.

机构信息

Department of Human and Molecular Genetics, Baylor College of Medicine, Houston, TX 77030, USA.

出版信息

Hum Gene Ther. 2012 Oct;23(10):1065-70. doi: 10.1089/hum.2012.003. Epub 2012 Aug 13.

DOI:10.1089/hum.2012.003
PMID:22888960
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3472516/
Abstract

Skeletal muscle represents an attractive target tissue for adenoviral gene therapy to treat muscle disorders and as a production platform for systemic expression of therapeutic proteins. However, adenovirus serotype 5 vectors do not efficiently transduce adult muscle tissue. Here we evaluated whether capsid modifications on adenoviral vectors could improve transduction in mature murine muscle tissue. First-generation and helper-dependent serotype 5 adenoviral vectors featuring the serotype 3 knob (5/3) showed significantly increased transduction of skeletal muscle after intramuscular injection in adult mice. Furthermore, we showed that full-length dystrophin could be more efficiently transferred to muscles of mdx mice using a 5/3-modified helper-dependent adenoviral vector. In contrast to first-generation vectors, helper-dependent adenoviral vectors mediated stable marker gene expression for at least 1 year after intramuscular injection. In conclusion, 5/3 capsid-modified helper-dependent adenoviral vectors show enhanced transduction in adult murine muscle tissue and mediate long-term gene expression, suggesting the suitability of these vectors for muscle-directed gene therapy.

摘要

骨骼肌是腺病毒基因治疗的理想靶组织,可以用于治疗肌肉疾病,并作为全身表达治疗性蛋白的生产平台。然而,腺病毒血清型 5 载体不能有效地转导成年肌肉组织。在这里,我们评估了腺病毒载体的衣壳修饰是否可以提高成熟肌肉组织的转导效率。第一代和辅助依赖性血清型 5 腺病毒载体具有血清型 3 knob(5/3),在成年小鼠肌肉内注射后,骨骼肌的转导效率显著提高。此外,我们表明,使用 5/3 修饰的辅助依赖性腺病毒载体,可以更有效地将全长肌营养不良蛋白转移到 mdx 小鼠的肌肉中。与第一代载体相比,辅助依赖性腺病毒载体介导的标记基因表达至少在肌肉内注射后 1 年内稳定。总之,5/3 衣壳修饰的辅助依赖性腺病毒载体在成年小鼠肌肉组织中显示出增强的转导效率,并介导长期基因表达,表明这些载体适合肌肉定向基因治疗。

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