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首页> 外文期刊>Neuromuscular disorders: NMD >In vivo delivery of naked antisense oligos in aged mdx mice: analysis of dystrophin restoration in skeletal and cardiac muscle.
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In vivo delivery of naked antisense oligos in aged mdx mice: analysis of dystrophin restoration in skeletal and cardiac muscle.

机译:裸露的反义寡核苷酸在衰老的mdx小鼠中的体内递送:骨骼肌和心肌中肌营养不良蛋白恢复的分析。

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Antisense-mediated exon skipping holds great potential for the treatment of DMD. In mdx mice, functional recovery of skeletal muscle has been obtained upon systemic delivery of "naked" oligonucleotides or viral vectors encoding for antisense snRNAs. However, amongst the studies reported so far, which used either neonatal or young adult animals--only one achieved dystrophin restoration in cardiac muscle, using an adeno-associated vector. Here we report the in vivo delivery of morpholino oligos in aged mdx mice, both in skeletal muscle, via intra-arterial injection, and in cardiac muscle, via intra-muscular injection. Localized intra-arterial delivery yielded high levels of dystrophin restoration and just two doses of 100 microg each resulted into detectable force recovery in the EDL muscles of treated limbs. On the other hand, upon intra-cardiac injections in the left ventricle wall the skipping effect was much lower than what obtained in tibialis anterior muscles injected with comparable amounts of oligos. This latter finding suggests that even upon direct delivery antisense-mediated dystrophin restoration in cardiac muscle might suffer from limitations that do not exist in skeletal muscle.
机译:反义介导的外显子跳跃在DMD的治疗中具有巨大的潜力。在mdx小鼠中,通过全身递送“裸”寡核苷酸或编码反义snRNA的病毒载体,可以恢复骨骼肌的功能。但是,到目前为止,在报道的研究中,无论是使用新生的还是成年的成年动物,只有一个通过使用腺相关的载体实现了肌营养不良蛋白的恢复。在这里,我们报告了在老年mdx小鼠体内体内吗啉代寡核苷酸的体内递送,无论是通过动脉内注射在骨骼肌中,还是通过肌肉内注射在心肌中。局部动脉内递送可产生高水平的肌营养不良蛋白恢复,而仅两剂100微克的剂量可在治疗四肢的EDL肌肉中产生可检测到的力恢复。另一方面,在左心室壁内进行心脏内注射时,其跳跃作用远低于注射了相当数量的寡核苷酸的胫骨前肌所获得的跳跃作用。后一个发现表明,即使直接递送,心肌中反义介导的肌营养不良蛋白的恢复也可能遭受骨骼肌中不存在的限制。

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