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Transgene Expression in Dogs After Liver-Directed Hydrodynamic Delivery of Sleeping Beauty Transposons Using Balloon Catheters

机译:犬用球囊导管定向输注睡眠美容转座子的水动力后在狗中转基因表达。

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摘要

The Sleeping Beauty transposon system has been extensively tested for integration of reporter and therapeutic genes in vitro and in vivo in mice. Dogs were used as a large animal model for human therapy and minimally invasive infusion of DNA solutions. DNA solutions were delivered into the entire liver or the left side of the liver using balloon catheters for temporary occlusion of venous outflow. A peak intravascular pressure between 80 and 140 mmHg supported sufficient DNA delivery in dog liver for detection of secretable reporter proteins. Secretable reporters allowed monitoring of the time course of gene products detectable in the circulation postinfusion. Canine secreted alkaline phosphatase reporter protein levels were measured in plasma, with expression detectable for up to 6 weeks, while expression of canine erythropoietin was detectable for 7–10 days. All animals exhibited a transient increase in blood transaminases that normalized within 10 days; otherwise the treated animals were clinically normal. These results demonstrate the utility of a secreted reporter protein for real-time monitoring of gene expression in the liver in a large animal model but highlight the need for improved delivery in target tissues to support integration and long-term expression of Sleeping Beauty transposons.
机译:睡美人转座子系统已在小鼠体内和体外进行了报道基因和治疗基因整合的广泛测试。狗被用作人类治疗和DNA溶液微创输注的大型动物模型。使用气囊导管将DNA溶液输送到整个肝脏或肝脏的左侧,以暂时阻塞静脉流出。在80至140mmHg之间的峰值血管内压力支持在犬肝中足够的DNA递送以检测可分泌的报道蛋白。秘密记者允许监测输注后循环中可检测到的基因产物的时间进程。测定血浆中犬分泌的碱性磷酸酶报告蛋白的水平,可检测长达6周的表达,而检测犬促红细胞生成素的表达可检测7-10天。所有动物在10天内恢复正常的血液转氨酶瞬时增加;否则治疗的动物在临床上是正常的。这些结果证明了分泌的报道蛋白在大型动物模型中实时监测肝脏中基因表达的实用性,但强调需要改善靶组织中的传递以支持Sleeping Beauty转座子的整合和长期表达。

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