首页> 外文期刊>Molecular therapy: the journal of the American Society of Gene Therapy >Negative-strand RNA viral vectors: intravenous application of sendai virus vectors for the systemic delivery of therapeutic genes.
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Negative-strand RNA viral vectors: intravenous application of sendai virus vectors for the systemic delivery of therapeutic genes.

机译:负链RNA病毒载体:仙台病毒载体的静脉内应用,用于治疗性基因的全身递送。

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Treatment by gene replacement is critical in the field of gene therapy. Suitable vectors for the delivery of therapeutic genes have to be generated and tested in preclinical settings. Recently, extraordinary features for a local gene delivery by Sendai virus vectors (SeVV) have been reported for different tissues. Here we show that direct intravenous application of SeVV in mice is not only feasible and safe, but it results in the secretion of therapeutic proteins to the circulation, for example, human clotting Factor IX (hFIX). In vitro characterization of first-generation SeVV demonstrated that secreted amounts of hFIX were at least comparable to published results for retroviral or adeno-associated viral vectors. Furthermore, as a consideration for application in humans, SeVV transduction led to efficient hFIX synthesis in primary human hepatocytes, and SeVV-encoded hFIX proteins could be shown to be functionally active in the human clotting cascade. In conclusion, our investigations demonstrate for the first time that intravenous administration of negative-strand RNA viral vectors may become a useful tool for the wide area of gene replacement requirements.
机译:基因替代治疗在基因治疗领域至关重要。用于递送治疗性基因的合适载体必须在临床前设置中产生和测试。近来,已经报道了仙台病毒载体(SeVV)递送局部基因对于不同组织的非凡特征。在这里,我们显示了在小鼠中直接静脉内应用SeVV不仅可行而且安全,而且还会导致治疗性蛋白质分泌到循环系统中,例如人凝血因子IX(hFIX)。第一代SeVV的体外表征表明,hFIX的分泌量至少与逆转录病毒或腺相关病毒载体的发表结果相当。此外,考虑到在人类中的应用,SeVV转导可在原代人肝细胞中有效地合成hFIX,并且显示SeVV编码的hFIX蛋白在人凝血级联反应中具有功能活性。总之,我们的研究首次证明,静脉内施用负链RNA病毒载体可能成为满足广泛的基因替代需求的有用工具。

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