Lack of immunotoxicity after regional intravenous (RI) delivery of rAAV to nonhuman primate skeletal muscle.

将 rAAV 进行区域静脉注射 (RI) 到非人灵长类动物骨骼肌后未观察到免疫毒性

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作者:Toromanoff Alice, Adjali Oumeya, Larcher Thibaut, Hill Marcelo, Guigand Lydie, Chenuaud Pierre, Deschamps Jack-Yves, Gauthier Olivier, Blancho Gilles, Vanhove Bernard, Rolling Fabienne, Chérel Yan, Moullier Philippe, Anegon Ignacio, Le Guiner Caroline
In the absence of an immune response from the host, intramuscular (IM) injection of recombinant adeno-associated virus (rAAV) results in the permanent expression of the transgene from mouse to primate models. However, recent gene transfer studies into animal models and humans indicate that the risk of transgene and/or capsid-specific immune responses occurs and depends on multiple factors. Among these factors, the route of delivery is important, although poorly addressed in large animal models. Here, we compare the IM and the drug-free regional intravenous (RI) deliveries of rAAV in nonhuman primate (NHP) skeletal muscle monitoring the host immune response toward the transgene. We show that IM is consistently associated with immunotoxicity and the destruction of the genetically modified myofibers, whereas RI allows the stable expression of the transgene. This has important implications for the design of clinical trials for gene transfer in skeletal muscle.

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