Publications by authors named "Jade J Samulski"
Vector capsid dose-dependent inflammation of transduced liver has limited the ability of adeno-associated virus (AAV) factor IX (FIX) gene therapy vectors to reliably convert severe to mild hemophilia B in human clinical trials. These trials also identified the need to understand AAV neutralizing antibodies and empty AAV capsids regarding their impact on clinical success. To address these safety concerns, we have used a scalable manufacturing process to produce GMP-grade AAV8 expressing the FIXR338L gain-of-function variant with minimal (<10%) empty capsid and have performed comprehensive dose-response, biodistribution, and safety evaluations in clinically relevant hemophilia models.
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- Efficient gene transfer is crucial for treating Duchenne muscular dystrophy (DMD), and the first clinical trial used a new chimeric adeno-associated virus (AAV) capsid variant called AAV2.5, which enhances muscle targeting while minimizing immune response.
- This phase I trial involved injecting AAV2.5 into the bicep of boys with DMD and comparing results to saline control injections, with some patients receiving an empty AAV capsid to differentiate immune responses.
- Results showed that AAV2.5 was safe, well tolerated, and effectively delivered genes, paving the way for customized AAV vectors to improve gene therapy approaches for DMD and potentially other conditions.