current challenges and future directions in recombinant aav-mediated gene therapy of duchenne muscular dystrophy

current challenges and future directions in recombinant aav-mediated gene therapy of duchenne muscular dystrophy

;Shin'ichi Takeda;Takashi Okada
journal of cerebral blood flow and metabolism 2013 Vol. 6 pp. 813-836
248
takeda2013pharmaceuticalscurrent

Abstract

Various characteristics of adeno-associated virus (AAV)-based vectors with long-term safe expression have made it an exciting transduction tool for clinical gene therapy of Duchenne muscular dystrophy (DMD). Although host immune reactions against the vector as well as transgene products were detected in some instances of the clinical studies, there have been promising observations. Methods of producing AAV vectors for considerable in vivo experimentation and clinical investigations have been developed and a number of studies with AAV vector-mediated muscle transduction were attempted. Notably, an intravenous limb perfusion transduction technique enables extensive transgene expression in the skeletal muscles without noticeable adverse events. Furthermore, cardiac transduction by the rAAV9-microdystrophin would be promising to prevent development of cardiac dysfunction. Recent achievements in transduction technology suggest that long-term transgene expression with therapeutic benefits in DMD treatment would be achieved by the rAAV-mediated transduction strategy with an adequate regimen to regulate host immune response.

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