[HTML][HTML] Safety of recombinant adeno-associated virus type 2–RPE65 vector delivered by ocular subretinal injection

SG Jacobson, GM Acland, GD Aguirre, TS Aleman… - Molecular Therapy, 2006 - cell.com
SG Jacobson, GM Acland, GD Aguirre, TS Aleman, SB Schwartz, AV Cideciyan, CJ Zeiss…
Molecular Therapy, 2006cell.com
AAV2 delivery of the RPE65 gene to the retina of blind RPE65-deficient animals restores
vision. This strategy is being considered for human trials in RPE65-associated Leber
congenital amaurosis (LCA), but toxicity and dose efficacy have not been defined. We
studied ocular delivery of AAV-2/2. RPE65 in RPE65-mutant dogs. There was no systemic
toxicity. Ocular examinations showed mild or moderate inflammation that resolved over 3
months. Retinal histopathology indicated that traumatic lesions from the injection were …
Abstract
AAV2 delivery of the RPE65 gene to the retina of blind RPE65-deficient animals restores vision. This strategy is being considered for human trials in RPE65-associated Leber congenital amaurosis (LCA), but toxicity and dose efficacy have not been defined. We studied ocular delivery of AAV-2/2.RPE65 in RPE65-mutant dogs. There was no systemic toxicity. Ocular examinations showed mild or moderate inflammation that resolved over 3 months. Retinal histopathology indicated that traumatic lesions from the injection were common, but thinning within the injection region occurred only at the two highest vector doses. Biodistribution studies at 3 months postinjection showed no vector in optic nerve or visual centers in the brain and only isolated non-dose-related detection in other organs. We also performed biodistribution studies in normal rats at about 2 weeks and 2 months postinjection and vector was not widespread outside the injected eye. Dose–response results in RPE65-mutant dogs indicated that the highest 1.5-log unit range of vector doses proved efficacious. The efficacy and toxicity limits defined in this study lead to suggestions for the design of a subretinal AAV-2/2.RPE65 human trial of RPE65-associated LCA.
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