| Literature DB >> 22828499 |
Nicola Brunetti-Pierri1, Aimee Liou, Priti Patel, Donna Palmer, Nathan Grove, Milton Finegold, Pasquale Piccolo, Elizabeth Donnachie, Karen Rice, Arthur Beaudet, Charles Mullins, Philip Ng.
Abstract
Hemophilia B is an excellent candidate for gene therapy because low levels of factor IX (FIX) (≥1%) result in clinically significant improvement of the bleeding diathesis. Helper-dependent adenoviral (HDAd) vectors can mediate long-term transgene expression without chronic toxicity. To determine the potential for HDAd-mediated liver-directed hemophilia B gene therapy, we administered an HDAd expressing hFIX into rhesus macaques through a novel and minimally invasive balloon occlusion catheter-based method that permits preferential, high-efficiency hepatocyte transduction with low, subtoxic vector doses. Animals given 1 × 10(12) and 1 × 10(11) virus particle (vp)/kg achieved therapeutic hFIX levels for the entire observation period (up to 1,029 days). At 3 × 10(10) and 1 × 10(10) vp/kg, only subtherapeutic hFIX levels were achieved which were not sustained long-term. Balloon occlusion administration of HDAd was well tolerated with negligible toxicity. Five of six animals developed inhibitors to hFIX. These results provide important information in assessing the clinical utility of HDAd for hemophilia B gene therapy.Entities:
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Year: 2012 PMID: 22828499 PMCID: PMC3464633 DOI: 10.1038/mt.2012.143
Source DB: PubMed Journal: Mol Ther ISSN: 1525-0016 Impact factor: 11.454