Abstract
BackgroundGene transfer into the amniotic fluid using recombinant adenovirus vectors was shown previously to result in high efficiency transfer of transgenes into the lungs and intestines. Adenovirus mediated in utero gene therapy, however, resulted in expression of the transgene for less than 30 days. Recombinant adenovirus associated viruses (rAAV) have the advantage of maintaining the viral genome in daughter cells thus providing for long-term expression of transgenes.MethodsRecombinant AAV2 carrying green fluorescent protein (GFP) was introduced into the amniotic sac of fetal rodents and nonhuman primates. Transgene maintenance and expression was monitor.ResultsGene transfer resulted in rapid uptake and long-term gene expression in mice, rats, and non-human primates. Expression and secretion of the reporter gene, GFP, was readily demonstrated within 72 hours post-therapy. In long-term studies in rats and nonhuman primates, maintenance of GFP DNA, protein expression, and reporter gene secretion was documented for over one year.ConclusionsBecause only multipotential stem cells are present at the time of therapy, these data demonstrated that in utero gene transfer with AAV2 into stem cells resulted in long-term systemic expression of active transgene roducts. Thus, in utero gene transfer via the amniotic fluid may be useful in treatment of gene disorders.
Highlights
Gene transfer into the amniotic fluid using recombinant adenovirus vectors was shown previously to result in high efficiency transfer of transgenes into the lungs and intestines
BMC Biotechnology 2003, 3 http://www.biomedcentral.com/1472-6750/3/16. This laboratory has shown that in utero gene transfer via amniotic fluid is an effective method for introducing genes into epithelial multipotential stem cells of the lung and intestines [3,4,5,6,7,8]
Non-human primate studies The in utero uptake of the rAAV2 in the mouse suggests that this vector could be effective, for the reversal of metabolic defects. For this gene therapy to be effective it must translate well from rodents to humans and it must persist over extended periods of time. To test both these parameters a Rhesus macaque was infected with rAAV2-green fluorescent protein (GFP) at 100 days' gestation, allowed to deliver, and tissues examined for GFP expression at 15 months of age (16 months post-infection)
Summary
In utero recombinant adeno-associated virus gene transfer in mice, rats, and primates. Address: 1Ochsner Children's Research Institute, Ochsner Clinic Foundation, New Orleans, LA, USA, 70121 and 2Departments of Medicine, Genetics, and Biochemistry, Louisiana State University Health Sciences Center, New Orleans, LA, 70112, USA
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