AAV-PHP.eB transduces both the inner and outer retina with high efficacy in mice

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2022Access:
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Palfi, A. and Chadderton, N. and Millington-Ward, S. and Post, I. and Humphries, P. and Kenna, P.F. and Farrar, G.J., AAV-PHP.eB transduces both the inner and outer retina with high efficacy in mice, Molecular Therapy - Methods and Clinical Development, 25, 2022, 236-249Download Item:
Abstract:
Recombinant adeno-associated virus (AAV) vectors are one of
the main gene delivery vehicles used in retinal gene therapy ap proaches; however, there is a need to further improve the effi cacy, tropism, and safety of these vectors. In this study, using
a CMV-EGFP expression cassette, we characterize the retinal
utility of AAV-PHP.eB, a serotype recently developed by in vivo
directed evolution, which can cross the blood-brain barrier and
target neurons with high efficacy in mice. Systemic and intravi treal delivery of AAV-PHP.eB resulted in the high transduction
efficacy of retinal ganglion and horizontal cells, with systemic
delivery providing pan-retinal coverage of the mouse retina.
Subretinal delivery transduced photoreceptors and retinal
pigment epithelium cells robustly. EGFP expression (number
of transduced cells and mRNA levels) were similar when the
retinas were transduced systemically or intravitreally with
AAV-PHP.eB or intravitreally with AAV2/2. Notably, in pho toreceptors, EGFP fluorescence intensities and mRNA levels
were 50–70 times higher, when subretinal injections with
AAV-PHP.eB were compared to AAV2/8. Our results demon strate the pan-retinal transduction of ganglion cells and
extremely efficient transduction of photoreceptor and retinal
pigment epithelium cells as the most valuable features of
AAV-PHP.eB in the mouse retina.
Author's Homepage:
http://people.tcd.ie/phumphrshttp://people.tcd.ie/gjfarrar
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Author: Humphries, Peter; Farrar, Gwyneth
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Series/Report no:
Molecular Therapy - Methods and Clinical Development25
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mouse retina, adeno-associated virus (AAV), gene delivery vehicles, AAV-PHP.eB, AAV2/2, AAV2/8, EGFP, Eye, Gene therapy, Mouse, Retina, Retinal degenerationDOI:
http://dx.doi.org/10.1016/j.omtm.2022.03.016Metadata
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