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DNA nanoparticle-mediated ABCA4 delivery rescues Stargardt dystrophy in mice
Zongchao Han, … , Mark J. Cooper, Muna I. Naash
Zongchao Han, … , Mark J. Cooper, Muna I. Naash
Published August 13, 2012
Citation Information: J Clin Invest. 2012;122(9):3221-3226. https://doi.org/10.1172/JCI64833.
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Brief Report Genetics

DNA nanoparticle-mediated ABCA4 delivery rescues Stargardt dystrophy in mice

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Abstract

Mutations in the photoreceptor-specific flippase ABCA4 are associated with Stargardt disease and many other forms of retinal degeneration that currently lack curative therapies. Gene replacement is a logical strategy for ABCA4-associated disease, particularly given the current success of traditional viral-mediated gene delivery, such as with adeno-associated viral (AAV) vectors. However, the large size of the ABCA4 cDNA (6.8 kbp) has hampered progress in the development of genetic treatments. Nonviral DNA nanoparticles (NPs) can accommodate large genes, unlike traditional viral vectors, which have capacity limitations. We utilized an optimized DNA NP technology to subretinally deliver ABCA4 to Abca4-deficient mice. We detected persistent ABCA4 transgene expression for up to 8 months after injection and found marked correction of functional and structural Stargardt phenotypes, such as improved recovery of dark adaptation and reduced lipofuscin granules. These data suggest that DNA NPs may be an excellent, clinically relevant gene delivery approach for genes too large for traditional viral vectors.

Authors

Zongchao Han, Shannon M. Conley, Rasha S. Makkia, Mark J. Cooper, Muna I. Naash

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Figure 2

NP-mediated ABCA4 gene delivery reduces retinal flecking in Abca4–/– mice.

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NP-mediated ABCA4 gene delivery reduces retinal flecking in Abca4–/– mic...
Shown are representative in vivo fundus images captured from treated Abca4–/– mice at 1 month PI (A) and 8 months PI (B). Age-matched WT and uninjected Abca4–/– mice were used as controls. White arrowheads show retinal flecking in uninjected and mutant-construct–injected animals but not WT or IRBP-ABCA4/MOP-ABCA4–treated animals.

Copyright © 2025 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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