4.4 Article

AAV8BP2 and AAV8 transduce the mammalian cochlear lateral wall and endolymphatic sac with high efficiency

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出版社

CELL PRESS
DOI: 10.1016/j.omtm.2022.07.013

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资金

  1. NIDCD Division of Intramural Research grant [DC000082-02, DC000060, DC000080]
  2. Foundation Fighting Blindness - CHOP -Penn Pediatric Center for Retinal Degenerations
  3. CHOP -Penn Pediatric Center for Retinal Degenerations
  4. Research to Prevent Blindness
  5. Paul and Evanina Mackall Foundation Trust
  6. F.M. Kirby Foundation
  7. National Eye Institute/NIH [R21EY020662, 8DP1EY023177]

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Inner ear gene therapy using AAVs has been successfully applied in mouse models, improving auditory function. This study identifies AAV8BP2 and AAV8 as highly efficient vectors for transducing cells in the cochlear lateral wall and the endolymphatic sac.
Inner ear gene therapy using adeno-associated viruses (AAVs) has been successfully applied to several mouse models of hereditary hearing loss to improve their auditory function. While most inner ear gene therapy studies have focused on the mechanosensory hair cells and supporting cells in the organ of Corti, the cochlear lateral wall and the endolymphatic sac have not garnered much attention. The cochlear lateral wall and the endolymphatic sac play critical roles in inner ear ionic and fluid homeostasis. Mutations in genes expressed in the cochlear lateral wall and the endolymphatic sac are present in a large percentage of patients with hereditary hearing loss. In this study, we examine the transduction patterns and effi- ciencies of conventional (AAV2 and AAV8) and synthetic (AAV2.7m8, AAV8BP2, and Anc80L65) AAVs in the mouse inner ear. We found that AAV8BP2 and AAV8 are capable of transducing the marginal cells and intermediate cells in the stria vascularis. These two AAVs can also transduce the epithe-lial cells of the endolymphatic sac. Our data suggest that AAV8BP2 and AAV8 are highly useful viral vectors for gene therapy studies targeting the cochlear lateral wall and the endolymphatic sac.

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