2017
DOI: 10.1089/humc.2017.028
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Safety and Efficacy Evaluation of rAAV2tYF-PR1.7-hCNGA3 Vector Delivered by Subretinal Injection in CNGA3 Mutant Achromatopsia Sheep

Abstract: {These authors contributed equally to this work.Applied Genetic Technologies Corporation (AGTC) is developing a recombinant adeno-associated virus (rAAV) vector expressing the human CNGA3 gene designated AGTC-402 (rAAV2tYF-PR1.7-hCNGA3) for the treatment of achromatopsia, an inherited retinal disorder characterized by markedly reduced visual acuity, extreme light sensitivity, and absence of color discrimination. The results are herein reported of a study evaluating safety and efficacy of AGTC-402 in CNGA3-defi… Show more

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Cited by 31 publications
(21 citation statements)
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“…Except for focal retinal atrophy in the right eye of animal M731, who received the lower dose of the vector expressing canine CNGB3, the pathologic changes were minimal or non-existent in the eyes treated with the lower vector dose. The dose-related inflammation seen in these studies is consistent with results seen in other studies of gene therapy vectors delivered by intraocular injection in a variety of species, 17,[21][22][23] but an explanation for the unexpected development of more severe chorioretinitis with the canine CNGB3 vector than with the human CNGB3 vector in study 3 is not apparent. It was not due to a mix-up in labeling of the vectors that were administered, since residual samples of vector collected after subretinal administration were tested by polymerase chain reaction (PCR) and determined to have the correct sequence of the canine or human CNGB3 cDNA specified in the protocol (data not shown).…”
Section: Aav-cngb3 Vectors In Achm Dogssupporting
confidence: 88%
“…Except for focal retinal atrophy in the right eye of animal M731, who received the lower dose of the vector expressing canine CNGB3, the pathologic changes were minimal or non-existent in the eyes treated with the lower vector dose. The dose-related inflammation seen in these studies is consistent with results seen in other studies of gene therapy vectors delivered by intraocular injection in a variety of species, 17,[21][22][23] but an explanation for the unexpected development of more severe chorioretinitis with the canine CNGB3 vector than with the human CNGB3 vector in study 3 is not apparent. It was not due to a mix-up in labeling of the vectors that were administered, since residual samples of vector collected after subretinal administration were tested by polymerase chain reaction (PCR) and determined to have the correct sequence of the canine or human CNGB3 cDNA specified in the protocol (data not shown).…”
Section: Aav-cngb3 Vectors In Achm Dogssupporting
confidence: 88%
“…Recently, successful gene therapies have been reported in CNGA3-deficient sheep, a large-animal model of achromatopsia [ 50 52 ]. In these studies, AAV serotype 2 and 5 vectors carry Cnga3 gene under control of a human red/green cone opsin promoter.…”
Section: Discussionmentioning
confidence: 99%
“…The first identified has a nonsense mutation (p.Arg236Ter) and the second a missense mutation (p.Gly540Ser) [84]. Adeno-associated virus gene therapy was able to restore cone function in both models [84,85].…”
Section: Cnga3mentioning
confidence: 99%