Literature DB >> 27003753

Safety and Biodistribution Evaluation in Cynomolgus Macaques of rAAV2tYF-PR1.7-hCNGB3, a Recombinant AAV Vector for Treatment of Achromatopsia.

Guo-jie Ye1, Ewa Budzynski2, Peter Sonnentag2, T Michael Nork3, Paul E Miller3, Alok K Sharma2, James N Ver Hoeve3, Leia M Smith4, Tara Arndt2, Roberto Calcedo5, Chantelle Gaskin1, Paulette M Robinson1, David R Knop1, William W Hauswirth6, Jeffrey D Chulay1.   

Abstract

Applied Genetic Technologies Corporation (AGTC) is developing rAAV2tYF-PR1.7-hCNGB3, a recombinant adeno-associated viral (rAAV) vector expressing the human CNGB3 gene, for treatment of achromatopsia, an inherited retinal disorder characterized by markedly reduced visual acuity, extreme light sensitivity, and absence of color discrimination. We report here results of a study evaluating the safety and biodistribution of rAAV2tYF-PR1.7-hCNGB3 in cynomolgus macaques. Three groups of animals (n = 2 males and 2 females per group) received a subretinal injection in one eye of 300 μl containing either vehicle or rAAV2tYF-PR1.7-hCNGB3 at one of two concentrations (4 × 10(11) or 4 × 10(12) vector genomes/ml) and were evaluated over a 3-month period before being euthanized. Administration of rAAV2tYF-PR1.7-hCNGB3 was associated with a dose-related anterior and posterior segment inflammatory response that was greater than that observed in eyes injected with the vehicle control. Most manifestations of inflammation improved over time except that vitreous cells persisted in vector-treated eyes until the end of the study. One animal in the lower vector dose group was euthanized on study day 5, based on a clinical diagnosis of endophthalmitis. There were no test article-related effects on intraocular pressure, visual evoked potential responses, hematology or clinical chemistry parameters, or gross necropsy observations. Histopathological examination demonstrated minimal mononuclear infiltrates in all vector-injected eyes. Serum anti-AAV antibodies developed in all vector-injected animals. No animals developed antibodies to CNGB3. Biodistribution studies demonstrated high levels of vector DNA in the injected eye but minimal or no vector DNA in any other tissue. These results support the use of rAAV2tYF-PR1.7-hCNGB3 in clinical studies in patients with achromatopsia caused by CNGB3 mutations.

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Year:  2016        PMID: 27003753      PMCID: PMC4851175          DOI: 10.1089/humc.2015.164

Source DB:  PubMed          Journal:  Hum Gene Ther Clin Dev        ISSN: 2324-8637            Impact factor:   5.032


  34 in total

1.  Safety and Biodistribution Evaluation of rAAV2tYF-CB-hRS1, a Recombinant Adeno-Associated Virus Vector Expressing Retinoschisin, in RS1-Deficient Mice.

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Journal:  Hum Gene Ther Clin Dev       Date:  2015-09       Impact factor: 5.032

2.  Safety and Biodistribution Evaluation in Cynomolgus Macaques of rAAV2tYF-CB-hRS1, a Recombinant Adeno-Associated Virus Vector Expressing Retinoschisin.

Authors:  Guo-Jie Ye; Ewa Budzynski; Peter Sonnentag; Paul E Miller; Alok K Sharma; James N Ver Hoeve; Kellie Howard; David R Knop; Martha Neuringer; Trevor McGill; Jonathan Stoddard; Jeffrey D Chulay
Journal:  Hum Gene Ther Clin Dev       Date:  2015-09       Impact factor: 5.032

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Authors:  Duska J Sidjanin; Jennifer K Lowe; John L McElwee; Bruce S Milne; Taryn M Phippen; David R Sargan; Gustavo D Aguirre; Gregory M Acland; Elaine A Ostrander
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8.  Safety and Biodistribution Evaluation in CNGB3-Deficient Mice of rAAV2tYF-PR1.7-hCNGB3, a Recombinant AAV Vector for Treatment of Achromatopsia.

Authors:  Guo-jie Ye; Ewa Budzynski; Peter Sonnentag; T Michael Nork; Paul E Miller; Leslie McPherson; James N Ver Hoeve; Leia M Smith; Tara Arndt; Savitri Mandapati; Paulette M Robinson; Roberto Calcedo; David R Knop; William W Hauswirth; Jeffrey D Chulay
Journal:  Hum Gene Ther Clin Dev       Date:  2016-03       Impact factor: 5.032

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  32 in total

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2.  An Alternative and Validated Injection Method for Accessing the Subretinal Space via a Transcleral Posterior Approach.

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4.  Noninvasive gene delivery to foveal cones for vision restoration.

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Journal:  JCI Insight       Date:  2018-01-25

5.  Synthetic Adeno-Associated Viral Vector Efficiently Targets Mouse and Nonhuman Primate Retina In Vivo.

Authors:  Livia S Carvalho; Ru Xiao; Sarah J Wassmer; Aliete Langsdorf; Eric Zinn; Simon Pacouret; Samiksha Shah; Jason I Comander; Leo A Kim; Laurence Lim; Luk H Vandenberghe
Journal:  Hum Gene Ther       Date:  2018-03-20       Impact factor: 5.695

6.  Toxicity and Efficacy Evaluation of an Adeno-Associated Virus Vector Expressing Codon-Optimized RPGR Delivered by Subretinal Injection in a Canine Model of X-linked Retinitis Pigmentosa.

Authors:  Valérie L Dufour; Artur V Cideciyan; Guo-Jie Ye; Chunjuan Song; Adrian Timmers; Perry L Habecker; Wei Pan; Nicole M Weinstein; Malgorzata Swider; Amy C Durham; Gui-Shuang Ying; Paulette M Robinson; Samuel G Jacobson; David R Knop; Jeffrey D Chulay; Mark S Shearman; Gustavo D Aguirre; William A Beltran
Journal:  Hum Gene Ther       Date:  2020-02-06       Impact factor: 5.695

7.  Optimization of Retinal Gene Therapy for X-Linked Retinitis Pigmentosa Due to RPGR Mutations.

Authors:  William A Beltran; Artur V Cideciyan; Shannon E Boye; Guo-Jie Ye; Simone Iwabe; Valerie L Dufour; Luis Felipe Marinho; Malgorzata Swider; Mychajlo S Kosyk; Jin Sha; Sanford L Boye; James J Peterson; C Douglas Witherspoon; John J Alexander; Gui-Shuang Ying; Mark S Shearman; Jeffrey D Chulay; William W Hauswirth; Paul D Gamlin; Samuel G Jacobson; Gustavo D Aguirre
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8.  AAV8 Can Induce Innate and Adaptive Immune Response in the Primate Eye.

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9.  Safety and Biodistribution Evaluation in CNGB3-Deficient Mice of rAAV2tYF-PR1.7-hCNGB3, a Recombinant AAV Vector for Treatment of Achromatopsia.

Authors:  Guo-jie Ye; Ewa Budzynski; Peter Sonnentag; T Michael Nork; Paul E Miller; Leslie McPherson; James N Ver Hoeve; Leia M Smith; Tara Arndt; Savitri Mandapati; Paulette M Robinson; Roberto Calcedo; David R Knop; William W Hauswirth; Jeffrey D Chulay
Journal:  Hum Gene Ther Clin Dev       Date:  2016-03       Impact factor: 5.032

10.  Safety and Efficacy of AAV5 Vectors Expressing Human or Canine CNGB3 in CNGB3-Mutant Dogs.

Authors:  Guo-Jie Ye; András M Komáromy; Caroline Zeiss; Roberto Calcedo; Christine D Harman; Kristin L Koehl; Gabriel A Stewart; Simone Iwabe; Vince A Chiodo; William W Hauswirth; Gustavo D Aguirre; Jeffrey D Chulay
Journal:  Hum Gene Ther Clin Dev       Date:  2017-10-11       Impact factor: 5.032

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