Evaluation of Dose and Safety of AAV7m8 and AAV8BP2 in the Non-Human Primate Retina

Ramachandran, Pavitra S.; Lee, Vivian; Wei, Zhengyu; Song, Ji Yun; Casal, Giulia; Cronin, Thérèse; Willett, Keirnan; Huckfeldt, Rachel M.; Morgan, Jessica Ijams Wolfing; Alemán, Tomás S.; Maguire, Albert M.; Bennett, Jean

doi:10.1089/hum.2016.111

Cited by 111 publications

(110 citation statements)

References 31 publications

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“…We and others have shown transduction of macaque cones using AAV variants with ubiquitous promoters (16,(29)(30)(31)(32), but achieving cone transduction by vitreally administered AAV has only been possible at high doses, leading to inflammation (16,29). We reasoned that foveal cone targeting could be achieved if we use a strong cone-specific promoter at lower intravitreally injected AAV doses compatible with safety (29,33). To test if such "dose sparing" is possible, we injected 2 macaque eyes with AAV2-7m8-PR1.7-GFP and 2 other macaque eyes were injected with AAV2-7m8-GFP under the control of the cytomegalovirus (CMV) promoter at a dose of 1 × 10 11 viral genomes (vg) per eye (Table 1).…”

Section: Resultsmentioning

confidence: 99%

“…Altogether, our data in NHPs show for the first time to our knowledge noninvasive, specific, and high-level primate foveal cone transduction compatible with optogenetic applications for vision restoration. However, as promoter activity shows important variations across species (16,29,36), we deemed it necessary to validate PR1.7 in human cells and tissues. Due to the lack of a good human photoreceptor cell line or other model that could be used to test efficiency of cone promoter activity, we used 3-D retinal organoids derived from human induced pluripotent stem cells (iPSCs) (37).…”

Section: Resultsmentioning

confidence: 99%

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Noninvasive gene delivery to foveal cones for vision restoration

Khabou¹,

Garita-Hernández²,

Chaffiol³

et al. 2018

JCI Insight

102

105

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Noninvasive gene delivery to foveal cones for vision restoration

Khabou¹,

Garita-Hernández²,

Chaffiol³

et al. 2018

JCI Insight

102

105

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“…Several AAVs have been tested for retinal gene delivery via the intravitreal route, and some have evoked safety concerns that have not been fully addressed at this stage. 25,43 For example, a recent study suggested that the engineered AAV variant AAV2-7m8 might be more immunogenic when used at high doses via intravitreal injections. 25 Therefore, we chose AAV2 for its known safety and efficacy in targeting RGCs in NHP studies [27][28][29] and the large body of work using this vector in human clinical trials.…”

Section: Discussionmentioning

confidence: 99%

“…25,43 For example, a recent study suggested that the engineered AAV variant AAV2-7m8 might be more immunogenic when used at high doses via intravitreal injections. 25 Therefore, we chose AAV2 for its known safety and efficacy in targeting RGCs in NHP studies [27][28][29] and the large body of work using this vector in human clinical trials. [20][21][22][23]44 High-level expression with a limited viral dose being a major parameter in obtaining functional expression, we designed a new RGC-specific promoter, driving strong transgene expression in RGCs.…”

Section: Discussionmentioning

confidence: 99%

“…First, optogenetically equipped cells require very high-level opsin expression, as there is no amplification cascade behind microbial opsins. 19 Although adeno-associated viruses (AAVs) have a favorable safety profile in clinical gene therapy, [20][21][22][23] their safety is dose dependent, 24,25 limiting the injected dose. This makes our ability to obtain functional-level microbial opsin expression with a safe viral dose uncertain.…”

Section: Introductionmentioning

confidence: 99%

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A New Promoter Allows Optogenetic Vision Restoration with Enhanced Sensitivity in Macaque Retina

et al. 2017

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The majority of inherited retinal degenerations converge on the phenotype of photoreceptor cell death. Second-and third-order neurons are spared in these diseases, making it possible to restore retinal light responses using optogenetics. Viral expression of channelrhodopsin in the third-order neurons under ubiquitous promoters was previously shown to restore visual function, albeit at light intensities above illumination safety thresholds. Here, we report (to our knowledge, for the first time) activation of macaque retinas, up to 6 months post-injection, using channelrhodopsin-Ca 2+ -permeable channelrhodopsin (CatCh) at safe light intensities. High-level CatCh expression was achieved due to a new promoter based on the regulatory region of the gamma-synuclein gene (SNCG) allowing strong expression in ganglion cells across species. Our promoter, in combination with clinically proven adeno-associated virus 2 (AAV2), provides CatCh expression in peri-foveolar ganglion cells responding robustly to light under the illumination safety thresholds for the human eye. On the contrary, the threshold of activation and the proportion of unresponsive cells were much higher when a ubiquitous promoter (cytomegalovirus [CMV]) was used to express CatCh. The results of our study suggest that the inclusion of optimized promoters is key in the path to clinical translation of optogenetics.

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Formulation and Evaluation of Polymer‐Based Nanoparticles for Intravitreal Gene‐Delivery Applications

et al. 2022

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The advent of the first-ever retinal gene therapy product, involving subretinal administration of a virus-based gene delivery platform, has garnered hope that this state-of-the-art therapeutic modality may benefit a broad spectrum of patients with diverse retinal disorders. On the other hand, clinical studies have revealed limitations of the applied delivery strategy that may restrict its universal use. To this end, intravitreal administration of synthetic gene-delivery platforms, such as polymer-based nanoparticles (PNPs), has emerged as an attractive alternative to the current mainstay. To achieve success, however, it is imperative that synthetic platforms overcome key biological barriers in human eyes encountered following intravitreal administration, including the vitreous gel and inner limiting membrane (ILM). Here, we introduce a series of experiments, from the fabrication of PNPs to a comprehensive evaluation in relevant experimental models, to determine whether PNPs overcome these barriers and efficiently deliver therapeutic gene payloads to retinal cells. We conclude the article by discussing a few important considerations for successful implementation of the strategy.

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Evaluation of Dose and Safety of AAV7m8 and AAV8BP2 in the Non-Human Primate Retina

Cited by 111 publications

References 31 publications

Noninvasive gene delivery to foveal cones for vision restoration

Noninvasive gene delivery to foveal cones for vision restoration

A New Promoter Allows Optogenetic Vision Restoration with Enhanced Sensitivity in Macaque Retina

Formulation and Evaluation of Polymer‐Based Nanoparticles for Intravitreal Gene‐Delivery Applications

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