Recombinant Adeno-Associated Viral Vectors (rAAV)-Vector Elements in Ocular Gene Therapy Clinical Trials and Transgene Expression and Bioactivity Assays

Buck, Thilo M.; Wijnholds, Jan

doi:10.3390/ijms21124197

Cited by 58 publications

(51 citation statements)

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“…Here, we further extended this concept by an in-depth analysis of various capsids linked to retinal gene therapy. The naturally occurring serotypes AAV2, AAV8, and the developed AAV2.7m8 were chosen, as they are currently applied in clinical trials or approved retinal therapy ( Buck and Wijnholds, 2020 ; Shahryari et al., 2019 ). Furthermore, AAV2.7m8 is a second-generation AAV developed via in vivo directed evolution, created and selected for more efficient delivery in ocular gene therapies ( Dalkara et al., 2013 ).…”

Section: Discussionmentioning

confidence: 99%

Human stem cell-based retina on chip as new translational model for validation of AAV retinal gene therapy vectors

et al. 2021

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Gene therapies using adeno-associated viruses (AAVs) are among the most promising strategies to treat or even cure hereditary and acquired retinal diseases. However, the development of new efficient AAV vectors is slow and costly, largely because of the lack of suitable non-clinical models. By faithfully recreating structure and function of human tissues, human induced pluripotent stem cell (iPSC)derived retinal organoids could become an essential part of the test cascade addressing translational aspects. Organ-on-chip (OoC) technology further provides the capability to recapitulate microphysiological tissue environments as well as a precise control over structural and temporal parameters. By employing our recently developed retina on chip that merges organoid and OoC technology, we analyzed the efficacy, kinetics, and cell tropism of seven first-and second-generation AAV vectors. The presented data demonstrate the potential of iPSC-based OoC models as the next generation of screening platforms for future gene therapeutic studies.

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Section: Discussionmentioning

confidence: 99%

Human stem cell-based retina on chip as new translational model for validation of AAV retinal gene therapy vectors

et al. 2021

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“…Although gene therapies based on lentiviral and nonviral vectors delivery are in development, vectors derived from adeno-associated virus (AAV) are currently the most commonly used platform for delivery of ocular gene therapy. 4 , 5 Wild-type AAV is a small DNA virus with many naturally occurring capsid serotypes, which can be used directly for gene therapy or first intentionally modified. The virus is primarily non-integrating but persists as episomal DNA.…”

Section: Meeting Goals In the Context Of Ocular Gene Therapy History mentioning

confidence: 99%

Inflammation in Viral Vector-Mediated Ocular Gene Therapy: A Review and Report From a Workshop Hosted by the Foundation Fighting Blindness, 9/2020

Chan

Dick²,

Hall³

et al. 2021

Trans. Vis. Sci. Tech.

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On September 14–15, 2020, the Foundation Fighting Blindness convened a virtual workshop to discuss intraocular inflammation during viral vector-mediated gene therapy for inherited retinal diseases. The workshop's goals were to understand immune activation's nature and significance during ocular gene therapy, consider whether ocular inflammation limits gene therapy's potential, and identify knowledge gaps for future research. The event brought together a small group of experienced researchers in the field to present and discuss current data. Collectively, participants agreed that clinical, as well as subclinical, inflammation during ocular gene therapy is common. The severity of inflammation in both animal and clinical studies varied widely but is generally related to vector dose. Severe inflammation was associated with reduced gene therapy efficacy. However, the relationship between outcomes and subclinical inflammation, pre-existing antivector antibodies, or induced adaptive immune responses is still unclear. Uncertainties about the contribution of vector manufacturing issues to inflammation were also noted. Importantly, various immunosuppressive treatment protocols are being used, and this heterogeneity confounds conclusions about optimal strategies. Proposed near-term next steps include establishing an immunological consultant directory, establishing a data repository for pertinent animal and clinical data, and developing a larger meeting. Priority areas for future research include deeper understanding of immune activation during retinal diseases and during ocular gene therapy; better, harmonized application of animal models; and identifying best practices for managing gene therapy vector-related ocular inflammation. Translational Relevance Subclinical or clinical inflammation often arises during ocular gene therapy with viral vectors. Understanding the biological bases and impacts on efficacy are important for clinical management and the improvement of future therapies.

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“…One of the first approaches to show gene transfer in mouse retina used rAAV vectors to deliver a reporter gene by subretinal injection into an adult mouse retina [62]. Since then, AAV-mediated gene delivery into the retina has been used in several proof-of-concept studies to target photoreceptors or the RPE in mice and larger models (such as dogs) [63][64][65]. Notably, one of the studies involving the delivery of the RPE65 gene into mutant dogs showed therapeutic potential, which subsequently led to the approval of the first gene therapy drug (Luxturna TM ) by the Food and Drug Administration in 2018 [66].…”

Section: Viral Vectorsmentioning

confidence: 99%

The Ocular Gene Delivery Landscape

2021

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The eye is at the forefront of developing therapies for genetic diseases. With the FDA approval of the first gene-therapy drug for a form of congenital blindness, numerous studies have been initiated to develop gene therapies for other forms of eye diseases. These examinations have revealed new information about the benefits as well as restrictions to using drug-delivery routes to the different parts of the eye. In this article, we will discuss a brief history of gene therapy and its importance to the eye and ocular delivery landscape that is currently being investigated, and provide insights into their advantages and disadvantages. Efficient delivery routes and vehicle are crucial for an effective, safe, and longer-lasting therapy.

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Recombinant Adeno-Associated Viral Vectors (rAAV)-Vector Elements in Ocular Gene Therapy Clinical Trials and Transgene Expression and Bioactivity Assays

Cited by 58 publications

References 296 publications

Human stem cell-based retina on chip as new translational model for validation of AAV retinal gene therapy vectors

Human stem cell-based retina on chip as new translational model for validation of AAV retinal gene therapy vectors

Inflammation in Viral Vector-Mediated Ocular Gene Therapy: A Review and Report From a Workshop Hosted by the Foundation Fighting Blindness, 9/2020

The Ocular Gene Delivery Landscape

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