Characterization of Gene Therapy Associated Uveitis Following Intravitreal Adeno-Associated Virus Injection in Mice

Tummala, Gayathri; Crain, Adam; Rowlan, Jessica S.; Pepple, Kathryn L.

doi:10.1167/iovs.62.2.41

Cited by 21 publications

(20 citation statements)

References 32 publications

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“…Following an intravitreal injection, a dose dependent immune response is observed presenting as cells in either the anterior chamber and/or the vitreous. Both cellular and humoral factors have been implicated ( 45 – 47 ). In mice, an AAV injection into the vitreous leads to a transient mild spontaneously resolving inflammation but the total number of CD45+ T cells remains elevated, even weeks after the injection.…”

Section: Immune Consequence Of Subretinal and Intravitreal Deliverymentioning

confidence: 99%

“…In mice, an AAV injection into the vitreous leads to a transient mild spontaneously resolving inflammation but the total number of CD45+ T cells remains elevated, even weeks after the injection. Both innate and adaptive immunity play a role regardless of prior immune status ( 45 ). A patient treated for Lebers with a single intravitreal dose of 9 × 10 10 vg and high pre-treatment titers of IgG neutralizing antibodies to AAV2, developed a significant post-injection ocular inflammation ( 46 ).…”

Section: Immune Consequence Of Subretinal and Intravitreal Deliverymentioning

confidence: 99%

“…While improved pre-injection screening may reduce the incidence of such events, they limit the applicability of this approach. The presence of inflammation also will limit the efficiency of transfection or the duration of the effect if it leads to the elimination of transfected cells ( 45 , 49 , 50 ).…”

Section: Immune Consequence Of Subretinal and Intravitreal Deliverymentioning

confidence: 99%

See 2 more Smart Citations

Subretinal Therapy: Technological Solutions to Surgical and Immunological Challenges

et al. 2022

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Recent advances in ocular gene and cellular therapy rely on precisely controlled subretinal delivery. Due to its inherent limitations, manual delivery can lead to iatrogenic damage to the retina, the retinal pigment epithelium, favor reflux into the vitreous cavity. In addition, it suffers from lack of standardization, variability in delivery and the need to maintain proficiency. With or without surgical damage, an eye challenged with an exogenous viral vector or transplanted cells will illicit an immune response. Understanding how such a response manifests itself and to what extent immune privilege protects the eye from a reaction can help in anticipating short- and long-term consequences. Avoidance of spillover from areas of immune privilege to areas which either lack or have less protection should be part of any mitigation strategy. In that regard, robotic technology can provide reproducible, standardized delivery which is not dependent on speed of injection. The advantages of microprecision medical robotic technology for precise targeted deliveries are discussed.

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Section: Immune Consequence Of Subretinal and Intravitreal Deliverymentioning

confidence: 99%

Section: Immune Consequence Of Subretinal and Intravitreal Deliverymentioning

confidence: 99%

Section: Immune Consequence Of Subretinal and Intravitreal Deliverymentioning

confidence: 99%

See 1 more Smart Citation

Subretinal Therapy: Technological Solutions to Surgical and Immunological Challenges

et al. 2022

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“…One general concern for AAV vectors is that pre-existing immunity and subsequent induced adaptive immunity following vector administration can significantly reduce retinal gene expression, as shown in pre-clinical studies [ 82 ]. Furthermore, there is growing appreciation for the risk of gene therapy associated uveitis following AAV administration, which appears to be related to the vector dose and route of administration [ 83 , 84 ]. However, optogenetic clinical trials thus far have demonstrated that intravitreal delivery of AAV-based vectors is mostly safe and well-tolerated [ 8 ].…”

Section: Using Optogenetics In Retinal Degeneration and Glaucomamentioning

confidence: 99%

Advances in Ophthalmic Optogenetics: Approaches and Applications

et al. 2022

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Recent advances in optogenetics hold promise for vision restoration in degenerative eye diseases. Optogenetics refers to techniques that use light to control the cellular activity of targeted cells. Although optogenetics is a relatively new technology, multiple therapeutic options are already being explored in pre-clinical and phase I/II clinical trials with the aim of developing novel, safe, and effective treatments for major blinding eye diseases, such as glaucoma and retinitis pigmentosa. Optogenetic approaches to visual restoration are primarily aimed at replacing lost or dysfunctional photoreceptors by inserting light-sensitive proteins into downstream retinal neurons that have no intrinsic light sensitivity. Such approaches are attractive because they are agnostic to the genetic causes of retinal degeneration, which raises hopes that all forms of retinal dystrophic and degenerative diseases could become treatable. Optogenetic strategies can also have a far-reaching impact on translational research by serving as important tools to study the pathogenesis of retinal degeneration and to identify clinically relevant therapeutic targets. For example, the CRY-CIBN optogenetic system has been recently applied to animal models of glaucoma, suggesting a potential role of OCRL in the regulation of intraocular pressure in trabecular meshwork. As optogenetic strategies are being intensely investigated, it appears crucial to consider the opportunities and challenges such therapies may offer. Here, we review the more recent promising optogenetic molecules, vectors, and applications of optogenetics for the treatment of retinal degeneration and glaucoma. We also summarize the preliminary results of ongoing clinical trials for visual restoration.

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“…Although there are several reports linking AAV ocular gene therapy to an immune/inflammatory response, especially at high doses, no adverse effects were reported following AAV-HLA-G subconjunctival, intracorneal, or intravitreal dosing [ 14 , 15 , 16 , 42 , 55 , 56 , 57 , 58 ]. Another concern for ocular gene therapy is the durability of the transgene expression following ocular delivery.…”

Section: Hla-g and The Eyementioning

confidence: 99%

Therapeutic Applications of Adeno-Associated Virus (AAV) Gene Transfer of HLA-G in the Eye

Gilger

Hirsch

2022

IJMS

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The purpose of this paper is to review human leukocyte antigen G (HLA-G) in the eye, its role in immune tolerance, and the potential therapeutic use of AAV gene transfer and expression of HLA-G in various ocular tissues. Several studies are reviewed that demonstrate efficacy in animal models of disease, including intracorneal delivery of AAV-HLA-G to treat corneal inflammation and prevent corneal graft rejection, subconjunctival injection of AAV-HLA-G for ocular graft vs. host disease and potentially dry eye disease, and intravitreal injection of AAV-HLA-G to inhibit uveitis. Furthermore, due to the anti-vascular function of HLA-G, AAV-HLA-G may be an effective therapy for posterior ocular diseases, such as neovascular age-related macular degeneration, diabetic retinopathy, and choroidal neovascularization. Therefore, AAV-mediated gene transfer of HLA-G may be an effective treatment for common immune-mediated, inflammatory, and neovascular diseases of the eye.

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Characterization of Gene Therapy Associated Uveitis Following Intravitreal Adeno-Associated Virus Injection in Mice

Cited by 21 publications

References 32 publications

Subretinal Therapy: Technological Solutions to Surgical and Immunological Challenges

Subretinal Therapy: Technological Solutions to Surgical and Immunological Challenges

Advances in Ophthalmic Optogenetics: Approaches and Applications

Therapeutic Applications of Adeno-Associated Virus (AAV) Gene Transfer of HLA-G in the Eye

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