Vector platforms for gene therapy of inherited retinopathies

Trapani, Ivana; Puppo, Agostina; Auricchio, Alberto

doi:10.1016/j.preteyeres.2014.08.001

Cited by 152 publications

(163 citation statements)

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“…rAAV has shown promise for retinal gene transfer (12)(13)(14)(15)(16). In addition to the influence of the capsid discussed above, the route of administration to the retina determines the transgene expression profile and efficacy.…”

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“…Subretinal (SR) delivery deposits the vec-tor between the outer nuclear layer (ONL) and the retinal pigment epithelium (RPE), which causes detachment of these two layers to accommodate the injected solution. Many AAV serotypes display transduction in the ONL and RPE layers, with some serotypes showing restricted tropism (16). Of the natural serotypes, rAAV8 is one of the best for SR delivery based on its rapid transgene expression and transduction of all retinal layers (17,18).…”

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confidence: 99%

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Heparan Sulfate Binding Promotes Accumulation of Intravitreally Delivered Adeno-associated Viral Vectors at the Retina for Enhanced Transduction but Weakly Influences Tropism

Woodard

Liang

Bennett

et al. 2016

J Virol

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Many adeno-associated virus (AAV) serotypes efficiently transduce the retina when delivered to the subretinal space but show limited success when delivered to the vitreous due to the inner limiting membrane (ILM). Subretinal delivery of AAV serotype 2 (AAV2) and its heparan sulfate (HS)-binding-deficient capsid led to similar expression, indicating transduction of the outer retina occurred by HS-independent mechanisms. However, intravitreal delivery of HS-ablated recombinant AAV2 (rAAV2) led to a 300-fold decrease in transduction compared to AAV2. Fluorescence in situ hybridization of AAV transgenes was used to identify differences in retinal trafficking and revealed that HS binding was responsible for AAV2 accumulation at the ILM. This mechanism was tested on human ex vivo retinas and showed similar accumulation with HS-binding AAV2 capsid only. To evaluate if HS binding could be applied to other AAV serotypes to enhance their transduction, AAV1 and AAV8 were modified to bind HS with a single-amino-acid mutation and tested in mice. Both HS-binding mutants of AAV1 and AAV8 had higher intravitreal transduction than their non-HS-binding parent capsid due to increased retinal accumulation. To understand the influence that HS binding has on tropism, chimeric AAV2 capsids with dual-glycan usage were tested intravitreally in mice. Compared to HS binding alone, these chimeric capsids displayed enhanced transduction that was correlated with a change in tropism. Taken together, these data indicate that HS binding serves to sequester AAV capsids from the vitreous to the ILM but does not influence retinal tropism. The enhanced retinal transduction of HS-binding capsids provides a rational design strategy for engineering capsids for intravitreal delivery. A deno-associated virus (AAV) is a small (25-nm), nonpathogenic virus that has been extensively studied as a vector for gene transfer applications (1-3). The virus consists of two parts: the viral genome and the protein capsid. The viral genome can be largely replaced with a desired transgene to create recombinant AAV (rAAV) vectors used for gene delivery. The protein capsid is responsible for cell attachment and entry via a variety of glycans and cell surface receptors. There are 11 naturally occurring serotypes of AAV, denoted AAV1 to AAV11. Glycans and receptors have been elucidated for several AAV serotypes. Heparan sulfate proteoglycan (HSPG) has been shown to be used for both rAAV2 and rAAV3 cell entry (4). rAAV6 displays dual-glycan interaction with HSPG and sialic acid; however, HSPG binding alone is insufficient for cellular entry (5). Various linkages of sialic acid are important for the transduction of the rAAV1, rAAV4, and rAAV5 serotypes (6,7). N-linked galactose is used for the transduction of the rAAV9 serotype (8). Glycans expressed on the cell surface dictate the tissue and cellular tropism observed with the various AAV capsids. In addition to attachment to these glycans, AAV serotypes interact with cell receptors, including human growth factor rec...

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confidence: 99%

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confidence: 99%

Heparan Sulfate Binding Promotes Accumulation of Intravitreally Delivered Adeno-associated Viral Vectors at the Retina for Enhanced Transduction but Weakly Influences Tropism

Woodard

Liang

Bennett

et al. 2016

J Virol

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“…In addition, the availability of various animal models, along with in vivo imaging techniques, allows for noninvasive and consistent monitoring of the effects of gene delivery; outcomes may be compared with disease progression in the contralateral control eye. 6,7 Leber congenital amaurosis type 2 (LCA2) is the first IRD to have been treated with retinal gene therapy in phase I/II clinical trials, the results of which represent the most successful example of ocular gene therapy, to date. LCA2, an autosomal recessive IRD, is caused by mutations in RPE65, an essential gene in the retinal pathway.…”

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confidence: 99%

“…However, when injected intravitreally, most viral vectors, including the majority of AAV serotypes, do not transduce the retina with the exception of AAV2/2, and to some extent AAV2/6 and AAV2/8, whose transduction is, however, mainly restricted to retinal ganglion and Müller cells in the inner retina. 6,40 The failure of vectors delivered intravitreally to transduce PR and RPE in the outer retina appears to be caused by the presence of physical barriers, such as the inner limiting membrane, which is particularly thick in large animals, as well as the relative abundance of AAV receptors that capture vectors after intravitreal administration. 41 Indeed, if retinal architecture is altered by a degenerative process [42][43][44] or by enzymatic digestion, 41 the diffusion of AAV viral particles to the outer retina from the vitreous side increases.…”

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confidence: 99%

“…49 However, Ad vectors efficiently transduce the RPE but less robustly adult mouse PR. 6,50,51 Similarly, LV vectors have been successfully used to transduce PR in newborn rat and mouse retinas and thus, to effectively improve the phenotype of animal models of IRDs. 27,29,[52][53][54][55][56] Although recent reports suggest that LV vectors transduce adult nonhuman primate PR, 28,29 RPE transduction has been primarily observed in adult animals.…”

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Gene Therapy of Inherited Retinal Degenerations: Prospects and Challenges

et al. 2015

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Because of its favorable anatomical and immunological characteristics, the eye has been at the forefront of translational gene therapy. Dozens of promising proofs of concept have been obtained in animal models of inherited retinal degenerations (IRDs), and some of them have been relayed to the clinic. The results from the first clinical trials for a congenital form of blindness have generated great interest and have demonstrated the safety and efficacy of intraocular administrations of viral vectors in humans. However, this progress has also generated new questions and posed challenges that need to be addressed to further expand the applicability of gene therapy in the eye, including safe delivery of viral vectors to the outer retina, treatment of dominant IRDs as well as of IRDs caused by mutations in large genes, and, finally, selection of the appropriate IRDs and patients to maximize the efficacy of gene transfer. This review summarizes the strategies that are currently being exploited to overcome these challenges and drive the clinical development of retinal gene therapy.

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Gene and Cell Therapy for Inherited Retinal Dystrophies

Garita-Hernández

Goureau

Dalkara

2016

Encyclopedia of Life Sciences

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Gene therapy and cell therapy are intersecting fields of biomedical research with the common aim of repairing the direct causes or consequences of genetic diseases by using genes and cells, respectively. Gene therapy is broadly defined as a set of strategies that modify the expression of an individual's genes for therapeutic benefit. It requires the administration of a specific deoxyribonucleic acid (DNA) (or ribonucleic acid (RNA)) into the patient's cells. Cell therapy on the other hand requires administration of a population of intact live cells to a patient whose cells have been lost due to injury or disease. These emerging strategies can also be applied in acquired diseases in order to re‐establish equilibrium and halt disease progression. In some cases, gene and cell therapy may be combined in order to obtain a therapeutic effect. In addition to becoming emerging therapeutics in the clinic, these two fields of research continually generate tools, concepts and techniques for elucidating biological questions across multiple disciplines. Key Concepts The retina lines the back of the eye and comprises six different types of neuronal cells and their underlying retinal pigment epithelium (RPE). Photoreceptors are the light‐sensitive first‐order neurons of the retina which capture the light stimulus and transform it into an electric signal. Human iPSC have the same features of hESC in terms of their differentiation capacity. Gene therapy is the use of genetic material as a drug to treat a chronic condition.

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Vector platforms for gene therapy of inherited retinopathies

Cited by 152 publications

References 297 publications

Heparan Sulfate Binding Promotes Accumulation of Intravitreally Delivered Adeno-associated Viral Vectors at the Retina for Enhanced Transduction but Weakly Influences Tropism

Heparan Sulfate Binding Promotes Accumulation of Intravitreally Delivered Adeno-associated Viral Vectors at the Retina for Enhanced Transduction but Weakly Influences Tropism

Gene Therapy of Inherited Retinal Degenerations: Prospects and Challenges

Gene and Cell Therapy for Inherited Retinal Dystrophies

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