The Human Rhodopsin Kinase Promoter in an AAV5 Vector Confers Rod- and Cone-Specific Expression in the Primate Retina

Boye, Shannon E.; Alexander, John J.; Boye, Sanford L.; Witherspoon, C. Douglas; Sandefer, Kristen J.; Conlon, Thomas J.; Erger, Kirsten; Sun, Jingfen; Ryals, Renee C.; Chiodo, Vince A.; Clark, Mark E.; Girkin, Christopher A.; Hauswirth, William W.; Gamlin, Paul D.

doi:10.1089/hum.2012.125

Cited by 97 publications

(120 citation statements)

References 68 publications

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“…The only reports of AAV8-mediated photoreceptor expression in NHP indicated that AAV8 at (1 · 10 10 vg) did not efficiently transduce foveal, parafoveal, or perifoveal cones following subretinal injection (Vandenberghe et al, 2011a(Vandenberghe et al, 2011b. In contrast, AAV5 efficiently transduces cones in all these areas of NHP retina at comparable vector concentration (Boye et al, 2012). Hence, assuming a subretinal delivery route, the evidence to date would support the use of AAV5 in conjunction with the GRK1 promoter for driving GC1 expression in a clinical setting.…”

Section: Discussionmentioning

confidence: 97%

“…Multiple studies have shown that the human rhodopsin kinase (hGRK1) promoter drives efficient and rod/cone-specific transgene expression in mice (Khani et al, 2007;Boye et al, 2010Boye et al, , 2011Pawlyk et al, 2010;Sun et al, 2010;Mihelec et al, 2011) and most recently in nonhuman primates (Boye et al, 2012). Notably, within the NHP retina, the hGRK1 promoter was active in foveal cones (Boye et al, 2012). Viral serotype choice is dependent upon the route of administration as transduction profiles differ greatly depending on where the vector is deposited (Vandenberghe and Auricchio, 2012).…”

Section: Discussionmentioning

confidence: 99%

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AAV-Mediated Gene Therapy in the Guanylate Cyclase (RetGC1/RetGC2) Double Knockout Mouse Model of Leber Congenital Amaurosis

et al. 2013

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Mutations in GUCY2D are associated with recessive Leber congenital amaurosis-1 (LCA1). GUCY2D encodes photoreceptor-specific, retinal guanylate cyclase-1 (RetGC1). Reports of retinal degeneration in LCA1 are conflicting; some describe no obvious degeneration and others report loss of both rods and cones. Proof of concept studies in models representing the spectrum of phenotypes is warranted. We have previously demonstrated adeno-associated virus (AAV)-mediated RetGC1 is therapeutic in GC1ko mice, a model exhibiting loss of cones only. The purpose of this study was to characterize AAV-mediated gene therapy in the RetGC1/RetGC2 double knockout (GCdko) mouse, a model lacking rod and cone function and exhibiting progressive loss of both photoreceptor subclasses. Use of this model also allowed for the evaluation of the functional efficiency of transgenic RetGC1 isozyme. Subretinal delivery of AAV8(Y733F) vector containing the human rhodopsin kinase (hGRK1) promoter driving murine Gucy2e was performed in GCdko mice at various postnatal time points. Treatment resulted in restoration of rod and cone function at all treatment ages and preservation of retinal structure in GCdko mice treated as late as 7 weeks of age. Functional gains and structural preservation were stable for at least 1 year. Treatment also conferred cortical-and subcortical-based visually-guided behavior. Functional efficiency of transgenic RetGC1 was indistinguishable from that of endogenous isozyme in congenic wild-type (WT) mice. This study clearly demonstrates AAV-mediated RetGC1 expression restores function to and preserves structure of rod and cone photoreceptors in a degenerative model of retinal guanylate cyclase deficiency, further supporting development of an AAV-based vector for treatment of LCA1.

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Section: Discussionmentioning

confidence: 97%

Section: Discussionmentioning

confidence: 99%

AAV-Mediated Gene Therapy in the Guanylate Cyclase (RetGC1/RetGC2) Double Knockout Mouse Model of Leber Congenital Amaurosis

et al. 2013

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“…Mice were injected intravitreally with 4 ϫ 10 10 vg (high dose) or 4 ϫ 10 9 vg (low dose) or subretinally with 1 ϫ 10 10 vg (high dose) or 2 ϫ 10 9 vg (low dose). Although C57Bl/6J mice do not have sortable photoreceptors and, thus, FACS cannot be used as described above, hGRK1 has been shown to restrict transgene expression to rods and cones following subretinal injection (14,57). Representative fundus images and retinal cross sections revealed a clear dose response for each vector following either injection route (Fig.…”

Section: Aav2 Y-f and Y-f؉t-v Variants Bind Hs Aav2-based Variants Cmentioning

confidence: 95%

“…Data described above revealed that both AAV2(quadY-FϩT-V) and AAV2(4pMut) transduce rod photoreceptors following Ivt injection. We next quantified the relative performance of these variants by utilizing a construct containing the photoreceptor-specific human rhodopsin kinase (hGRK1) promoter driving mCherry in C57Bl/6J mice (14,57). Mice were injected intravitreally with 4 ϫ 10 10 vg (high dose) or 4 ϫ 10 9 vg (low dose) or subretinally with 1 ϫ 10 10 vg (high dose) or 2 ϫ 10 9 vg (low dose).…”

Section: Aav2 Y-f and Y-f؉t-v Variants Bind Hs Aav2-based Variants Cmentioning

confidence: 99%

“…However, the majority of inherited retinal diseases are caused by defects in photoreceptors, highlighting the need to identify serotypes capable of transducing this cell type. We and others have shown that various subretinally delivered AAV serotypes are capable of efficient transduction of photoreceptors in nonhuman primates (NHP) (14)(15)(16)(17)(18)(19). However, subretinal injection of AAV2 under the fovea of some LCA2 patients led to central retinal thinning and loss of visual acuity (20).…”

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confidence: 99%

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Impact of Heparan Sulfate Binding on Transduction of Retina by Recombinant Adeno-Associated Virus Vectors

Boye

Bennett

Scalabrino

et al. 2016

J Virol

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Adeno-associated viruses (AAVsA deno-associated viruses (AAVs) are nonpathogenic, singlestranded packaging DNA dependoparvoviruses within the family Parvoviridae. As the genus name implies, wild-type (WT) AAV is dependent on helper viruses, such as those in the Adenoviridae and Herpesviridae families, for replication. For its safety and the availability of a wide variety of naturally occurring serotypes displaying various tissue tropisms, recombinant AAV (rAAV) has found wide utility as both a gene therapy vector and biotechnological tool (1). Capsid crystal structures also have been determined for many of the AAV serotypes (2-9), leading to a revolution in identifying the structural determinants of receptor attachment, tropism, and transduction efficiency and, by extension, the ability to modify the capsid to generate variants with desired transduction profiles.One of the major clinical applications of AAV is as a gene therapy vector for the treatment of blindness. The eye is a particularly well-suited organ for gene therapy due to its small size, compartmentalization, and immune-privileged status (10). Clinical trials for RPE65-Leber congenital amaurosis (LCA2) demonstrate the ability to deliver a therapeutic transgene to the retinal pigment epithelium (RPE), thereby restoring retinal function and visually evoked behavior to patients (11-13). However, the majority of inherited retinal diseases are caused by defects in photoreceptors, highlighting the need to identify serotypes capable of transducing this cell type. We and others have shown that various subretinally delivered AAV serotypes are capable of efficient transduction of photoreceptors in nonhuman primates (NHP) (14-19). However, subretinal injection of AAV2 under the fovea of some LCA2 patients led to central retinal thinning and loss of visual acuity (20). Similar decreases in retinal thickness were ob-

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The new landscape of retinal gene therapy

Pennesi

2020

American J of Med Genetics Pt C

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Novel therapeutics for inherited retinal dystrophies (IRDs) have rapidly evolved since groundbreaking clinical trials for LCA due to RPE65 mutations led to the first FDAapproved in vivo gene therapy. Since then, advancements in viral vectors have led to more efficient AAV transduction and developed other viral vectors for gene augmentation therapy of large gene targets. Furthermore, significant developments in gene editing and RNA modulation technologies have introduced novel capabilities for treatment of autosomal dominant diseases, intronic mutations, and/or large genes otherwise unable to be treated with current viral vectors. We highlight strategies currently being evaluated in gene therapy clinical trials and promising preclinical developments for IRDs.

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The Human Rhodopsin Kinase Promoter in an AAV5 Vector Confers Rod- and Cone-Specific Expression in the Primate Retina

Cited by 97 publications

References 68 publications

AAV-Mediated Gene Therapy in the Guanylate Cyclase (RetGC1/RetGC2) Double Knockout Mouse Model of Leber Congenital Amaurosis

AAV-Mediated Gene Therapy in the Guanylate Cyclase (RetGC1/RetGC2) Double Knockout Mouse Model of Leber Congenital Amaurosis

Impact of Heparan Sulfate Binding on Transduction of Retina by Recombinant Adeno-Associated Virus Vectors

The new landscape of retinal gene therapy

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