Development of an optimized AAV2/5 gene therapy vector for Leber congenital amaurosis owing to defects in RPE65.

A Georgiadis,Y Duran,B Sünkel-Laing,L Abelleira-Hervas,M Michaelides,E Cristante,J Ribeiro,A J Smith,A Gonzalez-Cordero,S Fourali,S J Robbie,J W B Bainbridge,R R Ali

doi:10.1038/gt.2016.66

A Georgiadis, Y Duran + Show 11 more

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https://doi.org/10.1038/gt.2016.66

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Journal: Gene therapy	Publication Date: Sep 22, 2016
Citations: 67	License type: CC BY 4.0

Affiliation: University College London, Moorfields Eye Hospital

Abstract

Leber congenital amaurosis is a group of inherited retinal dystrophies that cause severe sight impairment in childhood; RPE65-deficiency causes impaired rod photoreceptor function from birth and progressive impairment of cone photoreceptor function associated with retinal degeneration. In animal models of RPE65 deficiency, subretinal injection of recombinant adeno-associated virus (AAV) 2/2 vectors carrying RPE65 cDNA improves rod photoreceptor function, and intervention at an early stage of disease provides sustained benefit by protecting cone photoreceptors against retinal degeneration. In affected humans, administration of these vectors has resulted to date in relatively modest improvements in photoreceptor function, even when retinal degeneration is comparatively mild, and the duration of benefit is limited by progressive retinal degeneration. We conclude that the demand for RPE65 in humans is not fully met by current vectors, and predict that a more powerful vector will provide more durable benefit. With this aim we have modified the original AAV2/2 vector to generate AAV2/5-OPTIRPE65. The new configuration consists of an AAV vector serotype 5 carrying an optimized hRPE65 promoter and a codon-optimized hRPE65 gene. In mice, AAV2/5-OPTIRPE65 is at least 300-fold more potent than our original AAV2/2 vector.

Highlights

Leber congenital amaurosis (LCA) is a group of inherited retinal dystrophies that cause severe sight impairment in childhood.[1]Mutations in the gene encoding the 65 kDa retinal pigment epithelium–specific retinoid isomerase (RPE65) are responsible in upto 10% of affected individuals
Following subretinal injection of AAV2/8 vectors into wild-type (WT) mice, we found that the optimized promoter (NA65p) led to a marked increase in expression of green fluorescent protein (GFP) in RPE cells (Figure 1), compared with the original promoter
Comparison of GFP expression in the RPE driven by NA65p with that of the constitutive promoter CBA in mice in vivo was performed, following dissection of RPE/choroid from injected eyes and demonstrated significantly higher GFP messengerRNA levels driven by NA65p (P o 0.001; Supplementary Figure S2)

Summary

Introduction

Leber congenital amaurosis (LCA) is a group of inherited retinal dystrophies that cause severe sight impairment in childhood.[1]Mutations in the gene encoding the 65 kDa retinal pigment epithelium–specific retinoid isomerase (RPE65) (locus name LCA2; OMIM #204100) are responsible in upto 10% of affected individuals. The optimized vector AAV2/5-OPTIRPE65 improves retinal function with at least 300-fold greater potency.

Results

Conclusion