Patients and animal models of CNGβ1-deficient retinitis pigmentosa support gene augmentation approach.

Simon M Petersen-Jones,Vince Chiodo,Paige A Winkler,Winston Lee,Laurence M Occelli,Janet R Sparrow,Christian Schön,Jenina E Capasso,Stylianos Michalakis,William W Hauswirth,Sanford L Boye,Elvir Becirovic,Mathias W Seeliger,Mai Tsukikawa,Stephen H Tsang,Alex V Levin

doi:10.1172/jci95161

Abstract

Retinitis pigmentosa (RP) is a major cause of blindness that affects 1.5 million people worldwide. Mutations in cyclic nucleotide-gated channel β 1 (CNGB1) cause approximately 4% of autosomal recessive RP. Gene augmentation therapy shows promise for treating inherited retinal degenerations; however, relevant animal models and biomarkers of progression in patients with RP are needed to assess therapeutic outcomes. Here, we evaluated RP patients with CNGB1 mutations for potential biomarkers of progression and compared human phenotypes with those of mouse and dog models of the disease. Additionally, we used gene augmentation therapy in a CNGβ1-deficient dog model to evaluate potential translation to patients. CNGB1-deficient RP patients and mouse and dog models had a similar phenotype characterized by early loss of rod function and slow rod photoreceptor loss with a secondary decline in cone function. Advanced imaging showed promise for evaluating RP progression in human patients, and gene augmentation using adeno-associated virus vectors robustly sustained the rescue of rod function and preserved retinal structure in the dog model. Together, our results reveal an early loss of rod function in CNGB1-deficient patients and a wide window for therapeutic intervention. Moreover, the identification of potential biomarkers of outcome measures, availability of relevant animal models, and robust functional rescue from gene augmentation therapy support future work to move CNGB1-RP therapies toward clinical trials.

Highlights

Retinitis pigmentosa (RP) is a genetically heterogeneous cause of blindness, affecting approximately 1 in 4,000 individuals [1]
Three of the mutations had been previously described in RP type 45 (RP45) patients: c.2284C>T, p.Arg762Cys [16, 30]; c.1896C>A, p.Cys632* [15]; c.3150delG; and p.Phe1051Leufs*12 [15, 22]
Humans with CNGB1-related RP [12, 13, 16, 23], mice (Cngb1-X26) [27], and Cngb1–/– dogs with mutations that spare expression of the alternatively expressed GARP subunits share a similar phenotype characterized by a lack of rod-mediated retinal function from an early age, followed by a slowly progressive age-related loss of cone function and, in humans, constriction of visual fields

Summary

Introduction

Retinitis pigmentosa (RP) is a genetically heterogeneous cause of blindness, affecting approximately 1 in 4,000 individuals [1]. Mutations for nonsyndromic RP have been identified in over 80 different genes (RetNet, Retinal Information Network) [2]. Patients develop attenuation of superficial retinal blood vessels, optic disc pallor, and characteristic “bone-spicule” pigment clumping in the midperipheral retina [1]. There is no cure for RP, gene therapy approaches for other inherited retinal degenerations are showing promising results in phase I and II clinical trials [3,4,5,6,7,8,9,10,11].

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Results

Conclusion