Retinal Structure and Function in Achromatopsia: Implications for Gene Therapy

Overview

Journal Ophthalmology

Publisher Elsevier

Specialty Ophthalmology

Date 2013 Oct 24

PMID 24148654

Citations 91

Authors

Venki Sundaram

Caroline Wilde

Jonathan Aboshiha

Jill Cowing

Colin Han

Christopher S Langlo

Ravinder Chana

Alice E Davidson

Panagiotis I Sergouniotis

James W Bainbridge

Robin R Ali

Alfredo Dubra

Gary Rubin

Andrew R Webster

Anthony T Moore

Marko Nardini

Joseph Carroll

Michel Michaelides

Affiliations

Soon will be listed here.

Abstract

Purpose: To characterize retinal structure and function in achromatopsia (ACHM) in preparation for clinical trials of gene therapy.

Design: Cross-sectional study.

Participants: Forty subjects with ACHM.

Methods: All subjects underwent spectral domain optical coherence tomography (SD-OCT), microperimetry, and molecular genetic testing. Foveal structure on SD-OCT was graded into 5 distinct categories: (1) continuous inner segment ellipsoid (ISe), (2) ISe disruption, (3) ISe absence, (4) presence of a hyporeflective zone (HRZ), and (5) outer retinal atrophy including retinal pigment epithelial loss. Foveal and outer nuclear layer (ONL) thickness was measured and presence of hypoplasia determined.

Main Outcome Measures: Photoreceptor appearance on SD-OCT imaging, foveal and ONL thickness, presence of foveal hypoplasia, retinal sensitivity and fixation stability, and association of these parameters with age and genotype.

Results: Forty subjects with a mean age of 24.9 years (range, 6-52 years) were included. Disease-causing variants were found in CNGA3 (n = 18), CNGB3 (n = 15), GNAT2 (n = 4), and PDE6C (n = 1). No variants were found in 2 individuals. In all, 22.5% of subjects had a continuous ISe layer at the fovea, 27.5% had ISe disruption, 20% had an absent ISe layer, 22.5% had an HRZ, and 7.5% had outer retinal atrophy. No significant differences in age (P = 0.77), mean retinal sensitivity (P = 0.21), or fixation stability (P = 0.34) across the 5 SD-OCT categories were evident. No correlation was found between age and foveal thickness (P = 0.84) or between age and foveal ONL thickness (P = 0.12).

Conclusions: The lack of a clear association of disruption of retinal structure or function in ACHM with age suggests that the window of opportunity for intervention by gene therapy is wider in some individuals than previously indicated. Therefore, the potential benefit for a given subject is likely to be better predicted by specific measurement of photoreceptor structure rather than simply by age. The ability to directly assess cone photoreceptor preservation with SD-OCT and/or adaptive optics imaging is likely to prove invaluable in selecting subjects for future trials and measuring the trials' impact.

Citing Articles

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Longitudinal Imaging of the Foveal Cone Mosaic in CNGA3-Associated Achromatopsia.

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