Deep Phenotyping of PDE6C-Associated Achromatopsia

To perform deep phenotyping of subjects with PDE6C achromatopsia and examine disease natural history. Eight subjects with disease-causing variants in PDE6C were assessed in detail, including clinical phenotype, best-corrected visual acuity, fundus autofluorescence, and optical coherence tomography....

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Published in:Investigative ophthalmology & visual science 2019-12, Vol.60 (15), p.5112-5123
Main Authors: Georgiou, Michalis, Robson, Anthony G, Singh, Navjit, Pontikos, Nikolas, Kane, Thomas, Hirji, Nashila, Ripamonti, Caterina, Rotsos, Tryfon, Dubra, Alfredo, Kalitzeos, Angelos, Webster, Andrew R, Carroll, Joseph, Michaelides, Michel
Format: Article
Language:English
Subjects:
Adolescent
Adult
Child
Color Vision - physiology
Color Vision Defects - diagnosis
Color Vision Defects - genetics
Color Vision Defects - metabolism
Cyclic Nucleotide Phosphodiesterases, Type 6 - genetics
Cyclic Nucleotide Phosphodiesterases, Type 6 - metabolism
Electroretinography
Eye Proteins - genetics
Eye Proteins - metabolism
Female
Follow-Up Studies
Forecasting
Genetics
Humans
Male
Middle Aged
Ophthalmoscopy
Phenotype
Tomography, Optical Coherence - methods
Visual Acuity
Young Adult
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Summary:To perform deep phenotyping of subjects with PDE6C achromatopsia and examine disease natural history. Eight subjects with disease-causing variants in PDE6C were assessed in detail, including clinical phenotype, best-corrected visual acuity, fundus autofluorescence, and optical coherence tomography. Six subjects also had confocal and nonconfocal adaptive optics scanning light ophthalmoscopy, axial length, international standard pattern and full-field electroretinography (ERG), short-wavelength flash (S-cone) ERGs, and color vision testing. All subjects presented with early-onset nystagmus, decreased best-corrected visual acuity, light sensitivity, and severe color vision loss, and five of them had high myopia. We identified three novel disease-causing variants and provide phenotype data associated with nine variants for the first time. No subjects had foveal hypoplasia or residual ellipsoid zone (EZ) at the foveal center; one had an absent EZ, three had a hyporeflective zone, and four had outer retinal atrophy. The mean width of the central EZ lesion on optical coherence tomography at baseline was 1923 μm. The mean annual increase in EZ lesion size was 48.3 μm. Fundus autofluorescence revealed a central hypoautofluorescence with a surrounding ring of increased signal (n = 5). The mean hypoautofluorescent area at baseline was 3.33 mm2 and increased in size by a mean of 0.13 mm2/year. Nonconfocal adaptive optics scanning light ophthalmoscopy revealed residual foveal cones in only one of two cases. Full-field ERGs were consistent with severe generalized cone system dysfunction but with relative preservation of S-cone sensitivity. PDE6C retinopathy is a severe cone dysfunction syndrome often presenting as typical achromatopsia but without foveal hypoplasia. Myopia and slowly progressive maculopathy are common features. There are few (if any) residual foveal cones for intervention in older adults.
ISSN:1552-5783
0146-0404
1552-5783
DOI:10.1167/iovs.19-27761