Ophthalmic manifestations of NAA10‐related and NAA15‐related neurodevelopmental syndromes: Analysis of cortical visual impairment and refractive errors

Author:

Patel Rahi1,Park Agnes Y.1,Marchi Elaine1,Gropman Andrea L.23,Whitehead Matthew T.45,Lyon Gholson J.167ORCID

Affiliation:

1. Department of Human Genetics New York State Institute for Basic Research in Developmental Disabilities Staten Island New York USA

2. Department of Neurology George Washington University Washington DC USA

3. Division of Neuroradiology Children's Hospital of Philadelphia Philadelphia Pennsylvania USA

4. Department of Radiology Perelman School of Medicine University of Pennsylvania Philadelphia Pennsylvania USA

5. Division of Neurogenetics and Developmental Pediatrics Children's National Health System Washington DC USA

6. George A. Jervis Clinic New York State Institute for Basic Research in Developmental Disabilities Staten Island New York USA

7. Biology PhD Program, The Graduate Center The City University of New York New York New York USA

Abstract

AbstractNAA10‐related (Ogden syndrome) and NAA15‐related neurodevelopmental syndrome are known to present with varying degrees of intellectual disability, hypotonia, congenital cardiac abnormalities, seizures, and delayed speech and motor development. However, the ophthalmic manifestations of NAA10 and NAA15 variants are not yet fully characterized or understood. This study analyzed the prevalence of six ophthalmic conditions (cortical visual impairment, myopia, hyperopia, strabismus, nystagmus, and astigmatism) in 67 patients with pathogenic (P) or likely pathogenic (LP) variants in the NAA10 cohort (54 inherited, 10 de novo; 65 missense, 2 frameshift) and 19 patients with (L)P variants in the NAA15 cohort (18 de novo; 8 frameshift, 4 missense, 4 nonsense, and 1 splice site). Patients were interviewed virtually or in‐person to collect a comprehensive medical history verified by medical records. These records were then analyzed to calculate the prevalence of these ophthalmic manifestations in each cohort. Analysis revealed a higher prevalence of ophthalmic conditions in our NAA10 cohort compared to existing literature (myopia 25.4% vs. 4.7%; astigmatism 37.3% vs. 13.2%; strabismus 28.4% vs. 3.8%; CVI 22.4% vs. 8.5%, respectively). No statistically significant differences were identified in the prevalence of these conditions between the NAA10 and NAA15 variants. Our study includes novel neuroimaging of 13 NAA10 and 5 NAA15 probands, which provides no clear correlation between globe size and severity of comorbid ophthalmic disease. Finally, anecdotal evidence was compiled to underscore the importance of early ophthalmologic evaluations and therapeutic interventions.

Publisher

Wiley

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