AI Article Synopsis

  • The study aims to detail the eye-related symptoms in patients with sialidosis type I caused by a deficiency in the enzyme neuraminidase 1, while also introducing a new method for analyzing the 'macular cherry-red spot' using advanced imaging techniques.
  • Seven patients with sialidosis type I and one with galactosialidosis underwent comprehensive eye exams, revealing that all had a distinct macular cherry-red spot, good corneal clarity, and varied visual acuity.
  • Results showed that most patients maintained decent vision into adulthood, although those with optic atrophy had poorer outcomes; increased reflectivity in macular imaging was observed across the board, providing new insights for monitoring disease progression.

Article Abstract

Aim: To describe the ophthalmologic findings on the largest cohort of patients with sialidosis type I due to deficiency of the lysosomal sialidase, neuraminidase 1 (NEU1) and to introduce a quantitative neuroretinal image analysis approach to the associated 'macular cherry-red spot'.

Methods: Seven patients with sialidosis type I (mutations in ) and one with galactosialidosis (mutations in ) were included. All patients underwent detailed ophthalmological examinations. The reflectivity of macular optical coherence tomography (OCT) was measured using greyscale analysis (Fiji) and compared with age-matched healthy volunteers. Four patients were evaluated over a time of 1.5+0.5 years.

Results: The mean age of the patients at their first visit was 27.5+9.8 years. All patients had a macular cherry-red spot, clear corneas and visually non-significant lenticular opacities. The mean visual acuity was LogMar 0.4 (20/50)+0.4 (20/20 to 20/125). Six patients had good visual function. Optic atrophy was present in two individuals with reduced acuity. A significant increase in macular reflectivity was present in all patients compared to age-matched controls (p<0.0001).

Conclusion: Most of our patients (75%) have preserved visual acuity, even in adulthood. The presence of optic atrophy is associated with poor visual acuity. Increased macular reflectivity by OCT greyscale measurements is noted in all patients, although the underlying biological basis is unknown. These findings complement the current methods for examining and monitoring disease progression, especially in patients for whom visualisation of the cherry-red spot is not entirely clear.

Trial Registration Number: NCT00029965.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8142419PMC
http://dx.doi.org/10.1136/bjophthalmol-2020-316826DOI Listing

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