Current Issues in Molecular Biology (Jan 2023)

<i>OPA1</i> Dominant Optic Atrophy: Diagnostic Approach in the Pediatric Population

  • Natalia Arruti,
  • Patricia Rodríguez-Solana,
  • María Nieves-Moreno,
  • Marta Guerrero-Carretero,
  • Ángela del Pozo,
  • Victoria E. F. Montaño,
  • Fernando Santos-Simarro,
  • Emi Rikeros-Orozco,
  • Luna Delgado-Mora,
  • Elena Vallespín,
  • Susana Noval

DOI
https://doi.org/10.3390/cimb45010030
Journal volume & issue
Vol. 45, no. 1
pp. 465 – 478

Abstract

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A clinical and genetic study was conducted with pediatric patients and their relatives with optic atrophy 1 (OPA1) mutations to establish whether there is a genotype–phenotype correlation among the variants detected within and between families. Eleven children with a confirmed OPA1 mutation were identified during the study period. The main initial complaint was reduced visual acuity (VA), present in eight patients of the cohort. Eight of eleven patients had a positive family history of optic atrophy. The mean visual acuity at the start of the study was 0.40 and 0.44 LogMAR in the right and left eye, respectively. At the end of the study, the mean visual acuity was unchanged. Optical coherence tomography during the first visit showed a mean retinal nerve fiber layer thickness of 81.6 microns and 80.5 microns in the right and left eye, respectively; a mean ganglion cell layer of 52.5 and 52.4 microns, respectively, and a mean central macular thickness of 229.5 and 233.5 microns, respectively. The most common visual field defect was a centrocecal scotoma, and nine out of eleven patients showed bilateral temporal disc pallor at baseline. Sequencing of OPA1 showed seven different mutations in the eleven patients, one of which, NM_130837.3: c.1406_1407del (p.Thr469LysfsTer16), has not been previously reported. Early diagnosis of dominant optic atrophy is crucial, both for avoiding unnecessary consultations and/or treatments and for appropriate genetic counseling.

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