Scientific Reports (Sep 2021)

Characterization of SSBP1-related optic atrophy and foveopathy

  • Isabelle Meunier,
  • Béatrice Bocquet,
  • Sabine Defoort-Dhellemmes,
  • Vasily Smirnov,
  • Carl Arndt,
  • Marie Christine Picot,
  • Hélène Dollfus,
  • Majida Charif,
  • Isabelle Audo,
  • Hélèna Huguet,
  • Xavier Zanlonghi,
  • Guy Lenaers

DOI
https://doi.org/10.1038/s41598-021-98150-1
Journal volume & issue
Vol. 11, no. 1
pp. 1 – 9

Abstract

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Abstract Dominant optic atrophy (DOA) is genetically heterogeneous and most commonly caused by mutations in OPA1. To distinguish between the classical OPA1-related and the recently identified SSBP1-related DOAs, the retina and fovea of 27 patients carrying the SSBP1 p.Arg38Gln variant were scrutinized using 20° × 20° macular cube and 30° and 55° field fundus autofluorescence photographs. Age of onset, visual acuity, retinal nerve fiber layer and macular thicknesses were recorded. Three SSBP1-patients were asymptomatic, 10 had isolated DOA, and 12 had a combined DOA plus foveopathy. The foveopathy, with a tiny defect of the ellipsoid and interdigitation lines, was similar in all patients, independent of age. There were no significant statistical differences in terms of visual acuity and SD-OCT measurements between patients with isolated DOA (mean visual acuity in decimals: 0.54 ± 0.41) and those with combined foveopathy (0.50 ± 0.23). Two patients over 50 years of age developed a progressive rod-cone dystrophy, leading to severe visual impairment. SSBP1-related DOA shares similarities with OPA1-related DOA with an incomplete penetrance and an early childhood visual impairment. Nevertheless, the presence of a congenital foveopathy with no impact on visual acuity is a major criterion to distinguish SSBP1 cases and orient the appropriate genetic analysis.