Orphanet Journal of Rare Diseases (Aug 2020)

Onset features and time to diagnosis in Friedreich’s Ataxia

  • Elisabetta Indelicato,
  • Wolfgang Nachbauer,
  • Andreas Eigentler,
  • Matthias Amprosi,
  • Raffaella Matteucci Gothe,
  • Paola Giunti,
  • Caterina Mariotti,
  • Javier Arpa,
  • Alexandra Durr,
  • Thomas Klopstock,
  • Ludger Schöls,
  • Ilaria Giordano,
  • Katrin Bürk,
  • Massimo Pandolfo,
  • Claire Didszdun,
  • Jörg B. Schulz,
  • Sylvia Boesch,
  • on behalf of the EFACTS (European Friedreich’s Ataxia Consortium for Translational Studies)

DOI
https://doi.org/10.1186/s13023-020-01475-9
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 8

Abstract

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Abstract Background In rare disorders diagnosis may be delayed due to limited awareness and unspecific presenting symptoms. Herein, we address the issue of diagnostic delay in Friedreich’s Ataxia (FRDA), a genetic disorder usually caused by homozygous GAA-repeat expansions. Methods Six hundred eleven genetically confirmed FRDA patients were recruited within a multicentric natural history study conducted by the EFACTS (European FRDA Consortium for Translational Studies, ClinicalTrials.gov -Identifier NCT02069509). Age at first symptoms as well as age at first suspicion of FRDA by a physician were collected retrospectively at the baseline visit. Results In 554 of cases (90.7%), disease presented with gait or coordination disturbances. In the others (n = 57, 9.3%), non-neurological features such as scoliosis or cardiomyopathy predated ataxia. Before the discovery of the causal mutation in 1996, median time to diagnosis was 4(IQR = 2–9) years and it improved significantly after the introduction of genetic testing (2(IQR = 1–5) years, p < 0.001). Still, after 1996, time to diagnosis was longer in patients with a) non-neurological presentation (mean 6.7, 95%CI [5.5,7.9] vs 4.5, [4.2,5] years in those with neurological presentation, p = 0.001) as well as in b) patients with late-onset (3(IQR = 1–7) vs 2(IQR = 1–5) years compared to typical onset < 25 years of age, p = 0.03). Age at onset significantly correlated with the length of the shorter GAA repeat (GAA1) in case of neurological onset (r = − 0,6; p < 0,0001), but not in patients with non-neurological presentation (r = − 0,1; p = 0,4). Across 54 siblings’ pairs, differences in age at onset did not correlate with differences in GAA-repeat length (r = − 0,14, p = 0,3). Conclusions In the genetic era, presentation with non-neurological features or in the adulthood still leads to a significant diagnostic delay in FRDA. Well-known correlations between GAA1 repeat length and disease milestones are not valid in case of atypical presentations or positive family history.

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