Neurobiology of Disease (Dec 2022)

C9orf72 repeat length might influence clinical sub-phenotypes in dementia patients

  • Theresa König,
  • Raphael Wurm,
  • Tandis Parvizi,
  • Sara Silvaieh,
  • Christoph Hotzy,
  • Hakan Cetin,
  • Sigrid Klotz,
  • Ellen Gelpi,
  • Christian Bancher,
  • Thomas Benke,
  • Peter Dal-Bianco,
  • Michaela Defrancesco,
  • Peter Fischer,
  • Josef Marksteiner,
  • Hedwig Sutterlüty,
  • Gerhard Ransmayr,
  • Reinhold Schmidt,
  • Alexander Zimprich,
  • Elisabeth Stögmann

Journal volume & issue
Vol. 175
p. 105927

Abstract

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Background: C9orf72 repeat expansions have been observed in a wide variety of neurodegenerative disorders. The cut-off between normal and pathogenic alleles is not well established as repeat sizing methods are often semi-quantitative. However, intermediate alleles might influence disease prevalence and phenotype, as seen for other repeat expansion disorders. We aimed to further delineate the prevalence of small, intermediate and expanded C9orf72 alleles and elucidate their potential influence on the disease phenotype. Methods: DNA derived from patients (n = 1804) and healthy individuals (n = 643) was obtained from multiple collectives in Austria. Genotyping was performed using a two-step PCR assay followed by Southern blotting. Results: 3.4% of clinically diagnosed frontotemporal dementia (FTD; n = 5/147) cases and 0.8% of clinically diagnosed Alzheimer's disease (AD; n = 5/602) cases were carriers of a pathological C9orf72 repeat expansion. A significantly earlier disease onset was detected in expansion carriers compared to non-carriers in the FTD and AD cohorts (median 50 years, range 39–64 vs. median 64 years, range 36–92, p = 0.018 and median 63 years, range 54–71 vs. median 74 years, range 45–92, p = 0.006, respectively). C9orf72 intermediate alleles were significantly associated with cerebellar symptoms (p = 0.0004) and sensory deficits in the dementia cohort (p = 0.01). Conclusions: C9orf72 repeat expansion carriers showed earlier disease onset compared to non-carriers with clinical diagnosis of FTD and AD. Furthermore, C9orf72 intermediate repeats might modify the phenotypic expression in dementia.

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