BMC Medical Genetics (Jan 2009)

Genome screen in familial intracranial aneurysm

  • Langefeld Carl,
  • Bailey-Wilson Joan E,
  • Meissner Irene,
  • Hornung Richard,
  • Deka Ranjan,
  • Flaherty Matthew L,
  • Kleindorfer Dawn,
  • Woo Daniel,
  • Anderson Craig,
  • Brown Robert,
  • Sauerbeck Laura,
  • Foroud Tatiana,
  • Rouleau Guy,
  • Connolly E Sander,
  • Lai Dongbing,
  • Koller Daniel L,
  • Huston John,
  • Broderick Joseph P

DOI
https://doi.org/10.1186/1471-2350-10-3
Journal volume & issue
Vol. 10, no. 1
p. 3

Abstract

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Abstract Background Individuals with 1st degree relatives harboring an intracranial aneurysm (IA) are at an increased risk of IA, suggesting genetic variation is an important risk factor. Methods Families with multiple members having ruptured or unruptured IA were recruited and all available medical records and imaging data were reviewed to classify possible IA subjects as definite, probable or possible IA or not a case. A 6 K SNP genome screen was performed in 333 families, representing the largest linkage study of IA reported to date. A 'narrow' (n = 705 definite IA cases) and 'broad' (n = 866 definite or probable IA) disease definition were used in multipoint model-free linkage analysis and parametric linkage analysis, maximizing disease parameters. Ordered subset analysis (OSA) was used to detect gene × smoking interaction. Results Model-free linkage analyses detected modest evidence of possible linkage (all LOD Conclusion These data suggest it is unlikely that there is a single common variant with a strong effect in the majority of the IA families. Rather, it is likely that multiple genetic and environmental risk factors contribute to the susceptibility for intracranial aneurysms.