PLoS ONE (Jan 2017)

Phenome-wide association study using research participants' self-reported data provides insight into the Th17 and IL-17 pathway.

  • Margaret G Ehm,
  • Jennifer L Aponte,
  • Mathias N Chiano,
  • Laura M Yerges-Armstrong,
  • Toby Johnson,
  • Jonathan N Barker,
  • Suzanne F Cook,
  • Akanksha Gupta,
  • David A Hinds,
  • Li Li,
  • Matthew R Nelson,
  • Michael A Simpson,
  • Chao Tian,
  • Linda C McCarthy,
  • Deepak K Rajpal,
  • Dawn M Waterworth

DOI
https://doi.org/10.1371/journal.pone.0186405
Journal volume & issue
Vol. 12, no. 11
p. e0186405

Abstract

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A phenome-wide association study of variants in genes in the Th17 and IL-17 pathway was performed using self-reported phenotypes and genetic data from 521,000 research participants of 23andMe. Results replicated known associations with similar effect sizes for autoimmune traits illustrating self-reported traits can be a surrogate for clinically assessed conditions. Novel associations controlling for a false discovery rate of 5% included the association of the variant encoding p.Ile684Ser in TYK2 with increased risk of tonsillectomy, strep throat occurrences and teen acne, the variant encoding p.Arg381Gln in IL23R with a decrease in dandruff frequency, the variant encoding p.Asp10Asn in TRAF3IP2 with risk of male-pattern balding, and the RORC regulatory variant (rs4845604) with protection from allergies. This approach enabled rapid assessment of association with a wide variety of traits and investigation of traits with limited reported associations to overlay meaningful phenotypic context on the range of conditions being considered for drugs targeting this pathway.