Frontiers in Neuroscience (Sep 2016)

Targeted re-sequencing approach of candidate genes implicates rare potentially functional variants in Tourette Syndrome etiology

  • John Alexander,
  • Hera Potamianou,
  • Jinchuan Xing,
  • Jinchuan Xing,
  • Li Deng,
  • Li Deng,
  • Iordanis Karagiannidis,
  • Fotis Tsetsos,
  • Petros Drineas,
  • Tárnok Zsanett,
  • Renata Rizzo,
  • Tomasz Wolanczyk,
  • Luca Farkas,
  • Peter Nagy,
  • Urszula Szymanska,
  • Christos Androutsos,
  • Vaia Tsironi,
  • Anastasia Koumoula,
  • Csaba Barta,
  • Paul Sandor,
  • Cathy L. Barr,
  • Cathy L. Barr,
  • Jay Tischfield,
  • Jay Tischfield,
  • Peristera Paschou,
  • Gary Adam Heiman,
  • Gary Adam Heiman,
  • Marianthi Georgitsi,
  • Marianthi Georgitsi

DOI
https://doi.org/10.3389/fnins.2016.00428
Journal volume & issue
Vol. 10

Abstract

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Although the genetic basis of Tourette Syndrome (TS) remains unclear, several candidate genes have been implicated. Using a set of 382 TS individuals of European ancestry we investigated four candidate genes for TS (HDC, SLITRK1, BTBD9 and SLC6A4) in an effort to identify possibly causal variants using a targeted re-sequencing approach by next generation sequencing technology. Identification of possible disease causing variants under different modes of inheritance was performed using the algorithms implemented in VAAST. We prioritized variants using Variant ranker and validated five rare variants via Sanger sequencing in HDC and SLITRK1, all of which are predicted to be deleterious. Intriguingly, one of the identified variants is in linkage disequilibrium with a variant that is included among the top hits of a genome-wide association study tolerance to citalopram treatment, an antidepressant drug with off-label use also in obsessive compulsive disorder. Our findings provide additional evidence for the implication of these two genes in TS susceptibility and the possible role of these proteins in the pathobiology of TS should be revisited.

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