Rare coding mutations identify 36 large-effect risk genes in obsessive-compulsive disorder and chronic tic disorders

  1. Belinda Wang
  2. Matthew N. Tran
  3. Sheng Wang
  4. Yuting Liu
  5. Emily Olfson
  6. George Wang
  7. Nawei Sun
  8. Jeanselle Dea
  9. Charles Ochieng’ Olwal
  10. Lyvia Bertolace
  11. Michael H. Bloch
  12. Carolina Cappi
  13. Yi-Chieh Chang
  14. Denise Chavira
  15. Barbara J. Coffey
  16. Martha J. Falkenstein
  17. Adam C. Frank
  18. Martin E. Franklin
  19. Stephanie Garayalde
  20. Helena Garrido
  21. Marco Grados
  22. Rami Hatem
  23. Allyna-London Howell
  24. Starlette Khim
  25. Jennie M. Kuckertz
  26. Mindy M. Le
  27. Allison Libby
  28. Ryan J. McCarty
  29. Mary E. McNamara
  30. Daniel McNeil
  31. Euripedes C. Miguel
  32. Cara Nasello
  33. Binh Nguyen
  34. Tenzin Norbu
  35. Lauren Oh
  36. Ashley Ordway
  37. Catherine Paciotti
  38. Viviana A. Peskin
  39. Christopher Pittenger
  40. Helen Blair Simpson
  41. Heather Simpson Martin
  42. Max A. Tischfield
  43. Jinchuan Xing
  44. Jessica J. Zakrzewski
  45. Tourette International Collaborative Genetics (TIC Genetics)
  46. Andrea Dietrich
  47. Donald L. Gilbert
  48. Pieter J. Hoekstra
  49. Young Shin Kim
  50. Samuel Kuperman
  51. Alyssa Rosen
  52. Samuel H. Zinner
  53. Mehdi Bouhaddou
  54. Robert A. King
  55. Guy Rouleau
  56. Kerry J. Ressler
  57. Carol A. Mathews
  58. Nevan J. Krogan
  59. Nenad Sestan
  60. Jay A. Tischfield
  61. A. Moses Lee
  62. Gary A. Heiman
  63. Thomas V. Fernandez
  64. A. Jeremy Willsey
  65. Matthew W. State
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Abstract

Obsessive-compulsive disorder (OCD) and chronic tic disorders (CTD) are highly heritable. Recent progress in OCD genomics has highlighted small-effect common alleles. Rare mutations have previously been found to carry large risks for OCD and CTD but only four high-confidence (hc) genes have been identified. We analyzed whole-exome sequencing data from 3,964 individuals with OCD, CTD, or both, including 2,418 trios. We find an excess in cases of de novo and rare protein-damaging mutations and identify 36 hc genes (false discovery rate [FDR] < 0.1), four of which overlap with OCD GWAS loci. Risk genes are shared among OCD, CTD, autism spectrum disorder, and other neurodevelopmental conditions. Transcriptomic and network analyses highlight mechanistic convergence and increased risk gene expression in postnatal cerebellum and pre- and postnatal cortex and striatum. Dozens of large-effect OCDCTD genes offer insights into pathogenesis and a path forward for illuminating pathophysiology and identifying novel treatment targets.

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