Androgens mediate sexual dimorphism in Pilarowski-Bjornsson Syndrome

  1. Kimberley Jade Anderson
  2. Eirny Tholl Thorolfsdottir
  3. Ilana M. Nodelman
  4. Sara Tholl Halldorsdottir
  5. Stefania Benonisdottir
  6. Malak Alghamdi
  7. Naif Almontashiri
  8. Brenda J. Barry
  9. Matthias Begemann
  10. Jacquelyn F. Britton
  11. Sarah Burke
  12. Benjamin Cogne
  13. Ana S.A. Cohen
  14. Carles de Diego Boguñá
  15. Evan E. Eichler
  16. Elizabeth C. Engle
  17. Jill A. Fahrner
  18. Laurence Faivre
  19. Mélanie Fradin
  20. Nico Fuhrmann
  21. Christine W. Gao
  22. Gunjan Garg
  23. Dagmar Grečmalová
  24. Mina Grippa
  25. Jacqueline R. Harris
  26. Kendra Hoekzema
  27. Tova Hershkovitz
  28. Sydney Hubbard
  29. Katrien Janssens
  30. Julie A. Jurgens
  31. Stanislav Kmoch
  32. Cordula Knopp
  33. Meral Aktas Koptagel
  34. Farah A. Ladha
  35. Pablo Lapunzina
  36. Tobias Lindau
  37. Marije Meuwissen
  38. Andreina Minicucci
  39. Emily Neuhaus
  40. Mathilde Nizon
  41. Lenka Nosková
  42. Kristen Park
  43. Chirag Patel
  44. Rolph Pfundt
  45. Pankaj Prasun
  46. Nils Rahner
  47. Nathaniel H. Robin
  48. Carey Ronspies
  49. Jasmin Roohi
  50. Jill Rosenfeld
  51. Margarita Saenz
  52. Carol Saunders
  53. Zornitza Stark
  54. Isabelle Thiffault
  55. Sarah Thull
  56. Danita Velasco
  57. Clara Velmans
  58. Jolijn Verseput
  59. Antonio Vitobello
  60. Tianyun Wang
  61. Karin Weiss
  62. Ingrid M. Wentzensen
  63. Genay Pilarowski
  64. Thor Eysteinsson
  65. Madelyn Gillentine
  66. Kári Stefánsson
  67. Agnar Helgason
  68. Gregory D. Bowman
  69. Hans Tomas Bjornsson
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Abstract

Sex-specific penetrance in autosomal dominant Mendelian conditions is largely understudied. The neurodevelopmental disorder Pilarowski-Bjornsson syndrome (PILBOS) was initially described in females. Here, we describe the clinical and genetic characteristics of the largest PILBOS cohort to date, showing that both sexes can exhibit PILBOS features, although males are overrepresented. A mouse model carrying a human-derived Chd1 missense variant ( Chd1 R 616 Q /+ ) displays female-restricted phenotypes, including growth deficiency, anxiety and hypotonia. Orchiectomy unmasks a growth deficiency phenotype in male Chd1 R 616 Q /+ mice, while testosterone rescues the phenotype in females, implicating androgens in phenotype modulation. In the gnomAD and UK Biobank databases, rare missense variants in CHD1 are overrepresented in males, supporting a male protective effect. We identify 33 additional highly constrained autosomal genes with missense variant overrepresentation in males. Our results support androgen-regulated sexual dimorphism in PILBOS and open novel avenues to understand the mechanistic basis of sexual dimorphism in other autosomal Mendelian disorders.

Graphical Abstract

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