DDX3X syndrome: a multicenter genotype-phenotype study

  1. Emanuele G. Coci
  2. Christoph G.W. Gertzen
  3. Pilar Chacon Millan
  4. Maria Daniela D´Agostino
  5. Laura Russell
  6. Mouna Benamor
  7. Alberto Fernández-Jaén
  8. Ana Jimenez de Domingo
  9. Lenka Noskova
  10. Martin Magner
  11. Sumit Parikh
  12. Kimberly A Chapman
  13. Himanshu Goel
  14. Enrico Bertini
  15. Ginevra Zanni
  16. Ayman W. El-Hattab
  17. Arif Khan
  18. David Amor
  19. A. Micheil Innes
  20. Scott McLeod
  21. Vanesa López-González
  22. Maria J. Ballesta-Martinez
  23. Nino Spataro
  24. Carmen Manso
  25. Maria Piccione
  26. Emanuela Salzano
  27. Myriam Srour
  28. Sarah Alsubhi
  29. Deborah Renaud
  30. Martina Baethmann
  31. Mathias Wagner
  32. Pablo Prieto Matos
  33. Jill A. Rosenfeld
  34. Daryl A. Scott
  35. Syed A. Ahmed
  36. Kristyn L. Rawson
  37. Fróði Joensen
  38. Marine Tessarech
  39. Clement Proteau
  40. Hong Li
  41. David Michelson
  42. Farzad Hashemi-Gorji
  43. Audrey Putoux
  44. Nicolas Chatron
  45. Fanny Laffargue
  46. Isabelle Creveaux
  47. Rami Abou Jamra
  48. Virginia Pironi
  49. Hilde Van Esch
  50. Cruz Marino Tania
  51. Jessica Ricard
  52. Trine Bjørg Hammer
  53. Irene Valenzuela
  54. Amaia Lasa-Aranzasti
  55. Anna M. Cueto-Gonzalez
  56. Purificación Marín Reina
  57. Francisco Martinez
  58. Milena Mariani
  59. Claudia Ciaccio
  60. Stefano D’arrigo
  61. Annalaura Torella
  62. Vincenzo Nigro
  63. Manuela Morleo
  64. Elsebet Ostergaard
  65. Holger Gohlke
  66. Maria Palomares-Bralo
  67. Fernando Santos-Simarro
0 evaluations Published on
Read the full article Related papers
This article on Sciety

Abstract

DDX3X dysfunction causes an X-linked multisystem disorder with high penetrance and variable expressivity. The phenotypic spectrum spans from learning disability without somatic involvement to profound intellectual disability with severe impairments in the central nervous system and other organs. A few multicenter studies and single case reports have previously highlighted some common phenotypic patterns but were unable to delineate correlations between underlying DDX3X variants and phenotypic findings.From the second largest patient cohort published to date, we analysed clinical, psychometric and diagnostic findings of 52 female and 7 male individuals, harbouring de novo and inherited DDX3X variants. These female patients revealed previously unknown quantitative correlations between variant type and localization and specific phenotypic findings (growth features, epilepsy, brain anomalies, dysmorphisms, motor-focused neurological findings). Moreover, by analysing the in silico folding and RNA binding capability of mutant DDX3X monomers, we were able to delineate novel correlations between DDX3X monomer misfolding grade and phenotypic severity.

Related articles

Related articles are currently not available for this article.