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HUWE1 variants cause dominant X-linked intellectual disability: a clinical study of 21 patients.

Authors :
Moortgat S
Berland S
Aukrust I
Maystadt I
Baker L
Benoit V
Caro-Llopis A
Cooper NS
Debray FG
Faivre L
Gardeitchik T
Haukanes BI
Houge G
Kivuva E
Martinez F
Mehta SG
Nassogne MC
Powell-Hamilton N
Pfundt R
Rosello M
Prescott T
Vasudevan P
van Loon B
Verellen-Dumoulin C
Verloes A
Lippe CV
Wakeling E
Wilkie AOM
Wilson L
Yuen A
Study D
Low KJ
Newbury-Ecob RA
Source :
European journal of human genetics : EJHG [Eur J Hum Genet] 2018 Jan; Vol. 26 (1), pp. 64-74. Date of Electronic Publication: 2017 Nov 27.
Publication Year :
2018

Abstract

Whole-gene duplications and missense variants in the HUWE1 gene (NM_031407.6) have been reported in association with intellectual disability (ID). Increased gene dosage has been observed in males with non-syndromic mild to moderate ID with speech delay. Missense variants reported previously appear to be associated with severe ID in males and mild or no ID in obligate carrier females. Here, we report the largest cohort of patients with HUWE1 variants, consisting of 14 females and 7 males, with 15 different missense variants and one splice site variant. Clinical assessment identified common clinical features consisting of moderate to profound ID, delayed or absent speech, short stature with small hands and feet and facial dysmorphism consisting of a broad nasal tip, deep set eyes, epicanthic folds, short palpebral fissures, and a short philtrum. We describe for the first time that females can be severely affected, despite preferential inactivation of the affected X chromosome. Three females with the c.329 G  >  A p.Arg110Gln variant, present with a phenotype of mild ID, specific facial features, scoliosis and craniosynostosis, as reported previously in a single patient. In these females, the X inactivation pattern appeared skewed in favour of the affected transcript. In summary, HUWE1 missense variants may cause syndromic ID in both males and females.

Details

Language :
English
ISSN :
1476-5438
Volume :
26
Issue :
1
Database :
MEDLINE
Journal :
European journal of human genetics : EJHG
Publication Type :
Academic Journal
Accession number :
29180823
Full Text :
https://doi.org/10.1038/s41431-017-0038-6