Phenotypic expansion in DDX3X - a common cause of intellectual disability in females.

Authors :: Wang X
Posey JE
Rosenfeld JA
Bacino CA
Scaglia F
Immken L
Harris JM
Hickey SE
Mosher TM
Slavotinek A
Zhang J
Beuten J
Leduc MS
He W
Vetrini F
Walkiewicz MA
Bi W
Xiao R
Liu P
Shao Y
Gezdirici A
Gulec EY
Jiang Y
Darilek SA
Hansen AW
Khayat MM
Pehlivan D
Piard J
Muzny DM
Hanchard N
Belmont JW
Van Maldergem L
Gibbs RA
Eldomery MK
Akdemir ZC
Adesina AM
Chen S
Lee YC
Lee B
Lupski JR
Eng CM
Xia F
Yang Y
Graham BH
Moretti P
Source :: Annals of clinical and translational neurology [Ann Clin Transl Neurol] 2018 Sep 15; Vol. 5 (10), pp. 1277-1285. Date of Electronic Publication: 2018 Sep 15 (Print Publication: 2018).
Publication Year :: 2018
Abstract: De novo variants in DDX3X account for 1-3% of unexplained intellectual disability (ID) cases and are amongst the most common causes of ID especially in females. Forty-seven patients (44 females, 3 males) have been described. We identified 31 additional individuals carrying 29 unique DDX3X variants, including 30 postnatal individuals with complex clinical presentations of developmental delay or ID, and one fetus with abnormal ultrasound findings. Rare or novel phenotypes observed include respiratory problems, congenital heart disease, skeletal muscle mitochondrial DNA depletion, and late-onset neurologic decline. Our findings expand the spectrum of DNA variants and phenotypes associated with DDX3X disorders.

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