De Novo Truncating Variants in SON Cause Intellectual Disability, Congenital Malformations, and Failure to Thrive.

Authors :: Tokita MJ
Braxton AA
Shao Y
Lewis AM
Vincent M
Küry S
Besnard T
Isidor B
Latypova X
Bézieau S
Liu P
Motter CS
Melver CW
Robin NH
Infante EM
McGuire M
El-Gharbawy A
Littlejohn RO
McLean SD
Bi W
Bacino CA
Lalani SR
Scott DA
Eng CM
Yang Y
Schaaf CP
Walkiewicz MA
Source :: American journal of human genetics [Am J Hum Genet] 2016 Sep 01; Vol. 99 (3), pp. 720-727. Date of Electronic Publication: 2016 Aug 18.
Publication Year :: 2016
Abstract: SON is a key component of the spliceosomal complex and a critical mediator of constitutive and alternative splicing. Additionally, SON has been shown to influence cell-cycle progression, genomic integrity, and maintenance of pluripotency in stem cell populations. The clear functional relevance of SON in coordinating essential cellular processes and its presence in diverse human tissues suggests that intact SON might be crucial for normal growth and development. However, the phenotypic effects of deleterious germline variants in SON have not been clearly defined. Herein, we describe seven unrelated individuals with de novo variants in SON and propose that deleterious variants in SON are associated with a severe multisystem disorder characterized by developmental delay, persistent feeding difficulties, and congenital malformations, including brain anomalies.<br /> (Copyright © 2016 American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Subjects :: Adolescent
Brain abnormalities
Child
Child, Preschool
DNA-Binding Proteins chemistry
Exome genetics
Female
Humans
Male
Minor Histocompatibility Antigens chemistry
Pedigree
Young Adult
Congenital Abnormalities genetics
DNA-Binding Proteins genetics
Developmental Disabilities genetics
Failure to Thrive genetics
Intellectual Disability genetics
Minor Histocompatibility Antigens genetics
Sequence Deletion genetics

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