Identification of a syndrome comprising microcephaly and intellectual disability but not white matter disease associated with a homozygous c.676C>T p.R226W DEAF1 mutation

We evaluated a 13‐year‐old East Pakistani male affected with microcephaly, apparent intellectual disability, hypotonia, and brisk reflexes without spasticity. His parents were first cousins. The patient also had a brother who was similarly affected and died at 10 years due to an accident. Previous S...

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Bibliographic Details
Published in:American journal of medical genetics. Part A 2016-05, Vol.170A (5), p.1330-1332
Main Authors: Gund, Christian, Powis, Zöe, Alcaraz, Wendy, Desai, Sonal, Baranano, Kristin
Format: Article
Language:English
Subjects:
Adolescent
Chromosome Duplication
clinical diagnostic sequencing
consanguinity
DEAF1 protein
Exome
human
Humans
intellectual disability
Intellectual Disability - genetics
Intellectual Disability - physiopathology
Leukoencephalopathies - genetics
Leukoencephalopathies - pathology
Male
microcephaly
Microcephaly - genetics
Microcephaly - physiopathology
Muscle Hypotonia - genetics
Muscle Hypotonia - physiopathology
Mutation
Nuclear Proteins - genetics
Pakistan
Pedigree
Sequence Analysis, DNA
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Summary:We evaluated a 13‐year‐old East Pakistani male affected with microcephaly, apparent intellectual disability, hypotonia, and brisk reflexes without spasticity. His parents were first cousins. The patient also had a brother who was similarly affected and died at 10 years due to an accident. Previous SNP array testing showed a 1.63 Mb duplication at 16p13.11 of uncertain significance along with regions of homozygosity. Exome sequencing identified a known pathogenic homozygous alteration in DEAF1, c.676C>T (p.R226W), in this patient. The alteration had been reported in two individuals from a consanguineous Saudi Arabian family. Both individuals had microcephaly, intellectual disability, hypotonia, feeding difficulties, and poor growth. The patient reported here did not have evidence of white matter disease, as had been reported with prior patients. We conclude that this DEAF1 gene alteration caused this patient's symptoms and that white matter disease should not be considered a obligate feature of this syndrome. © 2016 Wiley Periodicals, Inc.
ISSN:1552-4825
1552-4833
DOI:10.1002/ajmg.a.37580