Exome Sequencing Reveals a Novel Splice Site Variant in HUWE1 Gene in Patients with Suspected Say-Meyer Syndrome

Overview

Journal Eur J Med Genet

Publisher Elsevier

Specialty Genetics

Date 2019 Feb 25

PMID 30797980

Citations 10

Authors

Babylakshmi Muthusamy

Thong T Nguyen

Aravind K Bandari

Salah Basheer

Lakshmi Dhevi N Selvan

Deepshikha Chandel

Jesna Manoj

Srimonta Gayen

Somasekar Seshagiri

Satish Chandra Girimaji

Akhilesh Pandey

Affiliations

Soon will be listed here.

Abstract

Say-Meyer syndrome is a rare and clinically heterogeneous syndrome characterized by trigonocephaly, short stature, developmental delay and hypotelorism. Nine patients with this syndrome have been reported thus far although no causative gene has yet been identified. Here, we report two siblings with clinical phenotypes of Say-Meyer syndrome with moderate to severe intellectual disability and autism spectrum disorder. Cytogenetics and array-based comparative genomic hybridization did not reveal any chromosome abnormalities or copy number alterations. Exome sequencing of the patients revealed a novel X-linked recessive splice acceptor site variant c.145-2A > G in intron 5 of HUWE1 gene in both affected siblings. RT-PCR and sequencing revealed the use of an alternate cryptic splice acceptor site downstream, which led to deletion of six nucleotides resulting loss of two amino acids p.(Cys49-Glu50del) in HUWE1 protein. Deletion of these two amino acids, which are located in a highly conserved region, is predicted to be deleterious and quite likely to affect the function of HUWE1 protein. This is the first report of a potential candidate gene mutation for Say-Meyer syndrome, which was initially described four decades ago.

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