Author:
Abu-Safieh Leen,Alrashed May,Anazi Shamsa,Alkuraya Hisham,Khan Arif O.,Al-Owain Mohammed,Al-Zahrani Jawahir,Al-Abdi Lama,Hashem Mais,Al-Tarimi Salwa,Sebai Mohammed-Adeeb,Shamia Ahmed,Ray-zack Mohamed D.,Nassan Malik,Al-Hassnan Zuhair N.,Rahbeeni Zuhair,Waheeb Saad,Alkharashi Abdullah,Abboud Emad,Al-Hazzaa Selwa A.F.,Alkuraya Fowzan S.
Abstract
Retinal dystrophy (RD) is a heterogeneous group of hereditary diseases caused by loss of photoreceptor function and contributes significantly to the etiology of blindness globally but especially in the industrialized world. The extreme locus and allelic heterogeneity of these disorders poses a major diagnostic challenge and often impedes the ability to provide a molecular diagnosis that can inform counseling and gene-specific treatment strategies. In a large cohort of nearly 150 RD families, we used genomic approaches in the form of autozygome-guided mutation analysis and exome sequencing to identify the likely causative genetic lesion in the majority of cases. Additionally, our study revealed six novel candidate disease genes (C21orf2, EMC1, KIAA1549, GPR125, ACBD5, and DTHD1), two of which (ACBD5 and DTHD1) were observed in the context of syndromic forms of RD that are described for the first time.
Publisher
Cold Spring Harbor Laboratory
Subject
Genetics(clinical),Genetics
Cited by
221 articles.
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