Value of whole exome sequencing for syndromic retinal dystrophy diagnosis in young patients.

[cohen syndrome]

Several retinal dystrophies are associated with syndromic features including such conditions as Bardet-Biedl and Joubert syndromes . Cohen syndrome is an autosomal recessive disorder associated with multiple clinical manifestations including developmental delay , acquired microcephaly , myopia , pigmentary retinopathy , joint hypermobility , truncal obesity , friendly disposition and intermittent neutropenia . In young patients , diagnosis is difficult , because several of the characteristic features may not be present until school age or later years and the intermittent neutropenia is not always detectable .This was a prospective study using whole exome sequencing in syndromic retinal dystrophy . It was undertaken in a hospital and research institute setting .Participants in this study were members of a consanguineous Australian family of Lebanese ethnicity with two siblings with retinal dystrophy , microcephaly and developmental delay .Detailed clinical evaluation was undertaken . Whole exome capture and sequencing of patient genomic DNA samples was followed by sequence alignment , variant detection , comparison and prioritization .Pathogenic variant identification in the disease-causing gene in affected individuals .We identified a novel homozygous deletion leading to a frameshift mutation in VPS 13 B , c .11327 del , p .(Asn 3776 Thrfs *102 ), the disease gene associated with Cohen syndrome .This report emphasizes the value of a broad -based whole exome sequencing approach in disease gene identification in the syndromic retinal dystrophies , where all disease characteristics may not be present in young patients to allow a clinical diagnosis . This facilitates improved prognostic and genetic information for patients and families .