Clinical exome sequencing for inherited retinal degenerations at a tertiary care center

Author:

Ganapathi Mythily,Thomas-Wilson Amanda,Buchovecky Christie,Dharmadhikari Avinash,Barua Subit,Lee Winston,Ruan Merry Z. C.,Soucy Megan,Ragi Sara,Tanaka Joy,Clark Lorraine N.,Naini Ali B.,Liao Jun,Mansukhani Mahesh,Tsang Stephen,Jobanputra Vaidehi

Abstract

AbstractInherited retinal degenerations are clinically and genetically heterogeneous diseases characterized by progressive deterioration of vision. This study aimed at assessing the diagnostic yield of exome sequencing (ES) for an unselected cohort of individuals with hereditary retinal disorders. It is a retrospective study of 357 unrelated affected individuals, diagnosed with retinal disorders who underwent clinical ES. Variants from ES were filtered, prioritized, and classified using the ACMG recommendations. Clinical diagnosis of the individuals included rod-cone dystrophy (60%), macular dystrophy (20%), cone-rod dystrophy (9%), cone dystrophy (4%) and other phenotypes (7%). Majority of the cases (74%) were singletons and 6% were trios. A confirmed molecular diagnosis was obtained in 24% of cases. In 6% of cases, two pathogenic variants were identified with phase unknown, bringing the potential molecular diagnostic rate to ~ 30%. Including the variants of uncertain significance (VUS), potentially significant findings were reported in 57% of cases. Among cases with a confirmed molecular diagnosis, variants in EYS, ABCA4, USH2A, KIZ, CERKL, DHDDS, PROM1, NR2E3, CNGB1, ABCC6, PRPH2, RHO, PRPF31, PRPF8, SNRNP200, RP1, CHM, RPGR were identified in more than one affected individual. Our results support the utility of clinical ES in the diagnosis of genetically heterogeneous retinal disorders.

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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