Autozygome‐guided exome‐first study in a consanguineous cohort with early‐onset retinal disease uncovers an isolated RIMS2 phenotype and a retina‐enriched RIMS2 isoform

Leber congenital amaurosis (LCA) and early‐onset retinal degeneration (EORD) are inherited retinal diseases (IRD) characterized by early‐onset vision impairment. Herein, we studied 15 Saudi families by whole exome sequencing (WES) and run‐of‐homozygosity (ROH) detection via AutoMap in 12/15 consangu...

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Bibliographic Details
Published in:Clinical genetics 2024-08, Vol.106 (2), p.127-139
Main Authors: Del Pozo‐Valero, Marta, Almoallem, Basamat, Dueñas Rey, Alfredo, Mahieu, Quinten, Van Heetvelde, Mattias, Jeddawi, Laila, Bauwens, Miriam, De Baere, Elfride
Format: Article
Language:English
Subjects:
autozygome
consanguinity
early‐onset retinal disease
exome sequencing
Genotypes
Guanylate cyclase 1
Heritability
Isoforms
Leber congenital amaurosis
non‐syndromic
Phenotypes
Retina
Retinal degeneration
retina‐enriched isoform
RIMS2
Whole genome sequencing
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Summary:Leber congenital amaurosis (LCA) and early‐onset retinal degeneration (EORD) are inherited retinal diseases (IRD) characterized by early‐onset vision impairment. Herein, we studied 15 Saudi families by whole exome sequencing (WES) and run‐of‐homozygosity (ROH) detection via AutoMap in 12/15 consanguineous families. This revealed (likely) pathogenic variants in 11/15 families (73%). A potential founder variant was found in RPGRIP1. Homozygous pathogenic variants were identified in known IRD genes (ATF6, CRB1, CABP4, RDH12, RIMS2, RPGRIP1, SPATA7). We established genotype‐driven clinical reclassifications for ATF6, CABP4, and RIMS2. Specifically, we observed isolated IRD in the individual with the novel RIMS2 variant, and we found a retina‐enriched RIMS2 isoform conserved but not annotated in mouse. The latter illustrates potential different phenotypic consequences of pathogenic variants depending on the particular tissue/cell‐type specific isoforms they affect. Lastly, a compound heterozygous genotype in GUCY2D in one non‐consanguineous family was demonstrated, and homozygous variants in novel candidate genes ATG2B and RUFY3 were found in the two remaining consanguineous families. Reporting these genes will allow to validate them in other IRD cohorts. Finally, the missing heritability of the two unsolved IRD cases may be attributed to variants in non‐coding regions or structural variants that remained undetected, warranting future WGS studies. Autozygome‐guided whole exome sequencing (WES) in Saudi families with early‐onset inherited retinal disease revealed a diagnosis in 73%. Genotype‐driven clinical reclassifications showed a novel genotype–phenotype association for non‐syndromic RIMS2‐IRD. We found a retina‐enriched RIMS2 isoform conserved but not annotated in mouse and report two novel candidate IRD genes, ATG2B and RUFY3.
ISSN:0009-9163
1399-0004
1399-0004
DOI:10.1111/cge.14517