Pathogenic genetic variants identified in Australian families with paediatric cataract

Objective Paediatric (childhood or congenital) cataract is an opacification of the normally clear lens of the eye and has a genetic basis in at least 18% of cases in Australia. This study aimed to replicate clinical gene screening to identify variants likely to be causative of disease in an Australian patient cohort. Methods and analysis Sixty--three reported isolated cataract genes were screened for rare coding variants in 37 Australian families using genome sequencing. Results Disease-causing variants were confirmed in eight families with variant classification as `likely pathogenic'. This included novel variants PITX3 p.(Ter303LeuextTer100), BFSP1 p.(Glu375GlyfsTer2), and GJA8 p.(Pro189Ser), as well as, previously described variants identified in genes GJA3, GJA8, CRYAA, BFSP1, PITX3, COL4A1 and HSF4. Additionally, eight variants of uncertain significance with evidence towards pathogenicity were identified in genes: GJA3, GJA8, LEMD2, PRX, CRYBB1, BFSP2, and MIP. Conclusion These findings expand the genotypephenotype correlations of both pathogenic and benign variation in cataract--associated genes. They further emphasise the need to develop additional evidence such as functional assays and variant classification criteria specific to paediatric cataract genes to improve interpretation of variants and molecular diagnosis in patients.

Automated summary

This study identified potential disease-causing variants for paediatric cataract through gene screening, expanding our understanding of the genotype-phenotype correlations in cataract-associated genes.