What does this research mean for the field?

Bilateral juvenile-onset cataracts can be associated with variants in the GCNT2 gene, including a novel missense variant in the lens-specific transcript GCNT2B. Novelty: ClaimNovelty.NOVEL_FINDING. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

This research aims to investigate the connection between GCNT2 variants and juvenile-onset cataracts.

February 22, 2026

Bilateral juvenile-onset cataracts associated with GCNT2 variants

Key Points

This research aims to investigate the connection between GCNT2 variants and juvenile-onset cataracts.
Case report of a proband with bilateral juvenile-onset cataracts.
Identification of genetic variants in GCNT2, notably in exon 3 and exon 1B.
Characterization of pathogenic and novel variants associated with cataract presentation.
Identified a known pathogenic variant in exon 3 of GCNT2.
Discovered a novel missense variant in the lens-specific transcript GCNT2B.
Expanded the mutational spectrum related to juvenile-onset cataracts linked to GCNT2.

Abstract

In this case, bilateral juvenile-onset cataracts were presumed to be related to GCNT2 variants sometimes associated with congenital cataracts (OMIM *600429). Notably, this proband had juvenile-onset cataracts rather than the congenital presentation exclusively associated with GCNT2. Intragenic changes within exon 3 have been most frequently identified, while exon 1B has only been disrupted as part of a gene deletion. Here, the known pathogenic variant is within exon 3, while the variant in exon 1B represents a novel change. In summary, this case demonstrates GCNT2-related cataracts may present in childhood and expands the mutational spectrum through the first report of a missense variant in the lens-specific transcript GCNT2B.

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