# Phenotypic and Genotypic Characterization of 171 Patients with Syndromic Inherited Retinal Diseases Highlights the Importance of Genetic Testing for Accurate Clinical Diagnosis

**Authors:** Sofia Kulyamzin, Rina Leibu, Hadas Newman, Miriam Ehrenberg, Nitza Goldenberg-Cohen, Shiri Zayit-Soudry, Eedy Mezer, Ygal Rotenstreich, Iris Deitch, Daan M. Panneman, Dinah Zur, Elena Chervinsky, Stavit A. Shalev, Frans P. M. Cremers, Dror Sharon, Susanne Roosing, Tamar Ben-Yosef

PMC · DOI: 10.3390/genes16070745 · 2025-06-26

## TL;DR

This study shows that genetic testing is crucial for accurately diagnosing rare inherited eye diseases that also affect other body systems.

## Contribution

The study highlights how genetic testing can revise clinical diagnoses in syndromic inherited retinal diseases.

## Key findings

- Genetic analysis led to revised diagnoses in 29% of families.
- Novel genotype–phenotype correlations were found, such as KATNIP variants causing kidney disease and IRD.
- The most common causative gene was USH2A, and the most common condition was Usher syndrome.

## Abstract

Background: Syndromic inherited retinal diseases (IRDs) are a clinically and genetically heterogeneous group of disorders, involving the retina and additional organs. Over 80 forms of syndromic IRD have been described. Methods: We aimed to phenotypically and genotypically characterize a cohort of 171 individuals from 140 Israeli families with syndromic IRD. Ophthalmic examination included best corrected visual acuity, fundus examination, visual field testing, retinal imaging and electrophysiological evaluation. Most participants were also evaluated by specialists in fields relevant to their extra-retinal symptoms. Genetic analyses included haplotype analysis, homozygosity mapping, Sanger sequencing and next-generation sequencing. Results: In total, 51% of the families in the cohort were consanguineous. The largest ethnic group was Muslim Arabs. The most common phenotype was Usher syndrome (USH). The most common causative gene was USH2A. In 29% of the families, genetic analysis led to a revised or modified clinical diagnosis. This included confirmation of an atypical USH diagnosis for individuals with late-onset retinitis pigmentosa (RP) and/or hearing loss (HL); diagnosis of Heimler syndrome in individuals with biallelic pathogenic variants in PEX6 and an original diagnosis of USH or nonsyndromic RP; and diagnosis of a mild form of Leber congenital amaurosis with early-onset deafness (LCAEOD) in an individual with a heterozygous pathogenic variant in TUBB4B and an original diagnosis of USH. Novel genotype–phenotype correlations included biallelic pathogenic variants in KATNIP, previously associated with Joubert syndrome (JBTS), in an individual who presented with kidney disease and IRD, but no other features of JBTS. Conclusions: Syndromic IRDs are a highly heterogeneous group of disorders. The rarity of some of these syndromes on one hand, and the co-occurrence of several syndromic and nonsyndromic conditions in some individuals, on the other hand, complicates the diagnostic process. Genetic analysis is the ultimate way to obtain an accurate clinical diagnosis in these individuals.

## Linked entities

- **Genes:** USH2A (usherin) [NCBI Gene 7399], PEX6 (peroxisomal biogenesis factor 6) [NCBI Gene 5190], TUBB4B (tubulin beta 4B class IVb) [NCBI Gene 10383], KATNIP (katanin interacting protein) [NCBI Gene 23247]
- **Diseases:** Usher syndrome (MONDO:0019501), retinitis pigmentosa (MONDO:0008377), hearing loss (MONDO:0005365), Heimler syndrome (MONDO:0100229), Leber congenital amaurosis (MONDO:0018998), Joubert syndrome (MONDO:0018772)

## Full-text entities

- **Genes:** KATNIP (katanin interacting protein) [NCBI Gene 23247] {aka JBTS26, KIAA0556}, TUBB4B (tubulin beta 4B class IVb) [NCBI Gene 10383] {aka Beta2, LCAEOD, TUBB2, TUBB2C}, PEX6 (peroxisomal biogenesis factor 6) [NCBI Gene 5190] {aka HMLR2, PAF-2, PAF2, PBD4A, PDB4B, PXAAA1}, USH2A (usherin) [NCBI Gene 7399] {aka RP39, US2, USH2, dJ1111A8.1}
- **Diseases:** LCAEOD (MESH:D057130), IRDs (MESH:D012164), IRD (MESH:D052919), HL (MESH:D034381), JBTS (MESH:C536293), RP (MESH:D012174), Syndromic Inherited Retinal Diseases (MESH:D030342), USH (MESH:D052245), Heimler syndrome (MESH:C535994), nonsyndromic (MESH:C580334), kidney disease (MESH:D007674)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Figures

2 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12295353/full.md

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Source: https://tomesphere.com/paper/PMC12295353