# Cystoid Macular Lesions in Inherited Retinal Diseases: Prevalence, Characteristics, and Genetic Associations in a Hungarian Cohort

**Authors:** Barbara Asboth, Alessandra Sanrocco, Barbara Besztercei, Balazs Lesch, Agnes Takacs, Rita Vamos, Balazs Varsanyi, Andras Vegh, Krisztina Knezy, Viktoria Szabo, Zoltan Zsolt Nagy, Ditta Zobor

PMC · DOI: 10.3390/genes16101212 · 2025-10-14

## TL;DR

This study finds that cystoid macular lesions are common in inherited retinal diseases in Hungary and are linked to specific genes, which could impact treatment effectiveness.

## Contribution

The study identifies genetic associations with cystoid macular lesions in inherited retinal diseases and emphasizes their impact on gene therapy outcomes.

## Key findings

- Cystoid macular lesions were detected in 13.2% of patients with inherited retinal diseases in a Hungarian cohort.
- Genes such as RS1, USH2A, and NR2E3 were frequently associated with cystoid macular lesions.
- Cystoid macular edema was more common in retinitis pigmentosa and had specific visual acuity and retinal thickness measurements.

## Abstract

Background/Objectives: Cystoid macular lesion (CML) is a treatable cause of central vision loss in inherited retinal diseases (IRDs). We aimed to determine the frequency of CML in a large Hungarian IRD cohort and examine associations with causative genes. Methods: This longitudinal, retrospective, monocentric study included patients with genetically confirmed IRD identified from our database. Targeted next-generation sequencing (351-gene panel) and comprehensive ophthalmic evaluation were performed, including best-corrected visual acuity (BCVA) and spectral domain optical coherence tomography (SD-OCT). CML was defined as intraretinal hyporeflective spaces with well-defined borders visible on at least two B-scans within the SD-OCT macular volume and was categorized as cystoid macular edema (CME) or non-CME. Results: We enrolled 430 patients with genetically confirmed IRDs. CML was detected in 93 eyes of 57 patients. Mean age at OCT was 36.6 ± 18.7 years (range, 3–76); 32 were male (56.1%). Inheritance patterns were autosomal recessive in 24 (42.1%), X-linked in 19 (33.3%), and autosomal dominant in 14 (24.6%). Frequently implicated genes were RS1 (12/57), USH2A (7/57), NR2E3 (7/57), PRPF31 (4/57), RPGR (4/57), and RHO (4/57). CME predominated in retinitis pigmentosa (32/57, 56%), with mean BCVA 0.44 ± 0.29 (decimal) and central retinal thickness (CRT) 401 ± 181 µm. Non-CME CML occurred in 25/57 (44%)—notably in X-linked retinoschisis and enhanced S-cone syndrome—with BCVA 0.40 ± 0.23 and CRT 465 ± 258 µm. BCVA did not correlate with CRT (rS = 0.18). Conclusions: CML occurred in 13.2% of patients within a large Hungarian cohort of genetically confirmed IRDs. Patients with IRD—mainly RP—are at higher risk for CML. Gene therapy is promising for retinal diseases, but CMLs can compromise effectiveness. Reducing and managing CME before gene therapy corroborates retinal stability and the functional state essential for the proper delivery and penetration of corrective genes to the target cells.

## Linked entities

- **Genes:** RS1 (retinoschisin 1) [NCBI Gene 6247], USH2A (usherin) [NCBI Gene 7399], NR2E3 (nuclear receptor subfamily 2 group E member 3) [NCBI Gene 10002], PRPF31 (pre-mRNA processing factor 31) [NCBI Gene 26121], RPGR (retinitis pigmentosa GTPase regulator) [NCBI Gene 6103], RHO (rhodopsin) [NCBI Gene 6010]
- **Diseases:** retinitis pigmentosa (MONDO:0008377), X-linked retinoschisis (MONDO:0010725), enhanced S-cone syndrome (MONDO:0100288)

## Full-text entities

- **Genes:** RHO (rhodopsin) [NCBI Gene 6010] {aka CSNBAD1, OPN2, RP4}, PRPF31 (pre-mRNA processing factor 31) [NCBI Gene 26121] {aka NY-BR-99, PRP31, RP11, SNRNP61}, RS1 (retinoschisin 1) [NCBI Gene 6247] {aka RS, XLRS1}, RPGR (retinitis pigmentosa GTPase regulator) [NCBI Gene 6103] {aka COD1, CORDX1, CRD, PCDX, RP15, RP3}, NR2E3 (nuclear receptor subfamily 2 group E member 3) [NCBI Gene 10002] {aka ESCS, ESCS1, PNR, RNR, RP37, rd7}, USH2A (usherin) [NCBI Gene 7399] {aka RP39, US2, USH2, dJ1111A8.1}
- **Diseases:** X-linked retinoschisis (MESH:D041441), RP (MESH:D012174), IRD (MESH:D052919), CME (MESH:D008269), S-cone syndrome (MESH:C564835), CMLs (MESH:C536093), vision loss (MESH:D014786), IRDs (MESH:D012164)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Figures

4 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12562411/full.md

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Source: https://tomesphere.com/paper/PMC12562411