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Comment
. 2025 Aug 1;143(8):692-701.
doi: 10.1001/jamaophthalmol.2025.2187.

Founder Homozygous Nonsense CREB3 Variant and Variable-Onset Retinal Degeneration

Manar Salameh  1 Ghadeer Abu Tair  1 Samira Mousa  1 Alexey Obolensky  1 Anand Swaroop  2 Susanne Roosing  3 Eedy Mezer  4   5 Shiri Soudry  6 Marianthi Karali  7   8 Francesca Simonelli  8 Sandro Banfi  7   9 Eyal Banin  1 Tamar Ben-Yosef  4 Dror Sharon  1 Samer Khateb  1
Affiliations
Comment

Founder Homozygous Nonsense CREB3 Variant and Variable-Onset Retinal Degeneration

Manar Salameh et al. JAMA Ophthalmol. .

Abstract

Importance: Uncovering the genetic basis of inherited retinal diseases (IRDs) can enhance both diagnostic accuracy and the development of targeted treatment strategies.

Objective: To evaluate the association between a homozygous nonsense variant in CREB3 with IRDs.

Design, setting, and participants: Thirteen patients with a clinical diagnosis of retinitis pigmentosa or cone-rod degeneration were analyzed by whole-genome sequencing (WGS) and whole-exome sequencing (WES). Clinically, patients presented with 2 main phenotypes, rod-cone and cone-rod dystrophies, demonstrating variable electrophysiological and fundoscopic findings. Expression analysis was performed on patient-derived skin fibroblasts using the reverse transcription-polymerase chain reaction and Western blot analysis, and by interrogating previously published retinal single-cell RNA sequence data. Immunohistochemistry staining was performed on wild-type mouse retinal sections using an anti-CREB3 antibody. Patients with variable phenotypes of IRDs were recruited from 3 medical centers in Israel and Italy. Ophthalmologists clinically diagnosed patients at the relevant medical centers and referred them for genetic screening. WES and WGS were performed at different national and international centers, and the findings of the previously unreported gene were shared between investigators.

Exposures: CREB3 and IRDs.

Main outcomes and measures: The main outcome was evidence supporting an association between CREB3 and IRD. Measures included WES, WGS, and immunohistochemistry staining.

Results: A founder homozygous nonsense variant in CREB3 (c.881G>A, p.Trp294*) was identified in 13 patients from 4 unrelated families; 12 descendent from North-African Jewish origins and 1 from Italian origins. All patients manifested retinal degeneration with varying ages at onset. In patient-derived fibroblasts, the variant mRNA transcript generated a truncated CREB3 protein. Expression analysis and immunohistochemistry staining revealed CREB3 RNA and protein expression in various retinal cell types, indicating its vital role in photoreceptor function.

Conclusions and relevance: This study found an association between CREB3 and IRDs. CREB3 was previously shown to be upregulated following ultraviolet radiation. This might contribute to the extensive clinical variability observed in this relatively large cohort of homozygous patients with the same truncated variant.

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Conflict of interest statement

Conflict of Interest Disclosures: Mrs Salameh reported funding from the Neubauer Family Foundation and the Science Training Encouraging Peace Foundation. No other disclosures were reported.

Comment on

References

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