Long term follow-up on a juvenile open angle glaucoma pedigree with a novel EFEMP1 mutation (c.1313, p.Tyr438Cys)

Brian P. Young; Angela W. Nyunt; Molly A. Clymer; Mallory R. Tollefson; Ben R. Roos; Michael J. Schnieders; Alan L. Robin; John H. Fingert

doi:10.1016/j.ogla.2025.08.003

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Long term follow-up on a juvenile open angle glaucoma pedigree with a novel EFEMP1 mutation (c.1313, p.Tyr438Cys)

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Long term follow-up on a juvenile open angle glaucoma pedigree with a novel EFEMP1 mutation (c.1313, p.Tyr438Cys)

Brian P. Young, Angela W. Nyunt, Molly A. Clymer, Mallory R. Tollefson, Ben R. Roos, Michael J. Schnieders, Alan L. Robin and John H. Fingert

Ophthalmology. Glaucoma, Vol.9(1), pp.75-85

01/2026

DOI: 10.1016/j.ogla.2025.08.003

PMCID: PMC12570167

PMID: 40876537

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https://pmc.ncbi.nlm.nih.gov/articles/PMC12570167/View

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Abstract

Purpose Determine the genetic cause of glaucoma in a JOAG pedigree of European ancestry. Design Case series / pedigree analysis Participants A three-generation JOAG pedigree Methods We obtained clinical data and tested DNA for mutations in known JOAG-causing genes with Sanger sequencing for MYOC and whole exome sequencing for EFEMP1. We assessed Identified mutations for pathogenicity by 1) frequency in control databases; 2) mutation analysis algorithms; 3) homology analyses; and 4) structural modeling of mutational effects on encoded proteins. Main Outcome Measures Detection of a mutation that is co-inherited with glaucoma in the JOAG pedigree. Secondary measures include descriptions of glaucoma phenotype (age at presentation, maximum intraocular pressure (IOP), progression rate, and response to therapy). Results Clinical data from an average follow-up of 11.5 ± 7.05 years was available from four family members with JOAG. Members of this pedigree had a mean age of diagnosis of 32.5 ± 8.6 years (range 25 to 43 years) and a mean maximum treated IOP of 32.3 ± 12.0 (range 20 to 50) mm Hg. Family members had visual field progression ranging from -0.25 to -1.1 dB / year and required an average of 1.8 ± 1.0 incisional glaucoma surgeries per eye for IOP control. No MYOC mutations were detected. A heterozygous missense mutation (c.1313A>G, p.Tyr438Cys) was detected in the EFEMP1 gene in all four family members with JOAG and is absent from control subjects. The p.Tyr438Cys mutation altered a highly conserved amino acid and was predicted to be pathogenic by 6 mutation analysis algorithms. Modeling of the p.Tyr438Cys mutation indicated it causes structural changes to EFEMP1 protein that are likely detrimental to its function. Conclusions This study identifies a novel mutation, p.Tyr438Cys, as the first known glaucoma-causing EFEMP1 mutation in a JOAG pedigree of European ancestry. Patients with the EFEMP1 mutation p.Tyr438Cys have an early-onset, severe glaucoma phenotype with high maximum IOPs that require surgical interventions and may have rapid progression. These data underscore the severity of this type of JOAG and the need for further research into its pathogenic mechanisms and therapeutic management.

Details

Title: Subtitle: Long term follow-up on a juvenile open angle glaucoma pedigree with a novel EFEMP1 mutation (c.1313, p.Tyr438Cys)
Creators: Brian P. Young
Angela W. Nyunt
Molly A. Clymer
Mallory R. Tollefson
Ben R. Roos
Michael J. Schnieders
Alan L. Robin
John H. Fingert
Resource Type: Journal article
Publication Details: Ophthalmology. Glaucoma, Vol.9(1), pp.75-85
DOI: 10.1016/j.ogla.2025.08.003
PMID: 40876537
PMCID: PMC12570167
NLM abbreviation: Ophthalmol Glaucoma
ISSN: 2589-4196
eISSN: 2589-4196
Language: English
Electronic publication date: 08/2025
Date published: 01/2026
Academic Unit: Roy J. Carver Department of Biomedical Engineering; The University of Iowa Institute for Vision Research; Biochemistry and Molecular Biology; Chemical and Biochemical Engineering; Ophthalmology and Visual Sciences
Record Identifier: 9984949264802771

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