Diagnostic genetic testing for patients with bilateral optic neuropathy and comparison of clinical features according to OPA1 mutation status

Eric D Gaier; Katherine Boudreault; Isao Nakata; Maria Janessian; Philip Skidd; Elizabeth DelBono; Keri F Allen; Louis R Pasquale; Emily Place; Dean M Cestari; Rebecca C Stacy; Joseph F Rizzo 3rd; Janey L Wiggs

Diagnostic genetic testing for patients with bilateral optic neuropathy and comparison of clinical features according to OPA1 mutation status

Mol Vis. 2017 Aug 10:23:548-560. eCollection 2017.

Authors

Affiliations

¹ Department of Ophthalmology, Harvard Medical School, Massachusetts Eye and Ear Infirmary Boston, MA.
² Departments of Ophthalmology and Neurology, University of Vermont College of Medicine, Burlington, MA.
³ Channing Division of Network Medicine, Brigham and Women's Hospital, Harvard Medical School, Boston, MA.

PMID: 28848318
PMCID: PMC5561143

Abstract

Purpose: Inherited optic neuropathy is genetically heterogeneous, and genetic testing has an important role in risk assessment and counseling. The purpose of this study is to determine the prevalence and spectrum of mutations in a group of patients referred for genetic testing to a tertiary center in the United States. In addition, we compared the clinical features of patients with and without mutations in OPA1, the gene most commonly involved in dominantly inherited optic atrophy.

Methods: Clinical data and genetic testing results were reviewed for 74 unrelated, consecutive patients referred with a history of insidious, relatively symmetric, bilateral visual loss secondary to an optic neuropathy. Patients were evaluated for disease-causing variants in OPA1, OPA3, WFS1, and the entire mitochondrial genome with DNA sequencing and copy number variation (CNV) testing.

Results: Pathogenic DNA variants were found in 25 cases, with the majority (24 patients) located in OPA1. Demographics, clinical history, and clinical features for the group of patients with mutations in OPA1 were compared to those without disease-causing variants. Compared to the patients without mutations, cases with mutations in OPA1 were more likely to have a family history of optic nerve disease (p = 0.027); however, 30.4% of patients without a family history of disease also had mutations in OPA1. OPA1 mutation carriers had less severe mean deviation and pattern standard deviation on automated visual field testing than patients with optic atrophy without mutations in OPA1 (p<0.005). Other demographic and ocular features were not statistically significantly different between the two groups, including the fraction of patients with central scotomas (42.9% of OPA1 mutation positive and 66.0% of OPA1 mutation negative).

Conclusions: Genetic testing identified disease-causing mutations in 34% of referred cases, with the majority of these in OPA1. Patients with mutations in OPA1 were more likely to have a family history of disease; however, 30.4% of patients without a family history were also found to have an OPA1 mutation. This observation, as well as similar frequencies of central scotomas in the groups with and without mutations in OPA1, underscores the need for genetic testing to establish an OPA1 genetic diagnosis.

Publication types

Comparative Study
Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Adult
DNA Copy Number Variations
DNA Mutational Analysis
DNA, Mitochondrial / genetics
Female
GTP Phosphohydrolases / genetics*
Genetic Testing*
Humans
Male
Membrane Proteins / genetics
Middle Aged
Mutation*
Mutation, Missense
Optic Nerve Diseases / diagnosis*
Optic Nerve Diseases / genetics*
Proteins / genetics
Sequence Analysis, DNA
Tertiary Care Centers
Vision Disorders / diagnosis
Vision Disorders / genetics
Visual Field Tests
Visual Fields

Substances

DNA, Mitochondrial
Membrane Proteins
OPA3 protein, human
Proteins
wolframin protein
GTP Phosphohydrolases
OPA1 protein, human

Grants and funding

P30 EY014104/EY/NEI NIH HHS/United States