Your search keyword '"Dominant Optic Atrophy"' showing total 154 results

151. Clinical features, molecular genetics, and pathophysiology of dominant optic atrophy

Author

Votruba, Marcela, Moore, Anthony T., Bhattacharya, Shom Shanker, Votruba, Marcela, Moore, Anthony T., and Bhattacharya, Shom Shanker

Abstract

Inherited optic neuropathies are a significant cause of childhood and adult blindness and dominant optic atrophy (DOA) is the most common form of autosomally inherited (non-glaucomatous) optic neuropathy. Patients with DOA present with an insidious onset of bilateral visual loss and they characteristically have temporal optic nerve pallor, centrocaecal visual field scotoma, and a colour vision deficit, which is frequently blue-yellow. Evidence from histological and electrophysiological studies suggests that the pathology is confined to the retinal ganglion cell. A gene for dominant optic atrophy (OPA1) has been mapped to chromosome 3q28-qter, and studies are under way to refine the genetic interval in which the gene lies, to map the region physically, and hence to clone the gene. A second locus for dominant optic atrophy has recently been shown to map to chromosome 18q12.2-12.3 near the Kidd blood group locus. The cloning of genes for dominant optic atrophy will provide important insights into the pathophysiology of the retinal ganglion cell in health and disease. These insights may prove to be of great value in the understanding of other primary ganglion cell diseases, such as the mitochondrially inherited Leber's hereditary optic neuropathy and other diseases associated with ganglion cell loss, such as glaucoma.

Published

1998

152. OPA1 increases the risk of normal but not high tension glaucoma.

Author

Yu-Wai-Man, P., Stewart, J. D., Hudson, G., Andrews, R. M., Griffiths, P. G., Birch, M. K., and Chinnery, P. F.

Subjects

GLAUCOMA, NEUROPATHY, RETINAL ganglion cells, CUPPING, MITOCHONDRIAL membranes, VISUAL fields

Abstract

Background: Primary open angle glaucoma is a progressive optic neuropathy characterised by the selective loss of retinal ganglion cells, pathological optic disc cupping and visual field defects. The OPA1 gene encodes an inner mitochondrial membrane protein crucial for normal mitochondrial function, and pathogenic mutations cause autosomal dominant optic atrophy by specifically targeting retinal ganglion cells. This raises the distinct possibility that more subtle genetic variations in OPA1 could alter the risk of developing glaucoma. Methods: 137 patients with primary open angle glaucoma (67 patients with high-tension glaucoma (HTG), 70 patients with normal-tension glaucoma (NTG)) and 75 controls from the North East of England were studied. Three single-nucleotide polymorphisms in intron 8 (IVS8+4c->t and IVS8+32t->c) and exon 4 (c.473A->G) of the OPA1 gene were genotyped in the study group. In addition, the entire OPA1 coding region was sequenced in 24 individuals with the CT/TT compound genotype using standard BigDye chemistries. Results: There was no difference in either allele or genotype frequency for the IVS8+32t->c single-nucleotide polymorphisms between patients and controls, but there was a significant association between the T allele at IVS8+4c->t and the risk of developing NTG (OR=2.04, 95% CI=1.10 to 3.81, p=0.004), but not HTG. Logistic regression analysis also confirmed a strong association between the CT/TT compound genotype at IVS8+4 and IVS8+32 with NTG (OR=29.75, 95% CI=3.83 to 231.21, p=0.001). Conclusions: The CT/TT compound genotype at IVS8+4 and IVS8+32 is a strong genetic risk determinant for NTG but not HTG. [ABSTRACT FROM AUTHOR]

Published

2010

153. [Hereditary optic neuropathies: from clinical signs to diagnosis].

Author

Meunier I, Lenaers G, Hamel C, and Defoort-Dhellemmes S

Subjects

Diagnosis, Differential, Diagnostic Techniques, Ophthalmological, Humans, Optic Atrophies, Hereditary genetics, Optic Atrophy, Hereditary, Leber diagnosis, Optic Atrophy, Hereditary, Leber therapy, Pedigree, Physical Examination, Optic Atrophies, Hereditary diagnosis

Abstract

Inherited optic atrophy must be considered when working up any optic nerve involvement and any systemic disease with signs of optic atrophy, even with a negative family history. There are two classical forms: dominant optic atrophy, characterized by insidious, bilateral, slowly progressive visual loss and temporal disc pallor, and Leber's optic atrophy, characterized by acute loss of central vision followed by the same event in the fellow eye within a few weeks to months, with disc hyperemia in the acute phase. Family history is critical for diagnosis. In the absence of family history, the clinician must rule out an identifiable acquired cause, i.e. toxic, inflammatory, perinatal injury, traumatic or tumoral, with orbital and brain imaging (MRI). Recessive optic atrophies are more rare and more severe and occur as part of multisystemic disorders, particularly Wolfram syndrome (diabetes mellitus, diabetes insipidus, and hearing loss). Effective treatments are limited; alcohol and smoking should be avoided. A cyclosporine trial (taken immediately upon visual loss in the first eye) is in progress in Leber's optic atrophy to prevent involvement of the fellow eye., (Copyright © 2013. Published by Elsevier Masson SAS.)

Published

2013

154. Clinical variability in hereditary optic neuropathies: Two novel mutations in two patients with dominant optic atrophy and Wolfram syndrome

Author

Alberto Galvez-Ruiz

Subjects

Research literature, medicine.medical_specialty, Pathology, Hereditary optic neuropathies, Future studies, Dominant optic atrophy, Wolfram syndrome, genetic structures, business.industry, Hearing loss, Case Report, Audiology, Deafness, medicine.disease, eye diseases, Ophthalmology, Atrophy, Diabetes mellitus, otorhinolaryngologic diseases, medicine, Differential diagnosis, medicine.symptom, business

Abstract

Dominant optic atrophy (DOA) and Wolfram syndrome share a great deal of clinical variability, including an association with hearing loss and the presence of optic atrophy at similar ages. The objective of this paper was to discuss the phenotypic variability of these syndromes with respect to the presentation of two clinical cases.We present two patients, each with either DOA or Wolfram syndrome, and contribute to the research literature through our findings of two novel mutations.The overlapping of several clinical characteristics in hereditary optic neuropathies can complicate the differential diagnosis. Future studies are needed to better determine the genotype-phenotype correlation for these diseases.