Lack of Association of Mutations in Optineurin With Disease in Patients With Adult-onset Primary Open-angle Glaucoma

Wiggs, Janey L.

doi:10.1001/archopht.121.8.1181

Cited by 71 publications

(32 citation statements)

References 16 publications

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“…Unexpectedly, we did not detect any convincing sequence variation that could be defined as a diseasecausing mutation. These results are in keeping with other recent studies from the US [1,23], UK [2] and, more interestingly, even from Japan [18,19].…”

Section: Discussionsupporting

confidence: 93%

Optineurin gene is not involved in the common high-tension form of primary open-angle glaucoma

Ariani

Longo

Frezzotti

et al. 2006

Graefe's Arch Clin Exp Ophthalmo

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Section: Discussionsupporting

confidence: 93%

Optineurin gene is not involved in the common high-tension form of primary open-angle glaucoma

Ariani

Longo

Frezzotti

et al. 2006

Graefe's Arch Clin Exp Ophthalmo

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“…Of the eight relatives who have not inherited a mutation, none are thought to have glaucomatous damage but one is being treated for ocular hypertension, suggesting the importance of other genetic factors in glaucoma susceptibility. One such possible gene, optineurin, was recently identified in POAG families (Rezaie et al 2002), but it has already been shown that mutations in this gene are not associated with high-tension glaucoma in the general population (Alward et al 2003;Aung et al 2003;Wiggs et al 2003). A specific p53 gene haplotype has also recently been associated with late-onset POAG (Ressiniotis et al 2004).…”

Section: Discussionmentioning

confidence: 99%

Low prevalence of MYOC mutations in UK primary open-angle glaucoma patients limits the utility of genetic testing

et al. 2004

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Primary open angle glaucoma (POAG) affects 1% of people over age 40. Early detection and treatment can prevent blindness, but the disease is often asymptomatic until a late stage. Positive family history is an important risk factor and previous studies indicate that approximately 5% of POAG results from mutations in the myocilin ( MYOC) gene, raising the possibility of identifying individuals genetically predisposed to glaucoma. We collected DNA samples from 426 unselected UK POAG patients and analyzed them for MYOC mutations. The Q368X mutation was found in six patients (1.4%). No other mutations were identified, suggesting that amongst patients unselected for family history, the prevalence of MYOC mutations in the UK is lower than in other populations. Genetic and glaucoma screening was offered to first-degree relatives of these six probands (group 1) and of age/sex-matched mutation-negative controls (group 2). Of 11 group-1 relatives, three carried Q368X, one of whom already had glaucoma. Notably, of the 13 relatives in both groups who were mutation negative, one was already being treated for ocular hypertension. We therefore caution against changing glaucoma surveillance regimens in such individuals and suggest that routine untargeted genetic testing for MYOC mutations in patients with POAG would be of limited value until additional significant genetic risk factors are identified.

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“…The first report on OPTN mutations indicated that the E50K mutation was the most prevalent mutation and observed in 13.5% of all familial POAG cases (Rezaie et al, 2002). Subsequence reports have demonstrated that the prevalence of mutations in the OPTN gene is between 0% and 6% in POAG patients and the prevalence of the E50K mutation is approximately 1% (Aung et al, 2003;Hauser et al, 2006b;Leung et al, 2003;Melki et al, 2003;Sripriya et al, 2006;Tang et al, 2003;Toda et al, 2004;Wiggs et al, 2003). Phenotypically, the E50K mutation has been reported to be associated with a younger age and a more severe form of NTG at the diagnosis (Aung et al, 2005a;Hauser et al, 2006b).…”

Section: Optineurinmentioning

confidence: 99%

Advances in glaucoma genetics

Sakurada

Mabuchi

2015

New Trends in Basic and Clinical Research of Glaucoma: A Neurodegenerative Disease of the Visual System, Part A

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Lack of Association of Mutations in Optineurin With Disease in Patients With Adult-onset Primary Open-angle Glaucoma

Cited by 71 publications

References 16 publications

Optineurin gene is not involved in the common high-tension form of primary open-angle glaucoma

Optineurin gene is not involved in the common high-tension form of primary open-angle glaucoma

Low prevalence of MYOC mutations in UK primary open-angle glaucoma patients limits the utility of genetic testing

Advances in glaucoma genetics

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