Literature DB >> 10815160

Myocilin Gln368stop mutation and advanced age as risk factors for late-onset primary open-angle glaucoma.

A Angius1, P Spinelli, G Ghilotti, G Casu, G Sole, A Loi, A Totaro, L Zelante, P Gasparini, N Orzalesi, M Pirastu, L Bonomi.   

Abstract

BACKGROUND: Juvenile open-angle glaucoma has been found to be associated with molecular defects in the myocilin (MYOC) gene. Most of the defects are missense mutations located in the third exon. The Gln368stop mutation has recently been found in several cases of late-onset primary open-angle glaucoma (POAG).
OBJECTIVE: To study the effect of glaucoma risk in a relatively homogeneous genetic population.
METHODS: A clinical study was performed in all living members of a 5-generation family. DNA analysis was performed for studying association with genetic markers and identifying the mutation.
RESULTS: We identified the Gln368stop molecular defect in 19 patients with POAG, 5 patients with ocular hypertension, and 22 healthy carriers. We compared affected and unaffected carriers based on age at onset and last examination, respectively. Besides the presence of 3 young patients with POAG (<40 years old), the number of glaucomatous patients in the advanced age group increased.
CONCLUSIONS: The penetrance of glaucoma increases with age in Gln368stop carriers, but some remain unaffected at advanced age and others are affected at an early age. This suggests that additional risk factors are operating within this family, which may be identified by a genome-wide linkage search in this large pedigree. CLINICAL RELEVANCE: The myocilin Gln368stop mutation shows a good genotype-phenotype correlation and should be investigated in all familiar cases of chronic POAG. This may be important for early diagnosis and periodical checkups of presymptomatic individuals belonging to these families.

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Year:  2000        PMID: 10815160     DOI: 10.1001/archopht.118.5.674

Source DB:  PubMed          Journal:  Arch Ophthalmol        ISSN: 0003-9950


  9 in total

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3.  Rapid mutation detection by the transgenomic wave analyser DHPLC identifies MYOC mutations in patients with ocular hypertension and/or open angle glaucoma.

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4.  Accurate Imputation-Based Screening of Gln368Ter Myocilin Variant in Primary Open-Angle Glaucoma.

Authors:  Puya Gharahkhani; Kathryn P Burdon; Alex W Hewitt; Matthew H Law; Emmanuelle Souzeau; Grant W Montgomery; Graham Radford-Smith; David A Mackey; Jamie E Craig; Stuart MacGregor
Journal:  Invest Ophthalmol Vis Sci       Date:  2015-08       Impact factor: 4.799

5.  Identification a novel MYOC gene mutation in a Chinese family with juvenile-onset open angle glaucoma.

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Review 7.  Myocilin-associated Glaucoma: A Historical Perspective and Recent Research Progress.

Authors:  Ritika Sharma; Abhinav Grover
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8.  Role of MYOC and OPTN sequence variations in Spanish patients with primary open-angle glaucoma.

Authors:  Francisco Lopez-Martinez; Maria-Pilar Lopez-Garrido; Francisco Sanchez-Sanchez; Ezequiel Campos-Mollo; Miguel Coca-Prados; Julio Escribano
Journal:  Mol Vis       Date:  2007-06-14       Impact factor: 2.367

9.  Presence of myocilin sequence variants in Japanese patients with open-angle glaucoma.

Authors:  MingGe Mengkegale; Nobuo Fuse; Akiko Miyazawa; Kana Takahashi; Motohiko Seimiya; Tomoki Yasui; Makoto Tamai; Toru Nakazawa; Kohji Nishida
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  9 in total

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