Founder effect in GLC1A‐linked familial open‐angle glaucoma in Northern France

Brézin, Antoine P.; Adam, Marie F.; Belmouden, Ahmed; Lureau, Marie‐Aude; Chaventré, André; Copin, Bruno; Gomez, Lucienne; Dinechin, S. Dupont de; Berkani, M; Valtot, F; Rouland, Jean‐François; Dascotte, J C; Bach, Jean‐François; Garchon, Henri‐Jean

doi:10.1002/(sici)1096-8628(19980413)76:5<438::aid-ajmg13>3.3.co;2-f

Cited by 8 publications

(22 citation statements)

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“…The Asn480Lys mutation is situated near a casein kinase II site and causes a change in charge in the local residue and a gain of α-helix in the structural conformation of the MYOC protein [24]. A POAG pedigree segregating this mutation was previously described by Adam et al [1,4].…”

Section: Discussionmentioning

confidence: 99%

“…These persons were screened for the presence or absence of the mutation by direct sequencing. To investigate the possibility of a founder effect with the patients described by Brézin et al [4], the alleles of four markers in the region of the disease gene were compared between these patients and the patients of our family, P26333. The markers D1S2851, D1S242, D1S218 and D1S1165 were tested.…”

Section: Dna Analysismentioning

confidence: 99%

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Myocilin mutations in a population-based sample of cases with open-angle glaucoma: the Rotterdam Study

Hulsman

Jong

Lettink

et al. 2002

Graefe's Arch Clin Exp Ophthalmol

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Section: Discussionmentioning

confidence: 99%

Section: Dna Analysismentioning

confidence: 99%

Myocilin mutations in a population-based sample of cases with open-angle glaucoma: the Rotterdam Study

Hulsman

Jong

Lettink

et al. 2002

Graefe's Arch Clin Exp Ophthalmol

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“…Stone et al (Stone et al 1997) identi®ed three mutations in the gene for MYOC/TIGR, which lies within the interval on chromosome 1 that was originally associated with juvenile open angle-glaucoma (GLC1A) (Shef®eld et al 1993;Richards et al 1994;Wiggs et al 1994). Subsequently, mutations in the same gene of patients with GLC1A-linked juvenile open-angle glaucoma were also reported by other researchers (Adam et al 1997;Kee & Ahn 1997;Stoilova et al 1997;Suzuki et al 1997;Brezin et al 1998;Mansergh et al 1998;Michels-Rautenstrauss et al 1998). Juvenile open-angle glaucoma refers to a subset of POAG that has an earlier age of onset, a highly penetrant mode of inheritance and is usually associated with a high IOP requiring early surgical treatment (Wiggs et al 1995;Johnson et al 1996).…”

Section: Introductionmentioning

confidence: 98%

Regulation of human myocilin/TIGR gene transcription in trabecular meshwork cells and astrocytes: role of upstream stimulatory factor

et al. 2000

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Background: Mutations in the myocilin (MYOC)/ TIGR gene are responsible for autosomal-dominant juvenile primary open-angle glaucoma (POAG). In patients with non-autosomal-dominant POAG, such mutations are rare, but the expression of MYOC/TIGR in the trabecular meshwork (TM) of the eye is considerably higher than in normals. We performed transfection, DNAse I footprinting, mutagenesis and electrophoretic mobility shift assays (EMSA) to identify elements responsible for the basal transcription of MYOC/TIGR in TM cells and astrocytes.

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“…The age-related penetrance of 50% at 30 and nearly 80% at 40 is comparable to other MYOC mutations, for example, Cys433Arg and Asn480Lys. 24,25 So far, all reported MYOC mutations have incomplete penetrance at 30, with Thr377Met resulting in the highest 26 and Gln368STOP in the lowest 22,27 age of onset.…”

Section: Discussionmentioning

confidence: 99%

Glaucoma phenotype in a large Swiss pedigree with the myocilin Gly367Arg mutation

Iliev

Bodmer

Gallati

et al. 2007

Eye

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Aims To characterize genotype, phenotype, and age-related penetrance in a Swiss pedigree with juvenile open-angle glaucoma (JOAG). Methods In a large Swiss family with history of glaucoma and 82 living members of four generations, we conducted molecular analysis and a detailed phenotype characterization in 52 family members. Mutation analysis was carried out using single-strand conformation polymorphism and DNA sequence analyses of the suspected candidate gene, myocilin (MYOC). Results We detected a Gly367Arg mutation in the MYOC gene of 13 family members. Nine of them (69.2%) had glaucoma: mean IOP 35.3 mm Hg, range 24-50 mm Hg; mean age at diagnosis 34.9 years, range 28-51 years. Two mutation carriers were glaucoma suspects, one (age 15) was unaffected, and one (age 16) not available for clinical examinations. Agerelated glaucoma penetrance was 50% at 30 and 78% at 40. Untreated IOP resulted in rapid disease progression, whereas good IOP control, usually only by means of filtration surgery, could stabilize the disease. None of the wild-type members had glaucoma. Conclusions This Swiss family is the largest reported Gly367Arg pedigree to date. The exact genotype and phenotype characterization allowed a reliable risk and prognosis assessment and targeted eye-care planning for the family. The study demonstrates the importance of genetic investigations in glaucoma families, carrying the potential of long-term socio-economic benefits.

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Founder effect in GLC1A‐linked familial open‐angle glaucoma in Northern France

Cited by 8 publications

References 0 publications

Myocilin mutations in a population-based sample of cases with open-angle glaucoma: the Rotterdam Study

Myocilin mutations in a population-based sample of cases with open-angle glaucoma: the Rotterdam Study

Regulation of human myocilin/TIGR gene transcription in trabecular meshwork cells and astrocytes: role of upstream stimulatory factor

Glaucoma phenotype in a large Swiss pedigree with the myocilin Gly367Arg mutation

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