Recurrent Mutations in a Single Exon Encoding the Evolutionarily Conserved Olfactomedin-Homology Domain of TIGR in Familial Open-Angle Glaucoma

Adam, Marie F.; Belmouden, Ahmed; Binisti, Philippe; Brézin, Antoine P.; Valtot, F; Béchetoille, A; Dascotte, J C; Copin, Bruno; Gomez, Lucienne; Chaventré, André; Bach, Jean‐François; Garchon, Henri‐Jean

doi:10.1093/hmg/6.12.2091

Cited by 235 publications

(196 citation statements)

References 22 publications

(30 reference statements)

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“…The Gln368Stop mutation confers mild risk, 55 Thr377Met and Gly252Arg mutations intermediate risk, 56,57 and the Pro370Leu mutation severe risk. [58][59][60][61] …”

Section: Genetic Loci and Glaucoma-associated Genesmentioning

confidence: 99%

Current concepts on primary open-angle glaucoma genetics: a contribution to disease pathophysiology and future treatment

Gemenetzi

Yang

Lotery

2011

Eye

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“…The Gln368Stop mutation confers mild risk, 55 Thr377Met and Gly252Arg mutations intermediate risk, 56,57 and the Pro370Leu mutation severe risk. [58][59][60][61] …”

Section: Genetic Loci and Glaucoma-associated Genesmentioning

confidence: 99%

Current concepts on primary open-angle glaucoma genetics: a contribution to disease pathophysiology and future treatment

Gemenetzi

Yang

Lotery

2011

Eye

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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: 99%

“…In addition to TM and retina, MYOC/TIGR is expressed in other ocular tissues such as the cornea, sclera, ciliary body, iris and optic nerve head (Adam et al 1997;Ortego et al 1997;Tomarev et al 1998;Karali et al 2000). The normal role of MYOC/TIGR and the mechanisms by which mutations in this gene cause glaucoma are unknown.…”

Section: Introductionmentioning

confidence: 99%

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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“…Mutations in the olfactomedin domain may be deleterious for the functions of these proteins. For example, mutations in the olfactomedin domain of the human MYOCILIN gene may lead to juvenile open-angle glaucoma and in some cases to adult onset glaucoma [17][18][19][20].…”

Section: Introductionmentioning

confidence: 99%

Optimedin induces expression of N-cadherin and stimulates aggregation of NGF-stimulated PC12 cells

Lee

Tomarev

2007

Experimental Cell Research

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Optimedin, also known as olfactomedin 3, belongs to a family of olfactomedin domain-containing proteins. It is expressed in neural tissues and Pax6 is involved in the regulation of its promoter. To study possible effects of optimedin on the differentiation of neural cells, we produced stably transfected PC12 cell lines expressing optimedin under a tetracycline-inducible promoter. Cells expressing high levels of optimedin showed higher growth rates and stronger adhesion to the collagen extracellular matrix as compared with control PC12 cells. After stimulation with nerve growth factor (NGF), optimedin-expressing cells demonstrated elevated levels of N-cadherin, β-catenin, α-catenin, and occludin as compared with stimulated, control PC12 cells. Expression of optimedin induced Ca 2+ -dependent aggregation of NGF-stimulated PC12 cells and this aggregation was blocked by the expression of N-cadherin siRNA. Expression of optimedin also changed the organization of the actin cytoskeleton and inhibited neurite outgrowth in NGF-stimulated PC12 cells. We suggest that expression of optimedin stimulates the formation of adherent and tight junctions on the cell surface and this may play an important role in the differentiation of the brain and retina through the modulation of cytoskeleton organization, cell-cell adhesion and migration.

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Recurrent Mutations in a Single Exon Encoding the Evolutionarily Conserved Olfactomedin-Homology Domain of TIGR in Familial Open-Angle Glaucoma

Cited by 235 publications

References 22 publications

Current concepts on primary open-angle glaucoma genetics: a contribution to disease pathophysiology and future treatment

Current concepts on primary open-angle glaucoma genetics: a contribution to disease pathophysiology and future treatment

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

Optimedin induces expression of N-cadherin and stimulates aggregation of NGF-stimulated PC12 cells

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