Glaucoma is a group of ocular diseases characterized by an optic neuropathy in which degeneration of retinal ganglion cells leads to a characteristic excavation of the optic nerve head. Primary openangle glaucoma (POAG) can be subdivided into two groups according to age of onset:‐ 1. the more common middle‐to late‐age onset, chronic open‐angle glaucoma (COAG) diagnosed after the age of 40 years; 2. the rarer juvenile open‐angle glaucoma (JOAG), which is diagnosed between the age of 3 years and early adulthood. Recently, the gene coding for the trabecular meshwork‐induced glucocorticoid response protein (TIGR), located in chromosome 1 (lq23‐25), was found mutated in patients affected by POAG. In this work we describe the clinical and molecular genetic features of several Italian families affected by autosomal dominant POAG, collected in various regions of Italy.
Molecular basis of open-angle glaucoma in Italy
FOSSARELLO, MAURIZIO;
1998-01-01
Abstract
Glaucoma is a group of ocular diseases characterized by an optic neuropathy in which degeneration of retinal ganglion cells leads to a characteristic excavation of the optic nerve head. Primary openangle glaucoma (POAG) can be subdivided into two groups according to age of onset:‐ 1. the more common middle‐to late‐age onset, chronic open‐angle glaucoma (COAG) diagnosed after the age of 40 years; 2. the rarer juvenile open‐angle glaucoma (JOAG), which is diagnosed between the age of 3 years and early adulthood. Recently, the gene coding for the trabecular meshwork‐induced glucocorticoid response protein (TIGR), located in chromosome 1 (lq23‐25), was found mutated in patients affected by POAG. In this work we describe the clinical and molecular genetic features of several Italian families affected by autosomal dominant POAG, collected in various regions of Italy.File | Dimensione | Formato | |
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