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1 General aspects (0)   1.1 Epidemiology (4)   1.2 Population genetics (0)   1.3 Pathogenesis (9)   1.4 Quality of life (7)   1.5 Glaucomas as cause of blindness (7)   1.6 Prevention and screening (3) 2 Anatomical structures in glaucoma (0)   2.1 Conjunctiva (3)   2.2 Cornea (23)   2.3 Sclera (1)   2.4 Anterior chamber angle (7)   2.5 Meshwork (0)     2.5.1 Trabecular meshwork (18)     2.5.2 Schlemms canal (0)     2.5.3 Scleral outlet channels (1)   2.6 Aqueous humor dynamics (0)     2.6.1 Production (0)     2.6.2 Outflow (0)       2.6.2.1 Trabecular meshwork (4)       2.6.2.2 Uveoscleral (1)     2.6.3 Compostion (8)   2.7 Episcleral veins and venous pressure (0)   2.8 Iris (3)   2.9 Ciliary body (2)   2.10 Lens (2)   2.11 Vitreous body (2)   2.12 Choroid, peripapillary choroid, peripapillary atrophy (3)   2.13 Retina and retinal nerve fibre layer (43)   2.14 Optic disc (18)   2.15 Optic nerve (3)   2.16 Chiasma and retrochiasmal central nervous system (0)   2.17 Stem cells (0)   2.20 Other (1) 3 Laboratory methods (0)   3.1 Microscopy (1)   3.2 Electron microscopy (0)   3.3 Immunohistochemistry (7)   3.4 Molecular genetics (0)     3.4.1 Linkage studies (0)     3.4.2 Gene studies (20)   3.5 Molecular biology incl. 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disorders (0)     9.4.1 Steroid-induced glaucoma (6)     9.4.2 Glaucomas associated with disorders of the cornea, conjunctiva, sclera (3)       9.4.2.1 Iridocorneal endothelial syndrome (ICE, incl. irisatrophy) (1)       9.4.2.2 Posterior polymorphous dystrophy (0)       9.4.2.3 Fuchs' endothelial dystrophy (0)       9.4.2.5 Other (4)     9.4.3 Glaucomas associated with disorders of the iris and ciliary body (0)       9.4.3.1 Pigmentary glaucoma (1)       9.4.3.5 Other (3)     9.4.4 Glaucomas associated with disorders of the lens (0)       9.4.4.1 Exfoliation syndrome (22)       9.4.4.2 Glaucomas associated with cataracts (4)       9.4.4.3 Glaucomas associated with lens dislocation (1)       9.4.4.5 Other (2)     9.4.5 Glaucomas associated with disorders of the retina, choroid and vitreous (1)       9.4.5.1 Neovascular glaucoma (5)       9.4.5.5 Other (9)     9.4.6 Glaucomas associated with inflammation, uveitis (10)     9.4.7 Glaucomas associated with ocular trauma (2)     9.4.8 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(12) 15 Miscellaneous (17)

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Abstract #20577 Published in IGR 10-1

Correlating nerve fibre layer defects spatially with functional loss

Schiefer U; Paetzold J; Krapp E; Nevalainen J; Besch D
Eye 2007; 21: S25-S28

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The ultimate aim of clinical glaucoma research is to maintain visual function in the patient. Visual field (VF) loss can be determined more effectively by considering the related structural damage (ie retinal nerve fibre layer (RNFL) defect, optic disc notching, and splinter haemorrhages). A stack of individually digitized RNFL traces, which are superimposed by appropriate rotation and zoom procedures, allows for characterizing so-called trajectories defining the average course of retinal nerve fibres.Individual test point density in perimetry can be increased in regions of interest, that is in areas, or at the edges of, already detected VF defects (VFD) using SCotoma-Oriented Perimetry (SCOPE) or can be tailored (locally condensed) in an evidence-based manner by considering the local morphological damage using fundus-oriented perimetry (FOP). Focusing on areas most likely to be damaged makes conventional perimetry more efficient by locally enhancing spatial resolution. This technique requires a mathematical model that provides age-related normative values of differential luminance sensitivity for any location of the VF. Automated static perimetry with enhancement of spatial resolution in regions of interest has indeed a higher sensitivity than standard automated perimetry using a conventional rectangular (6 x 6°) grid. The new method can also be used for follow-up purposes: both scotoma depth and area, as well as their changes with time, need to be considered. The clinician has to be aware of the fact that any kind of perimetry is a rather exhausting and artificial examination procedure. It is rather inadequate for predicting per sepatients' quality of life and daily functionality as it does not consider compensation for VFD, for example by gaze and head movements.

Dr. U. Schiefer, Centre for Ophthalmology, University of Tubingen, Tubingen, Germany

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Classification:

6.6.3 Special methods (e.g. color, contrast, SWAP etc.) (Part of: 6 Clinical examination methods > 6.6 Visual field examination and other visual function tests)
2.13 Retina and retinal nerve fibre layer (Part of: 2 Anatomical structures in glaucoma)
6.9.5 Other (Part of: 6 Clinical examination methods > 6.9 Computerized image analysis)

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