British Journal of Ophthalmology 2002;86:902-909
© 2002 British Journal of Ophthalmology
Epiretinal pathology of vitreomacular traction syndrome
A Gandorfer,
M Rohleder,
A Kampik
Department of Ophthalmology, Ludwig-Maximilians-University, Mathildenstrasse 8, D - 80336, München, Germany
Correspondence to:
Correspondence to:
Anselm Kampik, MD;
akampik{at}ak-i.med.uni-muenchen.de
Aims: To investigate the ultrastructure of the vitreoretinal interface in patients with vitreomacular traction syndrome.
Methods: 14 patients with vitreomacular traction syndrome underwent standard pars plana vitrectomy. After induction of posterior vitreous detachment, epiretinal tissue and the inner limiting membrane (ILM) of the retina were removed, and processed for transmission electron microscopy.
Results: Ultrastructural analysis revealed two basic patterns of vitreoretinal pathology in eyes with vitreomacular traction syndrome. Seven specimens showed mostly single cells or a cellular monolayer covering closely the vitreal side of the ILM, not resulting in a biomicroscopically detectable epiretinal fibrocellular proliferation. The other seven specimens revealed premacular fibrocellular tissue which was separated from the ILM by a layer of native collagen, resembling the clinical features of idiopathic epiretinal membranes. In both groups of eyes, the myofibroblast was the predominant cell type. Fibrous astrocytes and fibrocytes were less frequent. Retinal pigment epithelial cells and macrophages were absent. Deposits of newly formed collagen were present only adjacent to fibrocellular multilayers.
Conclusions: There are two distinct clinicopathological features of vitreomacular traction syndrome which suggest different forms of epiretinal fibrocellular proliferation: (1) epiretinal membranes interposed in native vitreous collagen and (2) single cells or a cellular monolayer proliferating directly on the ILM. The presence of remnants of the cortical vitreous which remain attached to the ILM following posterior vitreous separation may determine the clinicopathological feature of the disease. The predominance of myofibroblasts may help to explain the high prevalence of cystoid macular oedema and progressive vitreomacular traction characteristic for this disorder.
Keywords: vitreomacular traction syndrome; epiretinal membrane; vitreomacular interface
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