Theo L. van der Schaft scite author profile

The purpose of this study was to investigate whether immune complex deposits can be detected in maculae with early stages of ARMD and to explain the assumed macrophage reaction before the disciform reaction. We examined a series of human maculae by direct immunofluorescence light microscopy with antibodies against immunoglobulins, fibrinogen, and complement factors. Transmission electron microscopy was performed to identify the macrophages. Materials and methodsThe maculae of 20 human eyes from 13 subjects were obtained at autopsy or after surgical enucleation for intraocular melanoma. The ages 657 on 7 May 2018 by guest. Protected by copyright.

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Histologic Features of the Early Stages of Age-related Macular Degeneration

Schaft

et al. 1992

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Increased prevalence of disciform macular degeneration after cataract extraction with implantation of an intraocular lens.

Schaft

Mooy

Bruijn

et al. 1994

British Journal of Ophthalmology

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Immunohistochemical light and electron microscopy of basal laminar deposit

Schaft

Mooy

Bruijn

et al. 1994

Graefe's Arch Clin Exp Ophthalmol

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The formation of basal laminar deposit (BLD) is one of the histopathologic changes in the aging human macula. BLD is assumed to be an early stage of age-related macular degeneration. The location of BLD, between the RPE plasma membrane and its basement membrane and in the outer collagenous zone of Bruch's membrane, and its ultrastructure suggest that it is composed of excessive amounts of basement membrane material. The main components of basement membranes are type IV collagen, heparan sulfate proteoglycans (HSPG) and laminin. Labeled antibodies against these components can therefore be used for the identification and localization of basement membrane material by means of immunohistochemical techniques. In this study the presence of type IV collagen, laminin and HSPG was determined in aged human maculae by immunohistochemistry and immunoelectron microscopy. Tests for the presence of type VI collagen and fibronectin were also performed. We obtained 76 eyes from 68 human subjects at autopsy or after surgical enucleation for anteriorly located choroidal melanomas. The finely granular component of BLD stained positive with antibodies against type IV collagen, HSPG and laminin, but the long-spacing collagen component of BLD did not. Neither component of BLD was stained with antibodies against type VI collagen or fibronectin. We conclude that BLD consists partly of excess basement membrane material.

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Morphologic changes in age‐related maculopathy

Kliffen

Schaft

Mooy

et al. 1997

Microsc. Res. Tech.

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Age-related maculopathy (ARM) is a degenerative disorder of the central part of the retina with a rising prevalence in patients 50 years of age and older, and comprises different histopathological changes. The morphologic changes in ARM are described and illustrated with light-microscopical, electron microscopical, and fundus pictures. Furthermore, the most important biochemical data are given. The most prominent aging changes in early stages of ARM are drusen and basal laminar deposit (BLD), both extracellular deposits, that are assumed to be important in the development of ARM. Drusen accumulate within Bruch's membrane, whereas BLD is present between Bruch's membrane and the retinal pigment epithelium. Although the histopathologic characteristics of the deposits are well documented, the chemical composition has only been partly resolved. Biochemical analysis of these deposits is necessary to determine the source of the deposits and to find possible ways to avoid or treat them. The late stages of ARM, geographic atrophy, and neovascular (disciform) degeneration, are called age-related macular degeneration (AMD), and result in severe and irreversible visual impairment. Since there is still no adequate therapy for the majority of people disabled by AMD, and because of the aging population resulting in even more patients with this disease, it is necessary to intensify the research on ARM in order to prevent AMD or find a therapy for it.

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