FAD-mutation of APP is associated with a loss of its synaptotrophic activity

FAD-mutation of APP is associated with a loss of its synaptotrophic activity

Alzheimer's disease (AD) is a chronic neurodegenerative disorder associated with extracellular accumulation of Aβ peptide that derives from the amyloid precursor protein (APP). While amyloidogenic processing of APP has received most attention, the physiological function of APP and the sequelae...

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Main Authors: Gudrun Seeger, Ulrich Gärtner, Uwe Ueberham, Susanne Rohn, Thomas Arendt
Format: Article
Language:English
Published: Elsevier 2009-08-01
Series:Neurobiology of Disease
Subjects:
Mouse model
Alzheimer's disease
Neocortex
APP
FAD-linked mutations
Quantitative ultrastructural analysis
Online Access:http://www.sciencedirect.com/science/article/pii/S096999610900103X
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spelling doaj-d1b4346d6cfc4c948353651daef26fda2021-03-20T04:57:34ZengElsevierNeurobiology of Disease1095-953X2009-08-01352258263FAD-mutation of APP is associated with a loss of its synaptotrophic activityGudrun Seeger0Ulrich Gärtner1Uwe Ueberham2Susanne Rohn3Thomas Arendt4Department for Molecular and Cellular Mechanisms of Neurodegeneration, Paul Flechsig Institute of Brain Research, University of Leipzig, Jahnallee 59, D-04109 Leipzig, GermanyDepartment for Molecular and Cellular Mechanisms of Neurodegeneration, Paul Flechsig Institute of Brain Research, University of Leipzig, Jahnallee 59, D-04109 Leipzig, GermanyDepartment for Molecular and Cellular Mechanisms of Neurodegeneration, Paul Flechsig Institute of Brain Research, University of Leipzig, Jahnallee 59, D-04109 Leipzig, GermanyDepartment for Molecular and Cellular Mechanisms of Neurodegeneration, Paul Flechsig Institute of Brain Research, University of Leipzig, Jahnallee 59, D-04109 Leipzig, GermanyCorresponding author. Fax: +49 341 9725729.; Department for Molecular and Cellular Mechanisms of Neurodegeneration, Paul Flechsig Institute of Brain Research, University of Leipzig, Jahnallee 59, D-04109 Leipzig, GermanyAlzheimer's disease (AD) is a chronic neurodegenerative disorder associated with extracellular accumulation of Aβ peptide that derives from the amyloid precursor protein (APP). While amyloidogenic processing of APP has received most attention, the physiological function of APP and the sequelae of potentially impaired APP function are less understood. APP is a transmembrane glycoprotein being widely expressed in neurons in both central and peripheral nervous system. Its physiological function has been associated with neuronal survival, neurite outgrowth and neuronal plasticity. The aim of the present study was to determine whether FAD-linked mutations of APP, known to be associated with early onset of the disease, might impair its synaptotrophic function, potentially contributing to synaptic deficiencies seen in AD. We performed a quantitative electron microscopy study on synapses in well characterized expression-matched transgenic mice lines expressing either wildtype or FAD-mutated hAPP. Using serial electron microscopic sections, we comparatively analyzed by stereological methods the number and sizes of synaptic contacts and the number of synaptic vesicles in the neocortex. We could clearly show a synaptotrophic effect in mice overexpressing wildtype hAPP evidenced by a significant increase in the number of synapses and the number of vesicles per synapse. This effect was abolished when FAD-mutated APPSw,Ind was expressed instead of wildtype APP. The present study demonstrates a synaptotrophic effect of APP which is lost in the presence of a FAD-mutation. This failure could either be due to a synaptotoxic effect of Aβ potentially counteracting the synaptotrophic effect of APP. Alternatively, the FAD-mutation might impair the physiological function of the extracellular domain of APP and its fragments which might be required for the synaptotrophic effect. This suggests that not only “too much Aβ” but also “too less functional intact APP” might be relevant for synaptic pathology and degeneration in AD.http://www.sciencedirect.com/science/article/pii/S096999610900103XMouse modelAlzheimer's diseaseNeocortexAPPFAD-linked mutationsQuantitative ultrastructural analysis
collection DOAJ
language English
format Article
sources DOAJ
author Gudrun Seeger
Ulrich Gärtner
Uwe Ueberham
Susanne Rohn
Thomas Arendt
spellingShingle Gudrun Seeger
Ulrich Gärtner
Uwe Ueberham
Susanne Rohn
Thomas Arendt
FAD-mutation of APP is associated with a loss of its synaptotrophic activity
Neurobiology of Disease
Mouse model
Alzheimer's disease
Neocortex
APP
FAD-linked mutations
Quantitative ultrastructural analysis
author_facet Gudrun Seeger
Ulrich Gärtner
Uwe Ueberham
Susanne Rohn
Thomas Arendt
author_sort Gudrun Seeger
title FAD-mutation of APP is associated with a loss of its synaptotrophic activity
title_short FAD-mutation of APP is associated with a loss of its synaptotrophic activity
title_full FAD-mutation of APP is associated with a loss of its synaptotrophic activity
title_fullStr FAD-mutation of APP is associated with a loss of its synaptotrophic activity
title_full_unstemmed FAD-mutation of APP is associated with a loss of its synaptotrophic activity
title_sort fad-mutation of app is associated with a loss of its synaptotrophic activity
publisher Elsevier
series Neurobiology of Disease
issn 1095-953X
publishDate 2009-08-01
description Alzheimer's disease (AD) is a chronic neurodegenerative disorder associated with extracellular accumulation of Aβ peptide that derives from the amyloid precursor protein (APP). While amyloidogenic processing of APP has received most attention, the physiological function of APP and the sequelae of potentially impaired APP function are less understood. APP is a transmembrane glycoprotein being widely expressed in neurons in both central and peripheral nervous system. Its physiological function has been associated with neuronal survival, neurite outgrowth and neuronal plasticity. The aim of the present study was to determine whether FAD-linked mutations of APP, known to be associated with early onset of the disease, might impair its synaptotrophic function, potentially contributing to synaptic deficiencies seen in AD. We performed a quantitative electron microscopy study on synapses in well characterized expression-matched transgenic mice lines expressing either wildtype or FAD-mutated hAPP. Using serial electron microscopic sections, we comparatively analyzed by stereological methods the number and sizes of synaptic contacts and the number of synaptic vesicles in the neocortex. We could clearly show a synaptotrophic effect in mice overexpressing wildtype hAPP evidenced by a significant increase in the number of synapses and the number of vesicles per synapse. This effect was abolished when FAD-mutated APPSw,Ind was expressed instead of wildtype APP. The present study demonstrates a synaptotrophic effect of APP which is lost in the presence of a FAD-mutation. This failure could either be due to a synaptotoxic effect of Aβ potentially counteracting the synaptotrophic effect of APP. Alternatively, the FAD-mutation might impair the physiological function of the extracellular domain of APP and its fragments which might be required for the synaptotrophic effect. This suggests that not only “too much Aβ” but also “too less functional intact APP” might be relevant for synaptic pathology and degeneration in AD.
topic Mouse model
Alzheimer's disease
Neocortex
APP
FAD-linked mutations
Quantitative ultrastructural analysis
url http://www.sciencedirect.com/science/article/pii/S096999610900103X
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