Please use this identifier to cite or link to this item: http://hdl.handle.net/11452/21045
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dc.contributor.authorDavies, D. Ceri-
dc.contributor.authorKidd, M.-
dc.contributor.authorDuff, Karen-
dc.contributor.authorHowlett, D.R.-
dc.date.accessioned2021-07-05T07:58:19Z-
dc.date.available2021-07-05T07:58:19Z-
dc.date.issued2003-10-
dc.identifier.citationDavies, D.C. vd. (2003). “Hyperphosphorylated tau and paired helical filament-like structures in the brains of mice carrying mutant amyloid precursor protein and mutant presenilin-1 transgenes”. Neurobiology of Disease, 14(1), 89-97.en_US
dc.identifier.issn0969-9961-
dc.identifier.urihttps://doi.org/10.1016/S0969-9961(03)00084-6-
dc.identifier.urihttps://www.sciencedirect.com/science/article/pii/S0969996103000846-
dc.identifier.urihttp://hdl.handle.net/11452/21045-
dc.description.abstractSenile plaques composed mainly of beta-amyloid (Abeta) and neurofibrillary tangles principally composed of hyperphosphorylated tau are the major pathological features of Alzheimer's disease (AD). Despite the fact that increased expression of amyloid precursor protein (APP) and presenilin-1 (PS1) transgenes in mice lead to increased Abeta deposition in plaquelike structures in the brain, little is known about the nature and distribution of tau in these mice. Therefore the relationship between Abeta and hyperphosphorylated tau was investigated in mice carrying mutant APP and mutant PS1 transgenes using both light (LM) and electron microscopy (EM) with immunocytochemistry. LM immunocytochemistry revealed cerebral Abeta deposits to be present from 8 weeks of age, whereas hyperphosphorylated tau was not detected until 24 weeks of age, when it appeared as punctate deposits in close association with the Abeta deposits in the cortex and hippocampus. However, dystrophic neurites were not as heavily immunolabeled as they are in AD brain. EM revealed that aggregations of straight filaments (10-12 nm wide) were present in some cellular processes at the periphery of Abeta plaques in 8-month-old APP/PS1 mice. In one such mouse, single filaments and paired filaments showing a helical configuration (50-55 nm half-period, 25 nm max. width) were present in a dark, atrophic hippocampal neuron. Immunogold labeling of APP/PS1 mouse brain revealed hyperphosphorylated tau epitopes in some dystrophic neurites from 24 weeks of age that were similar to those present in AD. These results suggest that hyperphosphorylated tau appears in APP/PS1 mouse brain after the onset of Abeta depositition and although it is associated with Abeta deposits, its distribution is not identical to that in AD.en_US
dc.language.isoenen_US
dc.publisherAcademic Press Inc Elsevier Scienceen_US
dc.rightsinfo:eu-repo/semantics/closedAccessen_US
dc.subjectAlzheimer's diseaseen_US
dc.subjectBeta-amyloiden_US
dc.subjectDystrophic neuritesen_US
dc.subjectHyperphosphorylated tauen_US
dc.subjectNeurofibrillary tanglesen_US
dc.subjectPaired helical filamentsen_US
dc.subjectTransgenic mouse brainen_US
dc.subjectFamilial alzheimers-diseaseen_US
dc.subjectA-beta amyloidosisen_US
dc.subjectNeurofibrillary tanglesen_US
dc.subjectElectron microscopyen_US
dc.subjectMissense mutationsen_US
dc.subjectSenile plaquesen_US
dc.subjectGeneen_US
dc.subjectPathologyen_US
dc.subjectAccumulationen_US
dc.subjectPhosphorylationen_US
dc.titleHyperphosphorylated tau and paired helical filament-like structures in the brains of mice carrying mutant amyloid precursor protein and mutant presenilin-1 transgenesen_US
dc.typeArticleen_US
dc.identifier.wos000185438700010tr_TR
dc.identifier.scopus2-s2.0-0042334542tr_TR
dc.relation.publicationcategoryMakale - Uluslararası Hakemli Dergitr_TR
dc.contributor.departmentUludağ Üniversitesi/Tıp Fakültesi.tr_TR
dc.contributor.orcid0000-0003-3368-8123tr_TR
dc.identifier.startpage89tr_TR
dc.identifier.endpage97tr_TR
dc.identifier.volume14tr_TR
dc.identifier.issue1tr_TR
dc.relation.journalNeurobiology of Diseaseen_US
dc.contributor.buuauthorKurt, M. Ayberk-
dc.contributor.researcheridAAR-4341-2020tr_TR
dc.relation.collaborationYurt dışıtr_TR
dc.identifier.pubmed13678670tr_TR
dc.subject.wosNeurosciences & neurologyen_US
dc.subject.wosNeurosciencesen_US
dc.indexed.wosSCIEen_US
dc.indexed.scopusScopusen_US
dc.indexed.pubmedPubmeden_US
dc.wos.quartileQ1en_US
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