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Association of apolipoprotein J-positive β-amyloid plaques with dystrophic neurites in alzheimer’s disease brain
Authors:Matthew D. Martin-Rehrmann  Hyang-Sook Hoe  Eleonora M. Capuani  G. William Rebeck
Affiliation:1. Alzheimer Research Unit, Massachusetts General Hospital, 02129, Charlestown, MA, USA
2. Department of Neuroscience, Georgetown University Medical Center, 20007, Washington, DC, USA
3. Graduate School of Neural and Behavioural Sciences, International Max Planck Research School, University of Tuebingen, Tuebingen, Germany
Abstract:Apolipoprotein J (apoJ), also known as clusterin and SP-40,40, binds soluble beta-amyloid (Aβ and is up-regulated in the Alzheimer’s disease (AD) brain. In the present study we classified apoJ-immunopositive Aβ deposits in AD temporal cortex, and found apoJ-immunoreactive plaques were often associated with dystrophic neurites. Quantitative immunohistochemical analysis of five AD brains showed that 29% of Aβ deposited in the parenchyma was associated with apoJ. Of Aβ deposits with apoJ immunopositivity, 71% were associated with phospho-tau-positive dystrophic neurites in the surrounding tissue. Conversely, 64% of phospho-tau-labeled neuritic deposits were labeled with apoJ. ApoJ was found at the core of these deposits, and co-localized with the amyloid staining agent thioflavine-S. To test the direct effects of apoJ on tau metabolism, we treated cells in culture with apoJ-containing conditioned media, and we injected apoJ-containing media into the rat hippocampus. Using both systems, we observed increases in levels of tau and phosphorylated tau. Our findings demonstrate that apoJ immunopositivity strongly correlates with the presence of amyloid and associated neuritic dystrophy in the neuropil of AD temporal cortex, and supports a model where extracellular apoJ facilitates the conversion of diffuse Aβ deposits into amyloid and enhances tau phosphorylation in neurites surrounding these plaques.
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