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Psychotic Alzheimer's disease is associated with gender-specific tau phosphorylation abnormalities
Authors:Jeremy Koppel  Chris Acker  Peter Davies  Oscar L. Lopez  Heidy Jimenez  Miriam Azose  Blaine S. Greenwald  Patrick S. Murray  Caitlin M. Kirkwood  Julia Kofler  Robert A. Sweet
Affiliation:1. The Litwin-Zucker Research Center for the Study of Alzheimer''s Disease, The Feinstein Institute for Medical Research, Manhasset, NY, USA;2. The Zucker Hillside Hospital, The North-Shore LIJ Health System, Glen Oaks, NY, USA;3. Department of Psychiatry, University of Pittsburgh, Pittsburgh, PA, USA;4. Department of Neurology, University of Pittsburgh, Pittsburgh, PA, USA;5. Touro College, Brooklyn, NY, USA;6. VISN Q2 4 Mental Illness Research, Education and Clinical Center (MIRECC), VA Pittsburgh Healthcare System, Pittsburgh, PA, USA
Abstract:Converging evidence suggests that psychotic Alzheimer's disease (AD + P) is associated with an acceleration of frontal degeneration, with tau pathology playing a primary role. Previous histopathologic and biomarker studies have specifically implicated tau pathology in this condition. To precisely quantify tau abnormalities in the frontal cortex in AD + P, we used a sensitive biochemical assay of total tau and 4 epitopes of phospho-tau relevant in AD pathology in a postmortem sample of AD + P and AD − P. Samples of superior frontal gyrus from 26 AD subjects without psychosis and 45 AD + P subjects with psychosis were analyzed. Results of enzyme-linked immunosorbent assay demonstrate that AD + P females, but not males, had significantly higher levels of phosphorylated tau in the frontal cortex. In males, but not females, AD + P was associated with the presence of α-synuclein pathology. These results support a gender dissociation of pathology in AD + P. The design of future studies aimed at the elucidation of cognitive and/or functional outcomes; regional brain metabolic deficits; or genetic correlates of AD + P should take gender into consideration.
Keywords:Alzheimer's disease   Psychosis   Tau   Dementia with Lewy bodies   Alpha-synuclein   Neurofibrillary tangles
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