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Genetically augmenting tau levels does not modulate the onset or progression of Aβ pathology in transgenic mice
Author(s) -
Oddo Salvatore,
Caccamo Antonella,
Cheng David,
Jouleh Bahareh,
Torp Reidun,
LaFerla Frank M.
Publication year - 2007
Publication title -
journal of neurochemistry
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.75
H-Index - 229
eISSN - 1471-4159
pISSN - 0022-3042
DOI - 10.1111/j.1471-4159.2007.04607.x
Subject(s) - tauopathy , tau pathology , genetically modified mouse , hyperphosphorylation , transgene , neuroscience , pathology , tau protein , amyloid (mycology) , biology , alzheimer's disease , medicine , disease , neurodegeneration , microbiology and biotechnology , phosphorylation , genetics , gene
The two hallmark pathologies of Alzheimer’s disease (AD) are amyloid plaques, composed of the small amyloid‐β (Aβ) peptide, and neurofibrillary tangles, comprised aggregates of the microtubule binding protein, tau. The molecular linkage between these two lesions, however, remains unknown. Based on human and mouse studies, it is clear that the development of Aβ pathology can trigger tau pathology, either directly or indirectly. However, it remains to be established if the interaction between Aβ and tau is bidirectional and whether the modulation of tau will influence Aβ pathology. To address this question, we used the 3xTg‐AD mouse model, which is characterized by the age‐dependent buildup of both plaques and tangles. Here we show that genetically augmenting tau levels and hyperphosphorylation in the 3xTg‐AD mice has no effect on the onset and progression of Aβ pathology. These data suggest that the link between Aβ and tau is predominantly if not exclusively unidirectional, which is consistent with the Aβ cascade hypothesis and may explain why tauopathy‐only disorders are devoid of any Aβ pathology.