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P73 Regulates Neurodegeneration and Phospho-tau Accumulation During Aging and Alzheimer's Disease

Overview
Journal Neuron
Publisher Cell Press
Specialty Neurology
Date 2008 Sep 13
PMID 18786355
Citations 54
Authors
Monica K Wetzel
Sibel Naska
Christine L Laliberte
Vladimir V Rymar
Masashi Fujitani
Jeffrey A Biernaskie
Christy J Cole
Jason P Lerch
Shoshana Spring
S-H Wang
Paul W Frankland
R Mark Henkelman
Sheena A Josselyn
Abbas F Sadikot
Freda D Miller
David R Kaplan
Affiliations
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Abstract

The genetic mechanisms that regulate neurodegeneration are only poorly understood. We show that the loss of one allele of the p53 family member, p73, makes mice susceptible to neurodegeneration as a consequence of aging or Alzheimer's disease (AD). Behavioral analyses demonstrated that old, but not young, p73+/- mice displayed reduced motor and cognitive function, CNS atrophy, and neuronal degeneration. Unexpectedly, brains of aged p73+/- mice demonstrated dramatic accumulations of phospho-tau (P-tau)-positive filaments. Moreover, when crossed to a mouse model of AD expressing a mutant amyloid precursor protein, brains of these mice showed neuronal degeneration and early and robust formation of tangle-like structures containing P-tau. The increase in P-tau was likely mediated by JNK; in p73+/- neurons, the activity of the p73 target JNK was enhanced, and JNK regulated P-tau levels. Thus, p73 is essential for preventing neurodegeneration, and haploinsufficiency for p73 may be a susceptibility factor for AD and other neurodegenerative disorders.

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