TY - JOUR
T1 - A novel transgenic mouse expressing double mutant tau driven by its natural promoter exhibits tauopathy characteristics
AU - Rosenmann, Hanna
AU - Grigoriadis, Nikolaos
AU - Eldar-Levy, Hila
AU - Avital, Avi
AU - Rozenstein, Lea
AU - Touloumi, Olga
AU - Behar, Leah
AU - Ben-Hur, Tamir
AU - Avraham, Yosefa
AU - Berry, Elliot
AU - Segal, Menahem
AU - Ginzburg, Irith
AU - Abramsky, Oded
PY - 2008/7
Y1 - 2008/7
N2 - The neurofibrillary-tangles (NTFs), characteristic of tauopathies including Alzheimer's-disease (AD), are the pathological features which correlate best with dementia. The objective of our study was to generate an authentic transgenic (tg) animal model for NFT pathology in tauopathy/AD. Previous NFT-tg mice were driven by non-related/non-homologous promoters. Our strategy was to use the natural tau promoter for expressing the human-tau (htau) gene with two mutations K257T/P301S (double mutant, DM) associated with severe phenotypes of frontotemporal-dementia in humans. Cellular, biochemical, behavioral and electrophysiological studies were subsequently conducted. The tg mice showed a tolerated physiological level of the DM-htau protein, mostly in cortex and hippocampus. The mice demonstrated tauopathy-like characteristics, which increased with age, that included NFT-related pathology, astrogliosis, argyrophilic plaque-like (amyloid-free) structures in brain, with memory deficits and signs of anxiety. Moreover, the tg mice showed a robust synaptic plasticity deficit selectively expressed in a severe impairment in their ability to maintain hippocampal long-term-potentiation (LTP) in response to stimulation of the perforant path, providing evidence that "tau-pathology only" is sufficient to cause this memory and learning-associated deficit. This is a unique mutant-htau-tg model which presents a wide spectrum of features characteristic of tauopathy/AD, which does not show unrelated motor deficits described in other models of tauopathy. In addition, expressing the DM-htau in a neuronal cell model resulted in tau-aggregation, as well as impaired microtubule arrangement. Both animal and cell models, which were regulated under the natural tau promoter (of rat origin), provide authentic and reliable models for tauopathy, and offer valuable tools for understanding the molecular events underlying tauopathies including AD.
AB - The neurofibrillary-tangles (NTFs), characteristic of tauopathies including Alzheimer's-disease (AD), are the pathological features which correlate best with dementia. The objective of our study was to generate an authentic transgenic (tg) animal model for NFT pathology in tauopathy/AD. Previous NFT-tg mice were driven by non-related/non-homologous promoters. Our strategy was to use the natural tau promoter for expressing the human-tau (htau) gene with two mutations K257T/P301S (double mutant, DM) associated with severe phenotypes of frontotemporal-dementia in humans. Cellular, biochemical, behavioral and electrophysiological studies were subsequently conducted. The tg mice showed a tolerated physiological level of the DM-htau protein, mostly in cortex and hippocampus. The mice demonstrated tauopathy-like characteristics, which increased with age, that included NFT-related pathology, astrogliosis, argyrophilic plaque-like (amyloid-free) structures in brain, with memory deficits and signs of anxiety. Moreover, the tg mice showed a robust synaptic plasticity deficit selectively expressed in a severe impairment in their ability to maintain hippocampal long-term-potentiation (LTP) in response to stimulation of the perforant path, providing evidence that "tau-pathology only" is sufficient to cause this memory and learning-associated deficit. This is a unique mutant-htau-tg model which presents a wide spectrum of features characteristic of tauopathy/AD, which does not show unrelated motor deficits described in other models of tauopathy. In addition, expressing the DM-htau in a neuronal cell model resulted in tau-aggregation, as well as impaired microtubule arrangement. Both animal and cell models, which were regulated under the natural tau promoter (of rat origin), provide authentic and reliable models for tauopathy, and offer valuable tools for understanding the molecular events underlying tauopathies including AD.
KW - Alzheimer Disease/genetics
KW - Animals
KW - Brain/metabolism
KW - Disease Models, Animal
KW - Disease Progression
KW - Female
KW - Genetic Predisposition to Disease/genetics
KW - Hippocampus/metabolism
KW - Humans
KW - Long-Term Potentiation/genetics
KW - Memory Disorders/genetics
KW - Mice
KW - Mice, Inbred BALB C
KW - Mice, Inbred C57BL
KW - Mice, Transgenic
KW - Microtubules/metabolism
KW - Mutation/genetics
KW - Neurofibrillary Tangles/genetics
KW - Promoter Regions, Genetic/genetics
KW - Rats
KW - Tauopathies/genetics
KW - tau Proteins/genetics
UR - http://www.scopus.com/inward/record.url?scp=44949185340&partnerID=8YFLogxK
U2 - 10.1016/j.expneurol.2008.03.007
DO - 10.1016/j.expneurol.2008.03.007
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C2 - 18490011
SN - 0014-4886
VL - 212
SP - 71
EP - 84
JO - Experimental Neurology
JF - Experimental Neurology
IS - 1
ER -