Mutant Tau knock-in mice display frontotemporal dementia relevant behaviour and histopathology

David J. Koss; Lianne Robinson; Benjamin D. Drever; Kaja Plucińska; Sandra Stoppelkamp; Peter Veselcic; Gernot Riedel; Bettina Platt

doi:10.1016/j.nbd.2016.03.002

Mutant Tau knock-in mice display frontotemporal dementia relevant behaviour and histopathology

David J. Koss, Lianne Robinson, Benjamin D. Drever, Kaja Plucińska, Sandra Stoppelkamp, Peter Veselcic, Gernot Riedel (Lead / Corresponding author), Bettina Platt (Lead / Corresponding author)

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Abstract

Models of Tau pathology related to frontotemporal dementia (FTD) are essential to determine underlying neurodegenerative pathologies and resulting tauopathy relevant behavioural changes. However, existing models are often limited in their translational value due to Tau overexpression, and the frequent occurrence of motor deficits which prevent comprehensive behavioural assessments. In order to address these limitations, a forebrain-specific (CaMKIIα promoter), human mutated Tau (hTau_P301L ₊ _R406W) knock-in mouse was generated out of the previously characterised PLB1_Triple mouse, and named PLB2_Tau. After confirmation of an additional hTau species (~60 kDa) in forebrain samples, we identified age-dependent progressive Tau phosphorylation which coincided with the emergence of FTD relevant behavioural traits. In line with the non-cognitive symptomatology of FTD, PLB2_Tau mice demonstrated early emerging (~6 months) phenotypes of heightened anxiety in the elevated plus maze, depressive/apathetic behaviour in a sucrose preference test and generally reduced exploratory activity in the absence of motor impairments. Investigations of cognitive performance indicated prominent dysfunctions in semantic memory, as assessed by social transmission of food preference, and in behavioural flexibility during spatial reversal learning in a home cage corner-learning task. Spatial learning was only mildly affected and task-specific, with impairments at 12 months of age in the corner learning but not in the water maze task. Electroencephalographic (EEG) investigations indicated a vigilance-stage specific loss of alpha power during wakefulness at both parietal and prefrontal recording sites, and site-specific EEG changes during non-rapid eye movement sleep (prefrontal) and rapid eye movement sleep (parietal). Further investigation of hippocampal electrophysiology conducted in slice preparations indicated a modest reduction in efficacy of synaptic transmission in the absence of altered synaptic plasticity. Together, our data demonstrate that the transgenic PLB2_Tau mouse model presents with a striking behavioural and physiological face validity relevant for FTD, driven by the low level expression of mutant FTD hTau.

Original language	English
Pages (from-to)	105-123
Number of pages	19
Journal	Neurobiology of Disease
Volume	91
Early online date	4 Mar 2016
DOIs	https://doi.org/10.1016/j.nbd.2016.03.002
Publication status	Published - Jul 2016

Keywords

Anhedonia
Apathy
Cognition
EEG
Frontotemporal dementia
Phosphorylation
Semantic memory
Spatial memory
Tau
Tauopathies

ASJC Scopus subject areas

Neurology

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title = "Mutant Tau knock-in mice display frontotemporal dementia relevant behaviour and histopathology",

abstract = "Models of Tau pathology related to frontotemporal dementia (FTD) are essential to determine underlying neurodegenerative pathologies and resulting tauopathy relevant behavioural changes. However, existing models are often limited in their translational value due to Tau overexpression, and the frequent occurrence of motor deficits which prevent comprehensive behavioural assessments. In order to address these limitations, a forebrain-specific (CaMKIIα promoter), human mutated Tau (hTauP301L + R406W) knock-in mouse was generated out of the previously characterised PLB1Triple mouse, and named PLB2Tau. After confirmation of an additional hTau species (~60 kDa) in forebrain samples, we identified age-dependent progressive Tau phosphorylation which coincided with the emergence of FTD relevant behavioural traits. In line with the non-cognitive symptomatology of FTD, PLB2Tau mice demonstrated early emerging (~6 months) phenotypes of heightened anxiety in the elevated plus maze, depressive/apathetic behaviour in a sucrose preference test and generally reduced exploratory activity in the absence of motor impairments. Investigations of cognitive performance indicated prominent dysfunctions in semantic memory, as assessed by social transmission of food preference, and in behavioural flexibility during spatial reversal learning in a home cage corner-learning task. Spatial learning was only mildly affected and task-specific, with impairments at 12 months of age in the corner learning but not in the water maze task. Electroencephalographic (EEG) investigations indicated a vigilance-stage specific loss of alpha power during wakefulness at both parietal and prefrontal recording sites, and site-specific EEG changes during non-rapid eye movement sleep (prefrontal) and rapid eye movement sleep (parietal). Further investigation of hippocampal electrophysiology conducted in slice preparations indicated a modest reduction in efficacy of synaptic transmission in the absence of altered synaptic plasticity. Together, our data demonstrate that the transgenic PLB2Tau mouse model presents with a striking behavioural and physiological face validity relevant for FTD, driven by the low level expression of mutant FTD hTau.",

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author = "Koss, {David J.} and Lianne Robinson and Drever, {Benjamin D.} and Kaja Pluci{\'n}ska and Sandra Stoppelkamp and Peter Veselcic and Gernot Riedel and Bettina Platt",

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AU - Drever, Benjamin D.

AU - Plucińska, Kaja

AU - Stoppelkamp, Sandra

AU - Veselcic, Peter

AU - Riedel, Gernot

AU - Platt, Bettina

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KW - EEG

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KW - Semantic memory

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ER -

Mutant Tau knock-in mice display frontotemporal dementia relevant behaviour and histopathology

Abstract

Keywords

ASJC Scopus subject areas

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