Combining P301L and S320F tau variants produces a novel accelerated model of tauopathy

Koller, Emily J.; Cruz, Elsa Gonzalez De La; Machula, Timothy A.; Ibanez, Kristen R.; Lin, Wen Lang; Williams, Tosha; Riffe, Cara J.; Ryu, Doojin; Strang, Kevin H.; Liu, Xuefei; Janus, Christopher; Golde, Todd E.; Dickson, Dennis W.; Chakrabarty, Paramita

doi:10.1093/hmg/ddz151

Cited by 26 publications

(41 citation statements)

References 48 publications

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“…Consistent with reports from other laboratories (Ramsden et al, 2005 ; Schindowski et al, 2006 ), we observed that mice with accelerated NFT deposits also developed rapid memory impairment (Koller et al, 2019 ). While our results were consistent with human data (reviewed in Nelson et al, 2012 ), other preclinical studies have shown that tau conformers, independent of NFT, underlie memory deficits and network alterations (Santacruz et al, 2005 ; Bolós et al, 2017 ; Green et al, 2019 ).…”

Section: Neuroplasticity Loss In Ad and Related Tauopathiessupporting

confidence: 93%

“…Gliosis closely follows the development of tauopathy in transgenic mouse models (Ramsden et al, 2005 ; Schindowski et al, 2006 ; Yoshiyama et al, 2007 ; de Calignon et al, 2012 ; Maeda et al, 2016 ). We developed several mouse models of tauopathy in our lab to understand how gliosis is differentially regulated in the presence of intracellular phosphorylated tau and NFT inclusions (Koller et al, 2019 ). These models express different human mutant tau constructs following neonatal delivery of recombinant adeno-associated viruses (AAV).…”

Section: Neuroplasticity Loss In Ad and Related Tauopathiesmentioning

confidence: 99%

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Tau-Mediated Dysregulation of Neuroplasticity and Glial Plasticity

Koller

Chakrabarty

2020

Front. Mol. Neurosci.

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The inability of individual neurons to compensate for aging-related damage leads to a gradual loss of functional plasticity in the brain accompanied by progressive impairment in learning and memory. Whereas this loss in neuroplasticity is gradual during normal aging, in neurodegenerative diseases such as Alzheimer's disease (AD), this loss is accelerated dramatically, leading to the incapacitation of patients within a decade of onset of cognitive symptoms. The mechanisms that underlie this accelerated loss of neuroplasticity in AD are still not completely understood. While the progressively increasing proteinopathy burden, such as amyloid β (Aβ) plaques and tau tangles, definitely contribute directly to a neuron's functional demise, the role of non-neuronal cells in controlling neuroplasticity is slowly being recognized as another major factor. These non-neuronal cells include astrocytes, microglia, and oligodendrocytes, which through regulating brain homeostasis, structural stability, and trophic support, play a key role in maintaining normal functioning and resilience of the neuronal network. It is believed that chronic signaling from these cells affects the homeostatic network of neuronal and non-neuronal cells to an extent to destabilize this harmonious milieu in neurodegenerative diseases like AD. Here, we will examine the experimental evidence regarding the direct and indirect pathways through which astrocytes and microglia can alter brain plasticity in AD, specifically as they relate to the development and progression of tauopathy. In this review article, we describe the concepts of neuroplasticity and glial plasticity in healthy aging, delineate possible mechanisms underlying tau-induced plasticity dysfunction, and discuss current clinical trials as well as future disease-modifying approaches.

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Section: Neuroplasticity Loss In Ad and Related Tauopathiessupporting

confidence: 93%

Section: Neuroplasticity Loss In Ad and Related Tauopathiesmentioning

confidence: 99%

Tau-Mediated Dysregulation of Neuroplasticity and Glial Plasticity

Koller

Chakrabarty

2020

Front. Mol. Neurosci.

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“…Using a panel of FTD-associated tau mutants, HDAC6 showed increased binding to P301L and S320F mutations. The exact properties of these particular mutants that enable more robust engagement with HDAC6 is not clear, however a recent study indicated synergistic aggregation and seeding of the P301L and S320F mutations [59][60][61] . Our data suggest that HDAC6 may preferentially target specific aggregate-prone conformations, or strains, via a chaperone bridge, as mutations that abrogate tau-chaperone binding also diminished tau-HDAC6 binding (Fig.…”

Section: Discussionmentioning

confidence: 99%

An HDAC6-dependent surveillance mechanism suppresses tau-mediated neurodegeneration and cognitive decline

Trzeciakiewicz

Ajit²,

Tseng³

et al. 2020

Nat Commun

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Tauopathies including Alzheimer’s disease (AD) are marked by the accumulation of aberrantly modified tau proteins. Acetylated tau, in particular, has recently been implicated in neurodegeneration and cognitive decline. HDAC6 reversibly regulates tau acetylation, but its role in tauopathy progression remains unclear. Here, we identified an HDAC6-chaperone complex that targets aberrantly modified tau. HDAC6 not only deacetylates tau but also suppresses tau hyperphosphorylation within the microtubule-binding region. In neurons and human AD brain, HDAC6 becomes co-aggregated within focal tau swellings and human AD neuritic plaques. Using mass spectrometry, we identify a novel HDAC6-regulated tau acetylation site as a disease specific marker for 3R/4R and 3R tauopathies, supporting uniquely modified tau species in different neurodegenerative disorders. Tau transgenic mice lacking HDAC6 show reduced survival characterized by accelerated tau pathology and cognitive decline. We propose that a HDAC6-dependent surveillance mechanism suppresses toxic tau accumulation, which may protect against the progression of AD and related tauopathies.

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“…The tau inclusions that form are insoluble, Thioflavin S positive, and show fibrillar structure by electron microscopy (EM) [ 10 ]. Notably, BSCs are highly predictive of results obtained upon transgenic or rAAV-mediated expression of tau in rodent models [ 35 ].…”

Section: Introductionmentioning

confidence: 99%

Photodynamic studies reveal rapid formation and appreciable turnover of tau inclusions

et al. 2021

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Accumulation of the tau protein in fibrillar intracellular aggregates is a defining feature of multiple neurodegenerative diseases collectively referred to as tauopathies. Despite intensive study of tau, there is limited information on the formation and clearance dynamics of tau inclusions. Using rAAV vectors to mediate expression of Dendra2-tagged human wild-type, P301L and pro-aggregant P301L/S320F tau proteins, with and without the addition of exogenous tau fibrillar seeds, we evaluated tau inclusion dynamics in organotypic brain slice culture (BSC) models using long-term optical pulse labeling methodology. Our studies reveal that tau inclusions typically form in 12–96 h in tauopathy BSC models. Unexpectedly, we demonstrate appreciable turnover of tau within inclusions with an average half-life of ~ 1 week when inclusions are newly formed. When BSCs with inclusions are aged in culture for extended periods, tau inclusions continue to turnover, but their half-lives increase to ~ 2 weeks and ~ 3 weeks after 1 and 2 months in culture, respectively. Individual tau inclusions can be long-lived structures that can persist for months in these BSC models and for even longer in the human brain. However, our data indicate that tau inclusions, are not ‘tombstones’, but dynamic structures with appreciable turnover. Understanding the cellular processes mediating this inclusion turnover may lead to new therapeutic strategies that could reverse pathological tau inclusion formation.

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Combining P301L and S320F tau variants produces a novel accelerated model of tauopathy

Cited by 26 publications

References 48 publications

Tau-Mediated Dysregulation of Neuroplasticity and Glial Plasticity

Tau-Mediated Dysregulation of Neuroplasticity and Glial Plasticity

An HDAC6-dependent surveillance mechanism suppresses tau-mediated neurodegeneration and cognitive decline

Photodynamic studies reveal rapid formation and appreciable turnover of tau inclusions

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