Familial globular glial tauopathy linked to MAPT mutations: molecular neuropathology and seeding capacity of a prototypical mixed neuronal and glial tauopathy

Ferrer, Isidró; Andrés‐Benito, Pol; Zelaya, María Victoria; Aguirre, M.E. Erro; Carmona, Margarita; Ausín, Karina; Lachén-Montes, Mercedes; Fernández‐Irigoyen, Joaquín; Santamaría, Enrique; Río, José Antonio del

doi:10.1007/s00401-019-02122-9

Cited by 42 publications

(75 citation statements)

References 136 publications

(148 reference statements)

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“…Localization of phospho-tau in neurons and oligodendrocytes in AGD-inoculated mice was identified with double-labeling immunofluorescence with anti-phospho-tau antibodies in combination with NeuN and Olig2 antibodies, respectively ( Figures 7A–C ). Antibodies anti-p38-P (Thr180-Tyr182) revealed co-localization with phospho-tau (AT8) in the majority of grains or dots ( Figure 7D ), as well as in pre-tangles and coiled bodies, as detailed in other tauopathies ( Ferrer et al, 2018 , 2019 , 2020a ).…”

Section: Resultsmentioning

confidence: 73%

“…Tau seeding and spreading occur following unilateral inoculation of sarkosyl-insoluble fractions from AD, PART, ARTAG, PSP, PiD, FTLD linked to MAPT P301L mutation, and GGT in the hippocampus of WT mice using the protocol utilized in the present study ( Ferrer et al, 2018 , 2019 , 2020a , b ). Neurons and oligodendrocytes are the main targets of tau spreading, which progresses through synaptically connected areas, and along tracts such as the corpus callosum to reach the contralateral hemisphere in those settings.…”

Section: Discussionmentioning

confidence: 99%

“…Endogenous mouse tau is accumulated in oligodendrocytes in mice expressing transgenic human tau, thus indicating that mouse tau has the capacity to be recruited and aggregated in oligodendrocytes ( Ren et al, 2014 ). Moreover, oligodendrocytes are the only cell targets, beside threads, following inoculation of sarkosyl-insoluble fractions from a wide variety of tauopathies in the corpus callosum of WT mice ( Ferrer et al, 2018 , 2019 , 2020a , b ). Similarly, human tau can be trapped by axons following inoculation.…”

Section: Discussionmentioning

confidence: 99%

“…Our previous studies have shown tau seeding and spreading following inoculation of sarkosyl-insoluble fractions from AD, primary age-related tauopathy (PART), aging-related tau astrogliopathy (ARTAG), progressive supranuclear palsy (PSP), Pick’s disease (PiD), frontotemporal lobar degeneration linked to MAPT P301L mutation, and sporadic and familial globular glial tauopathy (GGT) into the hippocampus and corpus callosum of WT mice ( Ferrer et al, 2018 , 2019 , 2020a , b ). The present study is focused on the capacity for and characteristics of seeding and propagation of phospho-tau from homogenates of “pure” (not associated with AD or other tauopathies) AGD cases in the hippocampus of WT mice.…”

Section: Introductionmentioning

confidence: 99%

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Capacity for Seeding and Spreading of Argyrophilic Grain Disease in a Wild-Type Murine Model; Comparisons With Primary Age-Related Tauopathy

Ferrer

Andrés‐Benito

Sala-Jarque

et al. 2020

Front. Mol. Neurosci.

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Argyrophilic grain disease (AGD) is a common 4R-tauopathy, causing or contributing to cognitive impairment in the elderly. AGD is characterized neuropathologically by pre-tangles in neurons, dendritic swellings called grains, threads, thorn-shaped astrocytes, and coiled bodies in oligodendrocytes in the limbic system. AGD has a characteristic pattern progressively involving the entorhinal cortex, amygdala, hippocampus, dentate gyrus, presubiculum, subiculum, hypothalamic nuclei, temporal cortex, and neocortex and brainstem, thus suggesting that argyrophilic grain pathology is a natural model of tau propagation. One series of WT mice was unilaterally inoculated in the hippocampus with sarkosyl-insoluble and sarkosyl-soluble fractions from “pure” AGD at the age of 3 or 7/12 months and killed 3 or 7 months later. Abnormal hyper-phosphorylated tau deposits were found in ipsilateral hippocampal neurons, grains (dots) in the hippocampus, and threads, dots and coiled bodies in the fimbria, as well as the ipsilateral and contralateral corpus callosum. The extension of lesions was wider in animals surviving 7 months compared with those surviving 3 months. Astrocytic inclusions were not observed at any time. Tau deposits were mainly composed of 4Rtau, but also 3Rtau. For comparative purposes, another series of WT mice was inoculated with sarkosyl-insoluble fractions from primary age-related tauopathy (PART), a pure neuronal neurofibrillary tangle 3Rtau + 4Rtau tauopathy involving the deep temporal cortex and limbic system. Abnormal hyper-phosphorylated tau deposits were found in neurons in the ipsilateral hippocampus, coiled bodies and threads in the fimbria, and the ipsilateral and contralateral corpus callosum, which extended with time along the anterior-posterior axis and distant regions such as hypothalamic nuclei and nuclei of the septum when comparing mice surviving 7 months with mice surviving 3 months. Astrocytic inclusions were not observed. Tau deposits were mainly composed of 4Rtau and 3Rtau. These results show the capacity for seeding and spreading of AGD tau and PART tau in the brain of WT mouse, and suggest that characteristics of host tau, in addition to those of inoculated tau, are key to identifying commonalities and differences between human tauopathies and corresponding murine models.

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Section: Resultsmentioning

confidence: 73%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Capacity for Seeding and Spreading of Argyrophilic Grain Disease in a Wild-Type Murine Model; Comparisons With Primary Age-Related Tauopathy

Ferrer

Andrés‐Benito

Sala-Jarque

et al. 2020

Front. Mol. Neurosci.

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“…Whilst many studies focus on neuronal damage, white matter hyperintensities (evidence of demyelination) are commonly reported in the early stages of AD and other tauopathies and correlate with tau burden [173]. A recent study describes human familial globular glial tauopathy, linked to MAPT mutations, that result in extensive tau deposits in oligodendrocytes [73]. Affected individuals show severe demyelination, defective myelin synthesis, and concomitant axonal damage [73].…”

Section: Tau Is Important For Normal Myelinationmentioning

confidence: 99%

The physiological roles of tau and Aβ: implications for Alzheimer’s disease pathology and therapeutics

2020

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Tau and amyloid beta (Aβ) are the prime suspects for driving pathology in Alzheimer’s disease (AD) and, as such, have become the focus of therapeutic development. Recent research, however, shows that these proteins have been highly conserved throughout evolution and may have crucial, physiological roles. Such functions may be lost during AD progression or be unintentionally disrupted by tau- or Aβ-targeting therapies. Tau has been revealed to be more than a simple stabiliser of microtubules, reported to play a role in a range of biological processes including myelination, glucose metabolism, axonal transport, microtubule dynamics, iron homeostasis, neurogenesis, motor function, learning and memory, neuronal excitability, and DNA protection. Aβ is similarly multifunctional, and is proposed to regulate learning and memory, angiogenesis, neurogenesis, repair leaks in the blood–brain barrier, promote recovery from injury, and act as an antimicrobial peptide and tumour suppressor. This review will discuss potential physiological roles of tau and Aβ, highlighting how changes to these functions may contribute to pathology, as well as the implications for therapeutic development. We propose that a balanced consideration of both the physiological and pathological roles of tau and Aβ will be essential for the design of safe and effective therapeutics.

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Association Between Globular Glial Tauopathies and Frontotemporal Dementia—Expanding the Spectrum of Gliocentric Disorders

2021

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IMPORTANCE Globular glial tauopathies (GGTs), as defined by a consensus study in 2013, belong to the group of frontotemporal lobar degenerations and expand the spectrum of glial-predominant neurodegenerative diseases. Three neuropathological subtypes of GGT (types I-III) are characterized by phosphorylated tau-immunopositive inclusions that are predominantly in oligodendroglia and/or astroglia in the frontal, temporal, and/or precentral cortices. Type II is largely restricted to the corticospinal system. The low incidence of GGT (<10% of cases of frontotemporal lobar degeneration with tau pathology), together with its unusual combination of neuronal and nonneuronal pathology, has hindered identification and accurate diagnosis. This review collated clinical, demographic, neuropathological, and genetic data from 88 published GGT cases identified on PubMed to examine the association between GGT and frontotemporal dementia and associated disorders.

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Familial globular glial tauopathy linked to MAPT mutations: molecular neuropathology and seeding capacity of a prototypical mixed neuronal and glial tauopathy

Cited by 42 publications

References 136 publications

Capacity for Seeding and Spreading of Argyrophilic Grain Disease in a Wild-Type Murine Model; Comparisons With Primary Age-Related Tauopathy

Capacity for Seeding and Spreading of Argyrophilic Grain Disease in a Wild-Type Murine Model; Comparisons With Primary Age-Related Tauopathy

The physiological roles of tau and Aβ: implications for Alzheimer’s disease pathology and therapeutics

Association Between Globular Glial Tauopathies and Frontotemporal Dementia—Expanding the Spectrum of Gliocentric Disorders

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