Microglial internalization and degradation of pathological tau is enhanced by an anti-tau monoclonal antibody

Luo, Wenjie; Liu, Wen‐Cheng; Hu, Xiaoyan; Hanna, Mary; Caravaca, April S.; Paul, Steven M.

doi:10.1038/srep11161

Cited by 176 publications

(187 citation statements)

References 47 publications

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“…Recent studies demonstrate that microglia are involved in the uptake of tau protein. In primary cultures of microglia (Luo et al, 2015; Bolós et al, 2016) and P301S mice (Luo et al, 2015), microglia internalize extracellular soluble and insoluble tau in vitro and in vivo , respectively. Thus, microglia seem to play a protective mechanism in the clearance of tau.…”

Section: Discussionmentioning

confidence: 99%

Evidence of Tau Hyperphosphorylation and Dystrophic Microglia in the Common Marmoset

Rodríguez-Callejas

Fuchs

Pérez-Cruz

2016

Front. Aging Neurosci.

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Common marmosets (Callithrix jacchus) have recently gained popularity in biomedical research as models of aging research. Basically, they confer advantages from other non-human primates due to their shorter lifespan with onset of appearance of aging at 8 years. Old marmosets present some markers linked to neurodegeneration in the brain such as amyloid beta (Aβ)1-42 and Aβ1-40. However, there are no studies exploring other cellular markers associated with neurodegenerative diseases in this non-human primate. Using immunohistochemistry, we analyzed brains of male adolescent, adult, old, and aged marmosets. We observed accumulation of Aβ1-40 and Aβ1-42 in the cortex of aged subjects. Tau hyperphosphorylation was already detected in the brain of adolescent animals and increased with aging in a more fibrillary form. Microglia activation was also observed in the aging process, while a dystrophic phenotype accumulates in aged subjects. Interestingly, dystrophic microglia contained hyperphosphorylated tau, but active microglia did not. These results support previous findings regarding microglia dysfunctionality in aging and neurodegenerative diseases as Alzheimer’s disease. Further studies should explore the functional consequences of these findings to position this non-human primate as animal model of aging and neurodegeneration.

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Section: Discussionmentioning

confidence: 99%

Evidence of Tau Hyperphosphorylation and Dystrophic Microglia in the Common Marmoset

Rodríguez-Callejas

Fuchs

Pérez-Cruz

2016

Front. Aging Neurosci.

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“…Therefore, it is likely that most of the phospho-tau in our S1 fractions were originally located intraneuronally. However, it is also known that microglia cells could phagocytose apoptotic tau-bearing neurons [29, 35]. Thus, we also tested whether intracellular phospho-tau could be toxic for microglia after phagocytosis.…”

Section: Resultsmentioning

confidence: 99%

“…Sarkosyl-insoluble tau was isolated as described [29]. Human hippocampi were homogenized in “homogenization buffer” (10 mM Tris, 0.8 M NaCl, 1 mM EGTA, 10 % sucrose, pH 7.4, plus protease, and phosphatase inhibitors).…”

Section: Methodsmentioning

confidence: 99%

Soluble phospho-tau from Alzheimer’s disease hippocampus drives microglial degeneration

et al. 2016

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The role of microglial cells in the development and progression of Alzheimer’s disease (AD) has not been elucidated. Here, we demonstrated the existence of a weak microglial response in human AD hippocampus which is in contrast to the massive microglial activation observed in APP-based models. Most importantly, microglial cells displayed a prominent degenerative profile (dentate gyrus > CA3 > CA1 > parahippocampal gyrus), including fragmented and dystrophic processes with spheroids, a reduced numerical density, and a significant decrease in the area of surveillance (“microglial domain”). Consequently, there was a substantial decline in the area covered by microglia which may compromise immune protection and, therefore, neuronal survival. In vitro experiments demonstrated that soluble fractions (extracellular/cytosolic) from AD hippocampi were toxic for microglial cells. This toxicity was abolished by AT8 and/or AT100 immunodepletion, validating that soluble phospho-tau was the toxic agent. These results were reproduced using soluble fractions from phospho-tau-positive Thy-tau22 hippocampi. Cultured microglial cells were not viable following phagocytosis of SH-SY5Y cells expressing soluble intracellular phospho-tau. Because the phagocytic capacity of microglial cells is highly induced by apoptotic signals in the affected neurons, we postulate that accumulation of intraneuronal soluble phospho-tau might trigger microglial degeneration in the AD hippocampus. This microglial vulnerability in AD pathology provides new insights into the immunological mechanisms underlying the disease progression and highlights the need to improve or develop new animal models, as the current models do not mimic the microglial pathology observed in the hippocampus of AD patients.Electronic supplementary materialThe online version of this article (doi:10.1007/s00401-016-1630-5) contains supplementary material, which is available to authorized users.

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“…Targeting numerous other epitopes has been shown to be effective in several studies. These include non-phosphorylated- [27,30,32,41,42,46–48,69,70], phosphorylated- [20,24,25,27,29,35,39,43,49], conformational-/oligomeric [20,31,33,34,40,44,45], and a truncated epitope [66,71]. Since these studies have various designs, they cannot be easily compared to identify the best epitopes to target.…”

Section: How Does It Work?mentioning

confidence: 99%

Tau Immunotherapies for Alzheimer’s Disease and Related Tauopathies: Progress and Potential Pitfalls1

Sigurdsson

2018

JAD

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Tau immunotherapies have now advanced from proof-of-concept studies to Phase 2 clinical trials. This review briefly outlines developments in the field and discusses how these therapies may work, which involves multiple variables that are connected in complex ways. These various factors are likely to define therapeutic success in humans and have not been thoroughly investigated, at least based on published reports.

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Microglial internalization and degradation of pathological tau is enhanced by an anti-tau monoclonal antibody

Cited by 176 publications

References 47 publications

Evidence of Tau Hyperphosphorylation and Dystrophic Microglia in the Common Marmoset

Evidence of Tau Hyperphosphorylation and Dystrophic Microglia in the Common Marmoset

Soluble phospho-tau from Alzheimer’s disease hippocampus drives microglial degeneration

Tau Immunotherapies for Alzheimer’s Disease and Related Tauopathies: Progress and Potential Pitfalls1

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