Amyloid β-protein oligomers promote the uptake of tau fibril seeds potentiating intracellular tau aggregation

Shin, Woo Shik; Di, Jing; Cao, Qing; Li, Binsen; Seidler, Paul M.; Murray, Kevin; Bitan, Gal; Jiang, Lin

doi:10.1186/s13195-019-0541-9

Cited by 73 publications

(63 citation statements)

References 54 publications

(55 reference statements)

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“…Several research groups studied tau-Aβ cross-seeding [219,220] and found that aggregated Aβ promoted the formation of tau aggregates. It was demonstrated that AβO enhances tau seeding in mouse neurons [221,222] and facilitates intracellular tau aggregation by promoting the uptake of tau seeds. However, transduced Aβ fibrils slightly reduce tau seeding.…”

Section: Aβ-tau Crosstalkmentioning

confidence: 99%

Oligomerization and Conformational Change Turn Monomeric β-Amyloid and Tau Proteins Toxic: Their Role in Alzheimer’s Pathogenesis

2020

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The structural polymorphism and the physiological and pathophysiological roles of two important proteins, β-amyloid (Aβ) and tau, that play a key role in Alzheimer’s disease (AD) are reviewed. Recent results demonstrate that monomeric Aβ has important physiological functions. Toxic oligomeric Aβ assemblies (AβOs) may play a decisive role in AD pathogenesis. The polymorph fibrillar Aβ (fAβ) form has a very ordered cross-β structure and is assumed to be non-toxic. Tau monomers also have several important physiological actions; however, their oligomerization leads to toxic oligomers (TauOs). Further polymerization results in probably non-toxic fibrillar structures, among others neurofibrillary tangles (NFTs). Their structure was determined by cryo-electron microscopy at atomic level. Both AβOs and TauOs may initiate neurodegenerative processes, and their interactions and crosstalk determine the pathophysiological changes in AD. TauOs (perhaps also AβO) have prionoid character, and they may be responsible for cell-to-cell spreading of the disease. Both extra- and intracellular AβOs and TauOs (and not the previously hypothesized amyloid plaques and NFTs) may represent the novel targets of AD drug research.

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Section: Aβ-tau Crosstalkmentioning

confidence: 99%

Oligomerization and Conformational Change Turn Monomeric β-Amyloid and Tau Proteins Toxic: Their Role in Alzheimer’s Pathogenesis

2020

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“…These results indicate the contribution of mitochondrial ROS to tau oligomer formation and accumulation. Given that Aβ oligomers can seed and promote tau oligomerization and uptake of tau brils [25][26][27] , we propose that Aβ-mediated sustained mitochondrial stress and excessive ROS production could be a potential mechanism underlying Aβ-mediated/enhanced tau oligomers accumulation. Our studies suggest the role of the Aβ/ROS/mitochondria axis in aberrant tau oligomer accumulation, which links to cognitive dysfunction.…”

Section: Discussionmentioning

confidence: 96%

Mitochondrial perturbation drives tau oligomers pathology in Alzheimer’s disease

Chen

et al. 2020

Preprint

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Tau oligomers, prior to neurofibrillary tangle formation, are toxic species responsible for tau pathology, mitochondrial and synaptic damage, and memory impairment. The underlying mechanisms of abnormal tau accumulation and strategies to eliminate them remain largely unknown. The present study addresses whether mitochondrial reactive oxygen species (ROS) are major contributing factors for tau oligomer formation and, if so, whether eliminating mitochondrial ROS reduces accumulation of tau oligomers and improves mitochondrial and cognitive function in Alzheimer’s disease (AD). First, we determined whether increased oxidative stress correlates with aggregation of tau oligomers in human AD-affected brains, Aβ/tau overexpressed mouse models, human trans-mitochondrial “cybrid” (cytoplasmic hybrid) neuronal cells containing mild cognitive impairment (MCI) and AD-derived mitochondria, and Aβ/tau expressing neuronal cells. In P301S tau and AD mice, upregulation of tau oligomers correlates with ROS accumulation. Elevated tau oligomer levels are also correlated with elevated ROS levels in the AD patient hippocampus. Importantly, human cybrid cells, whose mitochondria are derived from platelets of patients with sporadic AD or MCI, displayed aggregated tau oligomers, which also correlated with upregulated ROS levels. Application of mito-Tempo, a mitochondria-targeted antioxidant, to inhibit the generation of mitochondrial and intracellular ROS in tau and AD neurons, as well as in MCI and AD cybrids ex vivo, leads to a striking decrease in tau oligomers. Finally, in AD mice, mito-Tempo inhibited tau oligomer accumulation and improved behavioral deficiency. Our work adds to the growing body of evidence that oxidative stress contributes to tau oligomer formation and that inhibition of oxidative stress ameliorates tauopathy in AD.

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“…Indeed, AβO have been shown to enhance, whereas Aβ fibrils reduce, the aggregation of tau (Shin et al 2019b). Furthermore, AβO promote the uptake of tau fibril seeds potentiating intracellular aggregation (Shin et al 2019a) and mediate neurite degeneration (Jin et al 2011). Mechanistic insights into this AβO-tau interaction arise from intriguing new data that demonstrate the involvement of NA, and α2 A adrenergic receptors (α2 A ARs) in mediating tau hyperphosphorylation and Alzheimer’s-related pathology in human and animal samples (Zhang et al 2020).…”

Section: Discussionmentioning

confidence: 99%

Identification of amyloid beta oligomers in locus coeruleus (LC) neurons of Alzheimer’s patients and their impact on LC oxidative stress, inhibitory neurotransmitter receptors and neuronal excitability

Kelly

Seifi

et al. 2020

Preprint

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Amyloid β oligomers (AβO) are potent modulators of two key Alzheimer's pathological processes, namely synaptic dysfunction and tau tangle formation in various brain regions. Remarkably, the impact of AβO in one of the earliest brain regions to exhibit Alzheimer's pathology, the locus coeruleus (LC), remains to be determined. Of particular importance is the effect of AβO on the excitability of individual LC neurons. This parameter determines brain-wide noradrenaline (NA) release, and thus NA-mediated brain functions, including cognition, emotion and immune function, which are all severely compromised in Alzheimer's. Using a mouse model of increased Aβ production (APP-PSEN1), together with correlative histopathological analyses in post mortem Alzheimer's patient samples, we determined the impact of Aβ pathology on various correlates of LC neuronal integrity. AβO immunoreactivity in the LC of APP-PSEN1 mice was replicated in patient samples, presenting as individual clusters located both intraneuronally, in mitochondrial compartments, as well as extracellularly in association with inhibitory synapses. No specific signal was detected in either patient control or wild type mouse samples. Accompanying this AβO expression profile was LC neuronal hyperexcitability and indicators of oxidative stress in APP-PSEN1 mice. LC hyperexcitability arose from a diminished inhibitory effect of GABA, due to impaired expression and function of the GABA-A receptor (GABA A R) α 3 subunit. Importantly, this altered LCα 3-GABA A R expression profile overlapped with AβO expression in both APP-PSEN1 mice and Alzheimer's patient samples. Finally, strychninesensitive glycine receptors (GlyRs) remained resilient to AβO-induced changes and their activation reversed LC hyperexcitability. Alongside this first demonstration of 4 AβO expression in the LC of Alzheimer's patients, the study is also first to reveal a direct association between AβO and LC neuronal excitability. GlyR-α3-GABA A R modulation of AβO-dependent LC hyperexcitability could delay the onset of cognitive and psychiatric symptoms arising from LC-NA deficits, thereby significantly diminishing the disease burden for Alzheimer's patients. particular relevance to the LC, and its early presentation of Alzheimer's pathology, is the emerging synergistic role of AβO in tau tangle formation (Pickett et al. 2019; Shin et al. 2019b). Intriguingly, while notable LC neuronal loss, attributed to tauopathy, is a core feature in Alzheimer's (Chan-Palay and Asan 1989), there appears to be discordance between the onset of such pathology, and LC neurodegeneration (Weinshenker 2018). Given such considerable evidence, it is reasonable to speculate that in the LC, initial, pre-symptomatic insults in the form of tau tangle and AβO interactions, cooperate to set in motion a range of pathological changes such as synaptic dysfunction, oxidative stress (De Felice et al. 2007) and altered LC excitability (Sanchez-Padilla et al. 2014). Such changes are likely to prove crucial in terms of the long-term viabili...

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Amyloid β-protein oligomers promote the uptake of tau fibril seeds potentiating intracellular tau aggregation

Cited by 73 publications

References 54 publications

Oligomerization and Conformational Change Turn Monomeric β-Amyloid and Tau Proteins Toxic: Their Role in Alzheimer’s Pathogenesis

Oligomerization and Conformational Change Turn Monomeric β-Amyloid and Tau Proteins Toxic: Their Role in Alzheimer’s Pathogenesis

Mitochondrial perturbation drives tau oligomers pathology in Alzheimer’s disease

Identification of amyloid beta oligomers in locus coeruleus (LC) neurons of Alzheimer’s patients and their impact on LC oxidative stress, inhibitory neurotransmitter receptors and neuronal excitability

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