Hyperactivity Induced by Soluble Amyloid-β Oligomers in the Early Stages of Alzheimer's Disease

Hector, Audrey; Brouillette, Jonathan

doi:10.3389/fnmol.2020.600084

Cited by 55 publications

(46 citation statements)

References 162 publications

(247 reference statements)

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“…However, the causes and consequences of AD-associated network dysfunctions remain to be fully elucidated. Evidence obtained in AD-related mouse models suggests that the human amyloid precursor protein (hAPP) or some of its metabolites and the microtubule-associated protein tau (MAPT) causally contribute to these dysfunctions ( Palop and Mucke, 2016 ; Harris et al., 2020 ; Johnson et al., 2020 ; Chang et al., 2021 ; Hector and Brouillette, 2021 ). Indications that hypersynchronous network activity may promote disease progression include the observations that cognitive decline is faster in AD patients with detectable epileptiform activity than those without ( Vossel et al., 2016 ), that treatment with the antiepileptic drug levetiracetam (LEV) reverses functional magnetic resonance imaging abnormalities and reduces some cognitive deficits in people with amnestic mild cognitive impairment ( Bakker et al., 2012 , 2015 ), and that treatment with LEV, or its analog brivaracetam, suppresses epileptiform activity and reverses both synaptic deficits and cognitive impairments in different lines of hAPP transgenic mice ( Sanchez et al., 2012 ; Shi et al., 2013 ; Nygaard et al., 2015 ; Fu et al., 2019 ).…”

Section: Introductionmentioning

confidence: 99%

Interdependence of neural network dysfunction and microglial alterations in Alzheimer’s disease-related models

et al. 2021

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Summary Nonconvulsive epileptiform activity and microglial alterations have been detected in people with Alzheimer’s disease (AD) and related mouse models. However, the relationship between these abnormalities remains to be elucidated. We suppressed epileptiform activity by treatment with the antiepileptic drug levetiracetam or by genetic ablation of tau and found that these interventions reversed or prevented aberrant microglial gene expression in brain tissues of aged human amyloid precursor protein transgenic mice, which simulate several key aspects of AD. The most robustly modulated genes included multiple factors previously implicated in AD pathogenesis, including TREM2, the hypofunction of which increases disease risk. Genetic reduction of TREM2 exacerbated epileptiform activity after mice were injected with kainate. We conclude that AD-related epileptiform activity markedly changes the molecular profile of microglia, inducing both maladaptive and adaptive alterations in their activities. Increased expression of TREM2 seems to support microglial activities that counteract this type of network dysfunction.

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Section: Introductionmentioning

confidence: 99%

Interdependence of neural network dysfunction and microglial alterations in Alzheimer’s disease-related models

et al. 2021

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“…Further, imbalanced activity represents a potential trigger of neurodegeneration (Busche and Konnerth, 2016;Palop and Mucke, 2016;Palop et al, 2007;Sosulina et al, 2021). Neuronal hyperactivity has been detected in patients with mild cognitive impairment (MCI), a prodromal stage of AD, and in carriers of the APOE4 allele, the most important genetic risk factor for late-onset sporadic AD, as well as in many transgenic AD mice (Hector and Brouillette, 2020). Furthermore, activity imbalance at the circuit level is reported in Alzheimer's disease and in AD model systems and is considered a potential trigger of neurodegeneration (Busche and Konnerth, 2016;Palop and Mucke, 2016;Palop et al, 2007;Sosulina et al, 2021).…”

Section: Discussionmentioning

confidence: 99%

“…Recent evidence indicates that synaptic failure in AD is at least partly induced by neuronal hyperactivity in the early stages of the disease, and this mechanism could also be involved in developing a late-onset autosomal dominant inherited form of PD (Hector and Brouillette, 2020;Lucumi Moreno et al, 2021;Nuriel et al, 2017). We thus tested whether activity of PRCs is linked to the axonal degeneration described in our model.…”

Section: Neurotransmission Is Involved In Axonal Degenerationmentioning

confidence: 92%

A quantitative model of sporadic axonal degeneration in theDrosophilavisual system

Richard

Doubková

Nitta

et al. 2021

Preprint

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In human neurodegenerative diseases, neurons undergo axonal degeneration months to years before they die. Here, we developed a system modelling early degenerative events in Drosophila adult photoreceptor cells. Thanks to the stereotypy of their axonal projections, this system delivers quantitative data on sporadic and progressive axonal degeneration of photoreceptor cells. Using this method, we show that exposure of adult flies to a constant light stimulation for several days overcomes the intrinsic resilience of R7 photoreceptors and leads to progressive axonal degeneration. This was not associated with apoptosis. We furthermore provide evidence that loss of synaptic integrity between R7 and a postsynaptic partner preceded axonal degeneration, thus recapitulating features of human neurodegenerative diseases. Finally, our experiments uncovered that neurotransmission to postsynaptic partners of R7 and their response are required to initiate degeneration, suggesting that postsynaptic cells signal back to the photoreceptor to maintain axonal structure. This model can be used to dissect cellular circuit mechanisms involved in the early events of axonal degeneration, allowing for a better understanding of how neurons cope with stress and lose their resilience capacities.

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“…One interpretation for this discrepancy is that the reduced level of sAß observed in APP/PS1xKO may be sufficient to restore synaptic efficiency independently of synaptic structural changes, e.g. by directly regulating neuronal excitability alterations associated with Aß peptide deposit 39 .…”

Section: P2rx4 Deletion Reverses Cognitive Performance Decline In App...mentioning

confidence: 99%

Microglial P2X4 receptors promote ApoE degradation and cognitive deficits in Alzheimer disease

Hua

Paco

Linck

et al. 2022

Preprint

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Numerous evidence support that microglia contributes to the progression of Alzheimer’s disease. P2X4 receptors are ATP-gated channels, which are de novo expressed in a subset of reactive microglia associated to various pathological contexts, contributing to microglial functions. Here, we investigated the role of P2X4 in the context of Alzheimer disease (AD). In both human AD brain and APPswe/PSEN1dE9 mice, P2X4 is almost exclusively expressed in plaque associated microglia. Genetic deletion of P2rx4 results in the reversal of cognitive declines and in a lower amount of soluble Aß1 −42 in 12 months old APP/PS1 mice, while no obvious alteration of plaque associated microglia characteristics is observed. Using proteomic, we identified ApoE as a specific P2X4 interacting protein. We found that P2X4 regulates lysosomal cathepsin B activity promoting ApoE degradation; P2rx4 deletion results in higher amount of intracellular and secreted ApoE in both BMDM and microglia from APP/PS1 brain. Our results support that microglial P2X4 promotes lysosomal ApoE degradation, indirectly altering Aß peptide clearance, which in turn might promote synaptic dysfunctions and cognitive deficits. Our findings also uncover a specific interplay between purinergic signaling, microglial ApoE, sAß species and cognitive deficits associated with AD.

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Hyperactivity Induced by Soluble Amyloid-β Oligomers in the Early Stages of Alzheimer's Disease

Cited by 55 publications

References 162 publications

Interdependence of neural network dysfunction and microglial alterations in Alzheimer’s disease-related models

Interdependence of neural network dysfunction and microglial alterations in Alzheimer’s disease-related models

A quantitative model of sporadic axonal degeneration in theDrosophilavisual system

Microglial P2X4 receptors promote ApoE degradation and cognitive deficits in Alzheimer disease

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