Functional network disruption in the degenerative dementias

Pievani, Michela; Haan, Willem de; Wu, Tao; Seeley, William W.; Frisoni, Giovanni B.

doi:10.1016/s1474-4422(11)70158-2

Cited by 419 publications

(388 citation statements)

References 145 publications

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“…Albeit being in line with our findings, all these studies were based on a localisation-based approach. This type of approach is not as suitable as a connectivity-based framework to characterise cellular and synaptic disruption, and its association to the underlying cognitive functions [66]. Moreover, it is worth noting that evidence emerging from connectivity analyses should not be taken for granted as the natural consequence of the aforementioned localisation-based differences reported in the literature.…”

Section: Discussionmentioning

confidence: 99%

ApoE ε4 Allele Related Alterations in Hippocampal Connectivity in Early Alzheimer’s Disease Support Memory Performance

Marco

Vallelunga

Meneghello

et al. 2017

CAR

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Section: Discussionmentioning

confidence: 99%

ApoE ε4 Allele Related Alterations in Hippocampal Connectivity in Early Alzheimer’s Disease Support Memory Performance

Marco

Vallelunga

Meneghello

et al. 2017

CAR

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“…The core function of the network continues to be defined, but it is active during stimulus-independent thought in the resting wakeful (and dreaming) brain [7,59,60] . Functional alterations in the DMN have been consistently identified in neuroimaging studies [6][7][8] of AD. Brainstem systems projecting to the DMN together with the DMN proper are likely to be integral to the development of AD; brainstem nuclei (in particular, the locus coeruleus) and ascending neurotransmitter systems comprise the 'isodendritic core' or reticular formation [66] and are among the earliest targets of AD pathology [1] .…”

Section: A 'Hypnic Hypothesis' Of Admentioning

confidence: 99%

“…The very earliest disease targets in AD remain somewhat contentious but are likely to include entorhinal cortex and brainstem sites, including locus coeruleus, dorsal raphe nuclei or nucleus tractus solitarius [2,8,84] . Consistent with the early disruption of circadian and sleep physiology observed clinically, neuropathological evidence in AD clearly implicates ascending brainstem pathways that govern the sleep-wake cycle at or near the outset of the disease, including cholinergic, dopaminergic, melatoninergic and neurosteroid systems [2,4,27,42,56,63] .…”

Section: Evidence For the Hypothesis: The Neuroanatomy Of Admentioning

confidence: 99%

“…However, converging evidence drawn from molecular biology, sleep neuroscience [21][22][23][24][25][26][27][28][29][30][31][32][33][34] and clinical neurology [35][36][37][38][39][40][41][42] suggests that sleep may interact in diverse and important ways with the pathophysiology of AD. Ramifications of long-term disruption in the sleep-wake cycle could include synaptic overactivity and excitotoxicity [10,21,[43][44][45] , impaired synaptic pruning [46] , failure of synaptic scaling and homeostatic responses [19,20,27,[47][48][49][50][51] , transmission of pathogenic proteins (β-amyloid and tau) [9,15,16] , and disruption of neural circuitry in the vulnerable DMN [6,8,12,21,52,53] . Such alterations might in turn underpin or contribute to the cognitive syndrome that characterises AD.…”

Section: Introductionmentioning

confidence: 99%

“…Molecular biological, biochemical and neuroimaging studies have yielded a substantial body of data on the causes and evolution of AD [1][2][3][4][5] , whilst the concept of a vulnerable distributed brain network provides a framework for explaining how molecular events might scale up to a clinical phenotype [6][7][8][9] . It is increasingly clear that AD has a protracted prodromal phase prior to clinical onset during which potentially pathogenic factors could operate and might have cumulative effects [5] .…”

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confidence: 99%

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P4–021: A hypnic hypothesis of Alzheimer's disease

Clark

Warren

2013

Alzheimer's & Dementia

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condition. Molecular biological, biochemical and neuroimaging studies have yielded a substantial body of data on the causes and evolution of AD [1][2][3][4][5] , whilst the concept of a vulnerable distributed brain network provides a framework for explaining how molecular events might scale up to a clinical phenotype [6][7][8][9] . It is increasingly clear that AD has a protracted prodromal phase prior to clinical onset during which potentially pathogenic factors could operate and might have cumulative effects [5] .On a biochemical level, synaptic alterations are hypothesised to play a key role in the pathogenesis of many neurodegenerative diseases, including AD [9][10][11] . Such alterations may promote the transfer of pathogenic molecular species (in particular, β-amyloid oligomers) leading to the diffusive spread of misfolded proteins (in particular, hyperphosphorylated tau) throughout a vulnerable, distributed brain network, the so-called 'default mode network' (DMN) that appears to be integral to the operation of the normal resting brain [12][13][14][15][16] . Most accounts of synaptic dysfunction in AD emphasise molecular and biochemical events impacting on synaptic physiology via a loss of structural integrity [11,17] . However, an alternative (and by no means mutually exclusive) possibility is the promotion of synaptic damage by altered patterns of synaptic activity and excitotoxicity [18] . A fundamental example of a pervasive, phasic alteration in synaptic activity is the circadian sleep-wake cycle, which is associated with profound changes in many aspects of cellular and synaptic function [19,20] . Key WordsSleep · Alzheimer's disease · Neurodegeneration · Default mode network Abstract Background: Understanding the pathophysiology of Alzheimer's disease (AD) is of fundamental importance for improved diagnosis, monitoring and ultimately, treatment. Objective: A role for the sleep-wake cycle in the pathogenesis of AD has been proposed, but remains to be worked out in detail. Methods: Here we draw together several lines of previous work to outline a 'hypnic hypothesis' of AD. Results: We propose that altered function of brainstem neuro transmitter pathways associated with sleep, promotes regio nally specific disintegration of a cortico-subcortical 'default mode' brain network that is selectively vulnerable in AD. Conclusion: The formation of a dynamic toxic state within this vulnerable network linked to sleep-wake disruption, would in turn lead to failure of synaptic repair, increased transmission of pathogenic misfolded proteins and a self-amplifying neurodegenerative process. We consider the evidence for this hypnic hypothesis and the implications that follow on from it.

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