Brain functional networks become more connected as amyotrophic lateral sclerosis progresses: a source level magnetoencephalographic study

Sorrentino, Pierpaolo; Rucco, Rosaria; Jacini, Francesca; Trojsi, Francesca; Lardone, Anna; Baselice, Fabio; Femiano, Cinzia; Santangelo, Gabriella; Granata, C.; Vettoliere, A.; Monsurrò, Maria Rosaria; Tedeschi, Gioacchino; Sorrentino, Giuseppe

doi:10.1016/j.nicl.2018.08.001

Cited by 72 publications

(87 citation statements)

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“…In the present work, we set out to study the functional alterations linked to mutations in the SPAST gene. More specifically, accordingly to ours [ 18 ] and other authors’ [ 19 ] previous studies, we hypothesized that the pathological process induces a global reorganization of the brain functional networks. To test our hypothesis, we applied the phase lag index (PLI), which quantifies synchronization between time series, followed by the minimum spanning tree (MST) algorithm, which allows the computation of statistically comparable metrics [ 20 ], to magnetoencephalography (MEG) data obtained from a cohort of SPG4 patients and healthy controls.…”

Section: Introductionmentioning

confidence: 86%

Mutations in the SPAST gene causing hereditary spastic paraplegia are related to global topological alterations in brain functional networks

et al. 2019

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Aim Our aim was to describe the rearrangements of the brain activity related to genetic mutations in the SPAST gene. Methods Ten SPG4 patients and ten controls underwent a 5 min resting state magnetoencephalography recording and neurological examination. A beamformer algorithm reconstructed the activity of 90 brain areas. The phase lag index was used to estimate synchrony between brain areas. The minimum spanning tree was used to estimate topological metrics such as the leaf fraction (a measure of network integration) and the degree divergence (a measure of the resilience of the network against pathological events). The betweenness centrality (a measure to estimate the centrality of the brain areas) was used to estimate the centrality of each brain area. Results Our results showed topological rearrangements in the beta band. Specifically, the degree divergence was lower in patients as compared to controls and this parameter related to clinical disability. No differences appeared in leaf fraction nor in betweenness centrality. Conclusion Mutations in the SPAST gene are related to a reorganization of the brain topology.

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Section: Introductionmentioning

confidence: 86%

Mutations in the SPAST gene causing hereditary spastic paraplegia are related to global topological alterations in brain functional networks

et al. 2019

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“…To date, however, there have been limited attempts to localise abnormal EEG patterns to specific brain regions. Moreover, although source-space studies that use frequency-specific analysis have also been performed in ALS (Fraschini et al, 2018;Sorrentino et al, 2018), the phase-and amplitude-based connectivity profiles of specific brain networks affected by ALS remain to be established. However, because network interactions are often marked by narrow band cortical oscillations (Buzsáki & Draguhn, 2004), it has not been possible to address the spectral aspects of ALS-specific changes in brain networks using broadband signals.…”

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confidence: 99%

“…However, because network interactions are often marked by narrow band cortical oscillations (Buzsáki & Draguhn, 2004), it has not been possible to address the spectral aspects of ALS-specific changes in brain networks using broadband signals. Moreover, although source-space studies that use frequency-specific analysis have also been performed in ALS (Fraschini et al, 2018;Sorrentino et al, 2018), the phase-and amplitude-based connectivity profiles of specific brain networks affected by ALS remain to be established.…”

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confidence: 99%

Patterned functional network disruption in amyotrophic lateral sclerosis

Dukic

McMackin

Buxó

et al. 2019

Human Brain Mapping

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Amyotrophic lateral sclerosis (ALS) is a progressive neurodegenerative disease primarily affecting motor function, with additional evidence of extensive nonmotor involvement. Despite increasing recognition of the disease as a multisystem network disorder characterised by impaired connectivity, the precise neuroelectric characteristics of impaired cortical communication remain to be fully elucidated. Here, we characterise changes in functional connectivity using beamformer source analysis on resting‐state electroencephalography recordings from 74 ALS patients and 47 age‐matched healthy controls. Spatiospectral characteristics of network changes in the ALS patient group were quantified by spectral power, amplitude envelope correlation (co‐modulation) and imaginary coherence (synchrony). We show patterns of decreased spectral power in the occipital and temporal (δ‐ to β‐band), lateral/orbitofrontal (δ‐ to θ‐band) and sensorimotor (β‐band) regions of the brain in patients with ALS. Furthermore, we show increased co‐modulation of neural oscillations in the central and posterior (δ‐, θ‐ and γl‐band) and frontal (δ‐ and γl‐band) regions, as well as decreased synchrony in the temporal and frontal (δ‐ to β‐band) and sensorimotor (β‐band) regions. Factorisation of these complex connectivity patterns reveals a distinct disruption of both motor and nonmotor networks. The observed changes in connectivity correlated with structural MRI changes, functional motor scores and cognitive scores. Characteristic patterned changes of cortical function in ALS signify widespread disease‐associated network disruption, pointing to extensive dysfunction of both motor and cognitive networks. These statistically robust findings, that correlate with clinical scores, provide a strong rationale for further development as biomarkers of network disruption for future clinical trials.

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“…In fact, excessive synchronization reduces the variability of the behaviour of the system, hence narrowing the number of states that are readily accessible (54,73,74). Hypersynchronization and hyperconnected topology have been associated with a variety of neurological diseases (75,76), as well as in preclinical conditions that carry an increased risk of neurodegeneration (77) hence investigations of the functional repertoires in these diseases and conditions could provide answers to this question.…”

Section: Discussionmentioning

confidence: 99%

Extensive functional repertoire underpins complex behaviours: insights from Parkinson’s disease

Sorrentino

Rucco

Baselice

et al. 2019

Preprint

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Rapid reconfigurations of brain activity support efficient neuronal communication and flexible behaviour. Suboptimal brain dynamics impair this adaptability, possibly leading to functional deficiencies. We hypothesize that impaired flexibility in brain activity can lead to motor and cognitive symptoms of Parkinson's disease (PD). To test this hypothesis, we studied the 'functional repertoire' the number of distinct configurations of neural activityusing source-reconstructed magnetoencephalography in PD patients and controls. We found stereotyped brain dynamics and reduced flexibility in PD. The intensity of this reduction was proportional to symptoms severity, and explained by beta-band hyper-synchronization. Moreover, the basal ganglia were prominently involved in the abnormal patterns of brain activity. Our findings support the hypotheses that: symptoms in PD reflect impaired brain flexibility, this impairment preferentially involves the basal ganglia, and beta-band hypersynchronization is associated with reduced brain flexibility. These findings highlight the importance of extensive functional repertoires for behaviour and motor.Parkinson's disease (PD) is a severe and disabling neurodegenerative disorder. It is characterized by reduced amplitude of movements, and slowing of cognitive processes, imposing major individual and social burden (24). The main histopathological finding in PD is a severe nigrostriatal dopamine depletion (25,26). PD has traditionally been regarded predominantly as a motor disease. However, recent clinical and neuroimaging findings have questioned these views (27). For example, the first symptoms to appear are often not motor, and the clinical phenotype clearly goes well beyond the motor impairment, with other domains, such as executive functioning, involved (28,29). Structural Magnetic Resonance Imaging (MRI) has also confirmed that PD is more widespread than previously thought (27). Although functional magnetic resonance (fMRI) studies have identified impairment in the corticostriatal network in PD patients, the observed changes in functional connectivity extend into many other brain systems (30). Similarly, magnetoencephalography (MEG) studies have also reported widespread functional connectivity alterations in PD (31-34) .The brain can be represented as a network, with, at the macro-scale, brain areas as 'nodes' and structural or functional relationships between the brain areas as 'edges ' (35, 36), following which the topology of the network can be characterised using graph theory. A rapidly growing body of research now uses graph theory to characterize large-scale patterns of brain activation in health (37) and disease (38). Graph theory has highlighted the multifaceted nature of large-scale interactions in PD, with studies reporting more-connected networks (39-42), less-connected networks (43-48), and a combination of both (49,50). However, most research in this area has assumed brain activity to be stationary, and did not explore the structure of dynamic fluctuations in activity...

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Brain functional networks become more connected as amyotrophic lateral sclerosis progresses: a source level magnetoencephalographic study

Cited by 72 publications

References 56 publications

Mutations in the SPAST gene causing hereditary spastic paraplegia are related to global topological alterations in brain functional networks

Mutations in the SPAST gene causing hereditary spastic paraplegia are related to global topological alterations in brain functional networks

Patterned functional network disruption in amyotrophic lateral sclerosis

Extensive functional repertoire underpins complex behaviours: insights from Parkinson’s disease

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