by Keyword: onset

Arnau, Marc, Sans, Jordi, Turon, Pau, Alemán, Carlos, (2022). Decarbonization of Polluted Air by SolarDriven CO2 Conversion into Ethanol Using Polarized Animal Solid Waste as Catalyst Advanced Sustainable Systems , 2200283

Espinoso A, Andrzejak RG, (2022). Phase irregularity: A conceptually simple and efficient approach to characterize electroencephalographic recordings from epilepsy patients Physical Review e 105, 34212

The severe neurological disorder epilepsy affects almost 1% of the world population. For patients who suffer from pharmacoresistant focal-onset epilepsy, electroencephalographic (EEG) recordings are essential for the localization of the brain area where seizures start. Apart from the visual inspection of the recordings, quantitative EEG signal analysis techniques proved to be useful for this purpose. Among other features, regularity versus irregularity and phase coherence versus phase independence allowed characterizing brain dynamics from the measured EEG signals. Can phase irregularities also characterize brain dynamics? To address this question, we use the univariate coefficient of phase velocity variation, defined as the ratio of phase velocity standard deviation and the mean phase velocity. Beyond that, as a bivariate measure we use the classical mean phase coherence to quantify the degree of phase locking. All phase-based measures are combined with surrogates to test null hypotheses about the dynamics underlying the signals. In the first part of our analysis, we use the Rössler model system to study our approach under controlled conditions. In the second part, we use the Bern-Barcelona EEG database which consists of focal and nonfocal signals extracted from seizure-free recordings. Focal signals are recorded from brain areas where the first seizure EEG signal changes can be detected, and nonfocal signals are recorded from areas that are not involved in the seizure at its onset. Our results show that focal signals have less phase variability and more phase coherence than nonfocal signals. Once combined with surrogates, the mean phase velocity proved to have the highest discriminative power between focal and nonfocal signals. In conclusion, conceptually simple and easy to compute phase-based measures can help to detect features induced by epilepsy from EEG signals. This holds not only for the classical mean phase coherence but even more so for univariate measures of phase irregularity. © 2022 American Physical Society.

JTD Keywords: brain, entropy, epileptogenic networks, functional connectivity, hilbert transform, seizure onset, surrogate data, synchronization, time-series, Biomedical signal processing, Brain areas, Brain dynamics, Dynamics, Electroencephalographic signals, Electroencephalography, Electrophysiology, Intracranial eeg signals, Localisation, Neurological disorders, Neurology, Phase based, Phase coherence, Signal detection, Simple++, Univariate, Velocity, World population

Seuma, M, Faure, AJ, Badia, M, Lehner, B, Bolognesi, B, (2021). The genetic landscape for amyloid beta fibril nucleation accurately discriminates familial Alzheimer's disease mutations Elife 10, e63364

Plaques of the amyloid beta (A beta) peptide are a pathological hallmark of Alzheimer's disease (AD), the most common form of dementia. Mutations in A beta also cause familial forms of AD (fAD). Here, we use deep mutational scanning to quantify the effects of >14,000 mutations on the aggregation of A beta. The resulting genetic landscape reveals mechanistic insights into fibril nucleation, including the importance of charge and gatekeeper residues in the disordered region outside of the amyloid core in preventing nucleation. Strikingly, unlike computational predictors and previous measurements, the empirical nucleation scores accurately identify all known dominant fAD mutations in A beta, genetically validating that the mechanism of nucleation in a cell-based assay is likely to be very similar to the mechanism that causes the human disease. These results provide the first comprehensive atlas of how mutations alter the formation of any amyloid fibril and a resource for the interpretation of genetic variation in A beta.

JTD Keywords: aggregation, kinetics, oligomers, onset, rates, state, Aggregation, Alzheimer's, Amyloid, Computational biology, Deep mutagenesis, Genetics, Genomics, Kinetics, Nucleation, Oligomers, Onset, Precursor protein, Rates, S. cerevisiae, State, Systems biology

Estrada, L., Santamaria, J., Isetta, V., Iranzo, A., Navajas, D., Farre, R., (2010). Validation of an EEG-based algorithm for automatic detection of sleep onset in the multiple sleep latency test Proceedings of the World Congress on Engineering 2010 World Congress on Engineering 2010 , IAENG (International Association of Engineers) (London, UK) 1, 1-3

The Multiple Sleep Latency Test (MSLT) is a standard test to objectively evaluate patients with excessive daytime sleepiness. Sleep onset latencies are determined by visual analysis, which is costly and time-consuming. The aim of this study was to implement and test a single automatic algorithm to detect the sleep onset in the MSLT on the basis of electroencephalographic (EEG) signals. The designed algorithm computed the relative EEG spectral powers in the occipital area and detected the sleep onset corresponding to the intersection point between the lower and alpha frequencies. The algorithm performance was evaluated by comparing the sleep latencies computed automatically by the algorithm and by a sleep specialist using MSLT recordings from a total of 19 patients (95 naps). The mean difference in sleep latency between the two methods was 0.025 min and the limits of agreement were ± 2.46 min (Bland-Altman analysis). Moreover, the intra-class correlation coefficient showed a considerable inter-rater reliability (0.90). The algorithm accurately detected the sleep onset in the MSLT. The devised algorithm can be a useful tool to support and speed up the sleep specialist’s work in routine clinical MSLT assessment.

JTD Keywords: Automatic Algorithm, Drowsiness, Electroencephalography, Multiple Sleep Latency Test, Polysomnography, Sleep onset