Objectives: The time series of single trial cortical evoked potentials typically have a random appearance, and their trial-to-trial variability is commonly explained by a model in which random ongoing background noise activity is linearly combined with a stereotyped evoked response. In this paper, we demonstrate that more realistic models, incorporating amplitude and latency variability of the evoked response itself, can explain statistical properties of cortical potentials that have often been attributed to stimulus-related changes in functional connectivity or other intrinsic neural parameters.
Methods: Implications of trial-to-trial evoked potential variability for variance, power spectrum, and interdependence measures like cross-correlation and spectral coherence, are first derived analytically. These implications are then illustrated using model simulations and verified experimentally by the analysis of intracortical local field potentials recorded from monkeys performing a visual pattern discrimination task. To further investigate the effects of trial-to-trial variability on the aforementioned statistical measures, a Bayesian inference technique is used to separate single-trial evoked responses from the ongoing background activity.
Results: We show that, when the average event-related potential (AERP) is subtracted from single-trial local field potential time series, a stimulus phase-locked component remains in the residual time series, in stark contrast to the assumption of the common model that no such phase-locked component should exist. Two main consequences of this observation are demonstrated for statistical measures that are computed on the residual time series. First, even though the AERP has been subtracted, the power spectral density, computed as a function of time with a short sliding window, can nonetheless show signs of modulation by the AERP waveform. Second, if the residual time series of two channels co-vary, then their cross-correlation and spectral coherence time functions can also be modulated according to the shape of the AERP waveform. Bayesian estimation of single-trial evoked responses provides further proof that these time-dependent statistical changes are due to remnants of the evoked phase-locked component in the residual time series.
Conclusions: Because trial-to-trial variability of the evoked response is commonly ignored as a contributing factor in evoked potential studies, stimulus-related modulations of power spectral density, cross-correlation, and spectral coherence measures is often attributed to dynamic changes of the connectivity within and among neural populations. This work demonstrates that trial-to-trial variability of the evoked response must be considered as a possible explanation of such modulation.
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http://dx.doi.org/10.1016/s1388-2457(01)00739-8 | DOI Listing |
Neural Comput
January 2025
Institute of Science and Technology for Brain-Inspired Intelligence, Fudan University, Shanghai, 200437, China
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Department of Neuroscience, Johns Hopkins University School of Medicine, Baltimore, USA.
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December 2024
Department of Physics, Hong Kong Baptist University, Kowloon Tong, Hong Kong SAR, China.
Unlabelled: Data-driven strategies have been widely used to distinguish experimental effects on single-trial EEG signals. However, how latency variability, such as within-condition jitter or latency shifts between conditions, affects the performance of EEG classifiers has not been well investigated. Without explicitly considering and disentangling such attributes of single trials, neural network-based classifiers have limitations in measuring their contributions.
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Program in Physical Therapy, Washington University School of Medicine, CB 8502, 4444 Forest Park Ave., Suite 1101, St. Louis, MO 63108-2212, United States; Program in Occupational Therapy, Washington University School of Medicine, MSC 8505-66-1, 4444 Forest Park Avenue, St. Louis, MO 63108-2212, United States; Department of Neurology, Washington University School of Medicine, MSC 8111-29-9000, 660 S. Euclid Ave., St. Louis, MO 63110, United States. Electronic address:
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Department of Biomedical Engineering, 9500 Euclid Avenue, ND-20, Cleveland, OH, 44195, USA.
The controlled release of grasping forces underlies skilled dexterous interactions with objects. While declines in force generation and maintenance are well documented in people with Parkinson's disease (PwPD), limited data exist related to how PD impacts the motor control of grasping force release. The aim of this project was to determine how PD impacts grip force release relative to the generation and maintenance of force.
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