What electrophysiology tells us about Alzheimer's disease: a window into the synchronization and connectivity of brain neurons

神经科学 神经病理学 脑电图 电生理学 脑磁图 神经影像学 心理学 神经退行性变 疾病 医学 病理
作者
Claudio Babiloni,Katarzyna J. Blinowska,Laura Bonanni,Andrzej Cichocki,Willem de Haan,Claudio Del Percio,Bruno Dubois,Javier Escudero,Alberto Fernández,Giovanni B. Frisoni,Bahar Güntekin,Mihály Hajós,Harald Hampel,Emmanuel Ifeachor,Kerry Kilborn,Sanjeev Kumar,Kristinn Johnsen,Magnús Jóhannsson,Jaeseung Jeong,Fiona E. N. LeBeau
出处
期刊:Neurobiology of Aging [Elsevier BV]
卷期号:85: 58-73 被引量:263
标识
DOI:10.1016/j.neurobiolaging.2019.09.008
摘要

Electrophysiology provides a real-time readout of neural functions and network capability in different brain states, on temporal (fractions of milliseconds) and spatial (micro, meso, and macro) scales unmet by other methodologies. However, current international guidelines do not endorse the use of electroencephalographic (EEG)/magnetoencephalographic (MEG) biomarkers in clinical trials performed in patients with Alzheimer's disease (AD), despite a surge in recent validated evidence. This position paper of the ISTAART Electrophysiology Professional Interest Area endorses consolidated and translational electrophysiological techniques applied to both experimental animal models of AD and patients, to probe the effects of AD neuropathology (i.e., brain amyloidosis, tauopathy, and neurodegeneration) on neurophysiological mechanisms underpinning neural excitation/inhibition and neurotransmission as well as brain network dynamics, synchronization, and functional connectivity, reflecting thalamocortical and corticocortical residual capacity. Converging evidence shows relationships between abnormalities in EEG/MEG markers and cognitive deficits in groups of AD patients at different disease stages. The supporting evidence for the application of electrophysiology in AD clinical research as well as drug discovery pathways warrants an international initiative to include the use of EEG/MEG biomarkers in the main multicentric projects planned in AD patients, to produce conclusive findings challenging the present regulatory requirements and guidelines for AD studies.
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