Contrôle homéostatique de l'activité corticale: Etude de la balance Excitation / Inhibition des neurones pyramidaux de couche 5 du cortex visuel.

Le Roux, Nicolas

21 June 2007

La plasticité homéostatique est un processus qui consiste à réguler l'efficacité globale des entrées synaptiques (excitatrices et inhibitrices) sur un neurone afin d'empêcher des modifications trop importantes de son niveau d'activité. Afin de caractériser les mécanismes à l'origine de ce processus, la balance Excitation/Inhibition des neurones pyramidaux de couche 5 du cortex visuel a été estimée. Elle est composée de 20 % d'excitation et de 80 % d'inhibition. A l'aide de protocoles de stimulation induisant des changements à long terme de l'efficacité des entrées synaptiques, les phénomènes de potentiation homéostatique et de dépression homéostatique ont été mis en évidence. L'induction de ces phénomènes, qui requiert l'activation de récepteurs NMDA et d'un signal NO, est sous le contrôle des systèmes inhibiteurs GABAergique et glycinergique. La récurrence entre signaux excitateurs et inhibiteurs apparaît comme l'élément clé de la régulation de l'activité neuronale.

balance Excitation/Inhibition

plasticité homéostatique

neurones pyramidaux

cortex

réseaux neuronaux

interactions récurrentes

Behavioral, Functional, and Neurophysiological Responses to One-week Administration of Escitalopram

Molloy, Eóin

12 July 2022

Doctoral thesis assessing the effects of one-week of escitalopram administration on healthy humans during sequence motor learning training. Published in 3 research articles.

info:eu-repo/classification/ddc/610

ddc:610

Dynamics underlying epileptic seizures: insights from a neural mass model

Fan, Xiaoya

17 December 2018

In this work, we propose an approach that allows to explore the potential pathophysiological mechanisms (at neuronal population level) of ictogenesis by combining clinical intracranial electroencephalographic (iEEG) recordings with a neural mass model. IEEG recordings from temporal lobe epilepsy (TLE) patients around seizure onset were investigated. Physiologically meaningful parameters (average synaptic gains of the excitatory, slow and fast inhibitory population, Ae, B and G) were identified during interictal to ictal transition. We analyzed the temporal evolution of four ratios, i.e. Ae/G, Ae/B, Ae/(B + G), and B/G. The excitation/inhibition ratio increased around seizure onset and decreased before seizure offset, suggesting the disturbance and restoration of balance between excitation and inhibition around seizure onset and before seizure offset, respectively. Moreover, the slow inhibition may have an earlier effect on the breakdown of excitation/inhibition balance. Results confirm the decrease in excitation/inhibition ratio upon seizure termination in human temporal lobe epilepsy, as revealed by optogenetic approaches both in vivo in animal models and in vitro. We further explored the distribution of the average synaptic gains in parameter space and their temporal evolution, i.e. the path through the model parameter space, in TLE patients. Results showed that the synaptic gain values located roughly on a plane before seizure onset, dispersed during ictal and returned when the seizure terminated. Cluster analysis was performed on seizure paths and demonstrated consistency in synaptic gain evolution across different seizures from individual patients. Furthermore, two patient groups were identified, each one corresponding to a specific synaptic gain evolution in the parameter space during a seizure. Results were validated by a bootstrapping approach based on comparison with random paths. The differences in the path revealed variations in EEG dynamics for patients despite showing an identical seizure onset pattern. Our approach may have the potential to classify the epileptic patients into subgroups based on different mechanisms revealed by subtle changes in synaptic gains and further enable more robust decisions regarding treatment strategy. The increase of excitation/inhibition ratios, i.e. Ae/G, Ae/B and Ae/(B+G), around seizure onset makes them potential cues for seizure detection. We explored the feasibility of a model based seizure detection algorithm. A simple thresholding method was employed. We evaluated the algorithm against the manual scoring of a human expert on iEEG samples from patients suffering from different types of epilepsy. Results suggest that Ae/(B+G), i.e. excitation/(slow + fast inhibition) ratio, allowed the best performance and that the algorithm best suited TLE patients. Leave-one-out cross-validation showed that the algorithm achieved 94.74% sensitivity for TLE patients. The median false positive rate was 0.16 per hour, and median detection delay was -1.0 s. Of interest, the values of the threshold determined by leave-one-out cross-validation for TLE patients were quite constant, suggesting a general excitation/inhibition balance baseline in background iEEG among TLE patients. Such a model-based seizure detection approach is of clinical interest and could also achieve good performance for other types of epilepsy provided that more appropriate model, i.e. better describe epileptic EEG waveforms for other types of epilepsy, is implemented. Altogether, this thesis contributes to the field of epilepsy research from two perspectives. Scientifically, it gives new insights into the mechanisms underlying interictal to ictal transition, and facilitates better understanding of epileptic seizures. Clinically, it provides a tool for reviewing EEG data in a more efficient and objective manner and offers an opportunity for on-demand therapeutic devices. / Doctorat en Sciences de l'ingénieur et technologie / info:eu-repo/semantics/nonPublished

Ingénierie biomédicale

Epilepsy

Excitation/inhibition balance

iEEG

Parameter identification

Neural mass model

Clustering analysis

Early seizure detection

Ictogenesis

Synaptic gain evolution

Modulation of cerebellar Purkinje cell discharge by subthreshold granule cell inputs / Modulation de la décharge des cellules de Purkinje du cervelet par des entrées sous-seuils des cellules des grains

Grangeray-Vilmint, Anais

02 June 2016

La décharge des cellules de Purkinje (CP), neurone de sortie du cortex cérébelleux, joue un rôle majeur dans le contrôle moteur. Les CP reçoivent des entrées excitatrices provenant des cellules des grains (CG), lesquelles génèrent également une inhibition antérograde sur les CP via l’activation d’interneurones de la couche moléculaire (IN). Lors de ma thèse, j’ai étudié l’influence simultanée de la balance excitation-inhibition (E/I) et des plasticités à court terme aux synapses CG-IN-CP sur la décharge des CP, par des techniques d’électrophysiologie, d’optogénétique et de simulation. Ces travaux démontrent l’existence d’une hétérogénéité d’E/I dans le cortex cérébelleux ainsi qu’une grande diversité de modulation des CP en réponse à la stimulation de CG. Le nombre de stimulation des CG influence fortement la direction et l’intensité de la modulation observée. Enfin, la combinaison de plasticités à court terme et d’E/I génère dans la décharge des CP des motifs de réponses complexes mais reproductibles, ayant sans doute un rôle essentiel dans l’encodage sensoriel. / Rate and temporal coding in Purkinje cells (PC), the sole output of the cerebellar cortex, play a major role in motor control. PC receives excitatory inputs from granule cells (GC) which also provide feedforward inhibition on PC through the activation of molecular layer interneurons (MLI). In this thesis, I studied the influence of the combined action of excitation/inhibition (E/I) balance and short-term plasticity of GC-MLI-PC synapses on PC discharge, by using electrophysiological recordings, optogenetic stimulation and modelling. This work demonstrates that E/I balances are not equalized in the cerebellar cortex and showed a wide distribution of PC discharge modulation in response to GC inputs, from an increase to a shut down of the discharge. The number of stims in GC bursts strongly controls the strength and sign of PC modulation. Lastly, the interplay between short-term plasticity and E/I balance implements complex but reproducible output patterns of PC responses to GC inputs that should play a key role in stimulus encoding by the cerebellar cortex.

Cellule de Purkinje

Cellule des grains

Cervelet

Électrophysiologie in vitro

Potentiel d’action

Codage neuronal

Balance excitation-inhibition

Plasticités synaptiques à court terme

Neurosciences

Purkinje cell

Granule cell

Cerebellum

In vitro electrophysiology

Spike

Feedforward inhibition

Short-term synaptic plasticity

Neural coding

Excitation-inhibition balance

Neuroscience

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