Origine des états actifs spontanés dans le néocortex pendant les oscillations du sommeil

Le sommeil à ondes lentes est composé d’une alternance entre un état actif et un état silencieux dans le système thalamocortical. Les mécanismes produisant l’état actif et l’état silencieux sont inconnus. Afin d’étudier l’origine des états actifs, nous avons procédé à l’enregistrement intracellulaire simultané de 2 à 4 neurones dans un environnement local (< 200μm) et dans un environnement distant (jusqu’à 12mm). Aussi, nous avons procédé à l’enregistrement simultané de potentiels de champ locaux (jusqu’à 16). Ces expériences ont été menées chez le chat anesthésié et chez le chat non-anesthésié. Nous avons trouvé que les cellules à bouffées de potentiels d’action ainsi que les cellules situées profondément ont tendance à être les premières à entrer dans l’état actif. Aussi, nous avons observé une grande variabilité dans les délais d’activation des cellules et ce, qu’elles soient situées près l’une de l’autre ou qu’elles soient distantes. De plus, nous avons observé que le déclenchement de l’état silencieux était beaucoup plus synchrone que le déclenchement de l’état actif.The slow-wave sleep is composed of an alternating period of active and silence state in the thalamocortical system. The mechanisms producing the active and silence state are unknown. In order to investigate the origin of active states, we performed simultaneous intracellular recording of 2 to 4 closely located (< 200μm) neurons and in a distant environment (up to 12mm). In addition, we performed simultaneous local field potentials (up to 16) recordings. These experiments were conducted on anesthetized and nonanesthetized cats. We found that Intrinsically-Bursting cells and deeply located cells have tendency to lead in the onset of the active state. We also observed a high, but similar, variability in the activation delay for closely located cells as well as for distantly located cells. In addition, we observed that the onset of silent state is much more synchronous than the onset of active state

Slow-wave sleep : generation and propagation of slow waves, role in long-term plasticity and gating

Tableau d’honneur de la Faculté des études supérieures et postdoctorales, 2012-2013.Le sommeil est connu pour réguler plusieurs fonctions importantes pour le cerveau et parmi celles-ci, il y a le blocage de l’information sensorielle par le thalamus et l’amélioration de la consolidation de la mémoire. Le sommeil à ondes lentes, en particulier, est considéré être critique pour ces deux processus. Cependant, leurs mécanismes physiologiques sont inconnus. Aussi, la marque électrophysiologique distinctive du sommeil à ondes lentes est la présence d’ondes lentes de grande amplitude dans le potentiel de champ cortical et l’alternance entre des périodes d’activités synaptiques intenses pendant lesquelles les neurones corticaux sont dépolarisés et déchargent plusieurs potentiels d’action et des périodes silencieuses pendant lesquelles aucune décharge ne survient, les neurones corticaux sont hyperpolarisés et très peu d’activités synaptiques sont observées. Tout d'abord, afin de mieux comprendre les études présentées dans ce manuscrit, une introduction générale couvrant l'architecture du système thalamocortical et ses fonctions est présentée. Celle-ci comprend une description des états de vigilance, suivie d'une description des rythmes présents dans le système thalamocortical au cours du sommeil à ondes lentes, puis par une description des différents mécanismes de plasticité synaptique, et enfin, deux hypothèses sur la façon dont le sommeil peut affecter la consolidation de la mémoire sont présentées. Puis, trois études sont présentées et ont été conçues pour caractériser les propriétés de l'oscillation lente du sommeil à ondes lentes. Dans la première étude (chapitre II), nous avons montré que les périodes d'activité (et de silence) se produisent de façon presque synchrone dans des neurones qui ont jusqu'à 12 mm de distance. Nous avons montré que l'activité était initiée en un point focal et se propageait rapidement à des sites corticaux voisins. Étonnamment, le déclenchement des états silencieux était encore plus synchronisé que le déclenchement des états actifs. L'hypothèse de travail pour la deuxième étude (chapitre III) était que les états actifs sont générés par une sommation de relâches spontanées de médiateurs. Utilisant différents enregistrements à la fois chez des animaux anesthésiés et chez d’autres non-anesthésiés, nous avons montré qu’aucune décharge neuronale ne se produit dans le néocortex pendant les états silencieux du sommeil à ondes lentes, mais certaines activités synaptiques peuvent ii être observées avant le début des états actifs, ce qui était en accord avec notre hypothèse. Nous avons également montré que les neurones de la couche V étaient les premiers à entrer dans l’état actif pour la majorité des cycles, mais ce serait ainsi uniquement pour des raisons probabilistes; ces cellules étant équipées du plus grand nombre de contacts synaptiques parmi les neurones corticaux. Nous avons également montré que le sommeil à ondes lentes et l’anesthésie à la kétamine-xylazine présentent de nombreuses similitudes. Ayant utilisé une combinaison d'enregistrements chez des animaux anesthésiés à la kétamine-xylazine et chez des animaux non-anesthésiés, et parce que l'anesthésie à la kétamine-xylazine est largement utilisée comme un modèle de sommeil à ondes lentes, nous avons effectué des mesures quantitatives des différences entre les deux groupes d'enregistrements (chapitre IV). Nous avons trouvé que l'oscillation lente était beaucoup plus rythmique sous anesthésie et elle était aussi plus cohérente entre des sites d’enregistrements distants en comparaison aux enregistrements de sommeil naturel. Sous anesthésie, les ondes lentes avaient également une amplitude plus grande et une durée plus longue par rapport au sommeil à ondes lentes. Toutefois, les ondes fuseaux (spindles) et gamma étaient également affectées par l'anesthésie. Dans l'étude suivante (Chapitre V), nous avons investigué le rôle du sommeil à ondes lentes dans la formation de la plasticité à long terme dans le système thalamocortical. À l’aide de stimulations pré-thalamiques de la voie somatosensorielle ascendante (fibres du lemnisque médial) chez des animaux non-anesthésiés, nous avons montré que le potentiel évoqué enregistré dans le cortex somatosensoriel était augmenté dans une période d’éveil suivant un épisode de sommeil à ondes lentes par rapport à l’épisode d’éveil précédent et cette augmentation était de longue durée. Nous avons également montré que le sommeil paradoxal ne jouait pas un rôle important dans cette augmentation d'amplitude des réponses évoquées. À l’aide d'enregistrements in vitro en mode cellule-entière, nous avons caractérisé le mécanisme derrière cette augmentation et ce mécanisme est compatible avec la forme classique de potentiation à long terme, car il nécessitait une activation à la fois les récepteurs NMDA et des récepteurs AMPA, ainsi que la présence de calcium dans le neurone post-synaptique. iii La dernière étude incluse dans cette thèse (chapitre VI) a été conçue pour caractériser un possible mécanisme physiologique de blocage sensoriel thalamique survenant pendant le sommeil. Les ondes fuseaux sont caractérisées par la présence de potentiels d’action calcique à seuil bas et le calcium joue un rôle essentiel dans la transmission synaptique. En utilisant plusieurs techniques expérimentales, nous avons vérifié l'hypothèse que ces potentiels d’action calciques pourraient causer un appauvrissement local de calcium dans l'espace extracellulaire ce qui affecterait la transmission synaptique. Nous avons montré que les canaux calciques responsables des potentiels d’action calciques étaient localisés aux synapses et que, de fait, une diminution locale de la concentration extracellulaire de calcium se produit au cours d’un potentiel d’action calcique à seuil bas spontané ou provoqué, ce qui était suffisant pour nuire à la transmission synaptique. Nous concluons que l'oscillation lente est initiée en un point focal et se propage ensuite aux aires corticales voisines de façon presque synchrone, même pour des cellules séparées par jusqu'à 12 mm de distance. Les états actifs de cette oscillation proviennent d’une sommation de relâches spontanées de neuromédiateurs (indépendantes des potentiels d’action) et cette sommation peut survenir dans tous neurones corticaux. Cependant, l’état actif est généré plus souvent dans les neurones pyramidaux de couche V simplement pour des raisons probabilistes. Les deux types d’expériences (kétamine-xylazine et sommeil à ondes lentes) ont montré plusieurs propriétés similaires, mais aussi quelques différences quantitatives. Nous concluons également que l'oscillation lente joue un rôle essentiel dans l'induction de plasticité à long terme qui contribue très probablement à la consolidation de la mémoire. Les ondes fuseaux, un autre type d’ondes présentes pendant le sommeil à ondes lentes, contribuent au blocage thalamique de l'information sensorielle.Sleep is known to mediate several major functions in the brain and among them are the gating of sensory information during sleep and the sleep-related improvement in memory consolidation. Slow-wave sleep in particular is thought to be critical for both of these processes. However, their physiological mechanisms are unknown. Also, the electrophysiological hallmark of slow-wave sleep is the presence of large amplitude slow waves in the cortical local field potential and the alternation of periods of intense synaptic activity in which cortical neurons are depolarized and fire action potentials and periods of silence in which no firing occurs, cortical neurons are hyperpolarized, and very little synaptic activities are observed. First, in order to better understand the studies presented in this manuscript, a general introduction covering the thalamocortical system architecture and function is presented, which includes a description of the states of vigilance, followed by a description of the rhythms present in the thalamocortical system during slow-wave sleep, then by a description of the mechanisms of synaptic plasticity, and finally two hypotheses about how sleep might affect the consolidation of memory are presented. Then, three studies are presented and were designed to characterize the properties of the sleep slow oscillation. In the first study (Chapter II), we showed that periods of activity (and silence) occur almost synchronously in neurons that are separated by up to 12 mm. The activity was initiated in a focal point and rapidly propagated to neighboring sites. Surprisingly, the onsets of silent states were even more synchronous than onsets of active states. The working hypothesis for the second study (Chapter III) was that active states are generated by a summation of spontaneous mediator releases. Using different recordings in both anesthetized and non-anesthetized animals, we showed that no neuronal firing occurs in the neocortex during silent states of slow-wave sleep but some synaptic activities might be observed prior to the onset of active states, which was in agreement with our hypothesis. We also showed that layer V neurons were leading the onset of active states in most of the cycles but this would be due to probabilistic reasons; these cells being equipped with the most numerous synaptic contacts among cortical neurons. We also showed that slow-wave sleep and ketamine-xylazine shares many similarities. v Having used a combination of recordings in ketamine-xylazine anesthetized and non-anesthetized animals, and because ketamine-xylazine anesthesia is extensively used as a model of slow-wave sleep, we made quantitative measurements of the differences between the two groups of recordings (Chapter IV). We found that the slow oscillation was much more rhythmic under anesthesia and it was also more coherent between distant sites as compared to recordings during slow-wave sleep. Under anesthesia, slow waves were also of larger amplitude and had a longer duration as compared to slow-wave sleep. However, spindles and gamma were also affected by the anesthesia. In the following study (Chapter V), we investigated the role of slow-wave sleep in the formation of long-term plasticity in the thalamocortical system. Using pre-thalamic stimulations of the ascending somatosensory pathway (medial lemniscus fibers) in non-anesthetized animals, we showed that evoked potential recorded in the somatosensory cortex were enhanced in a wake period following a slow-wave sleep episode as compared to the previous wake episode and this enhancement was long-lasting. We also showed that rapid eye movement sleep did not play a significant role in this enhancement of response amplitude. Using whole-cell recordings in vitro, we characterized the mechanism behind this enhancement and it was compatible with the classical form of long-term potentiation, because it required an activation of both NMDA and AMPA receptors as well as the presence of calcium in the postsynaptic neuron. The last study included in this thesis (Chapter VI) was designed to characterise a possible physiological mechanism of thalamic sensory gating occurring during sleep. Spindles are characterized by the presence of low-threshold calcium spikes and calcium plays a critical role in the synaptic transmission. Using several experimental techniques, we verified the hypothesis that these calcium spikes would cause a local depletion of calcium in the extracellular space which would impair synaptic transmission. We showed that calcium channels responsible for calcium spikes were co-localized with synapses and that indeed, local extracellular calcium depletion occurred during spontaneous or induced low-threshold calcium spike, which was sufficient to impair synaptic transmission. We conclude that slow oscillation originate at a focal point and then propagate to neighboring cortical areas being almost synchronous even in cells located up to 12 mm vi apart. Active states of this oscillation originate from a summation of spike-independent mediator releases that might occur in any cortical neurons, but happens more often in layer V pyramidal neurons simply due to probabilistic reasons. Both experiments in ketamine-xylazine anesthesia and non-anesthetized animals showed several similar properties, but also some quantitative differences. We also conclude that slow oscillation plays a critical role in the induction of long-term plasticity, which very likely contributes to memory consolidation. Spindles, another oscillation present in slow-wave sleep, contribute to the thalamic gating of information

Sleep slow oscillation and plasticity

It is well documented that sleep contributes to memory consolidation and it is also accepted that long-term synaptic plasticity plays a critical role in memory formation. The mechanisms of this sleep-dependent memory formation are unclear. Two main hypotheses are proposed. According to the first one, synapses are potentiated during wake; and during sleep they are scaled back to become available for the learning tasks in the next day. The other hypothesis is that sleep slow oscillations potentiate synapses that were depressed due to persistent activities during the previous day and that potentiation provides physiological basis for memory consolidation. The objective of this review is to group information on whether cortical synapses are up-scaled or down-scaled during sleep. We conclude that the majority of cortical synapses are up-regulated by sleep slow oscillation

Properties of slow oscillation during slow-wave sleep and anesthesia in cats

Deep anesthesia is commonly used as a model of slow-wave sleep (SWS). Ketamine–xylazine anesthesia reproduces the main features of sleep slow oscillation: slow, large-amplitude waves in field potential, which are generated by the alternation of hyperpolarized and depolarized states of cortical neurons. However, direct quantitative comparison of field potential and membrane potential fluctuations during natural sleep and anesthesia is lacking, so it remains unclear how well the properties of sleep slow oscillation are reproduced by the ketamine–xylazine anesthesia model. Here, we used field potential and intracellular recordings in different cortical areas in the cat to directly compare properties of slow oscillation during natural sleep and ketamine–xylazine anesthesia. During SWS cortical activity showed higher power in the slow/delta (0.1–4 Hz) and spindle (8–14 Hz) frequency range, whereas under anesthesia the power in the gamma band (30–100 Hz) was higher. During anesthesia, slow waves were more rhythmic and more synchronous across the cortex. Intracellular recordings revealed that silent states were longer and the amplitude of membrane potential around transition between active and silent states was bigger under anesthesia. Slow waves were mostly uniform across cortical areas under anesthesia, but in SWS, they were most pronounced in associative and visual areas but smaller and less regular in somatosensory and motor cortices. We conclude that, although the main features of the slow oscillation in sleep and anesthesia appear similar, multiple cellular and network features are differently expressed during natural SWS compared with ketamine–xylazine anesthesia

Precise long-range synchronization of activity and silence in neocortical neurons during slow-wave sleep

Slow-wave sleep is characterized by alternating periods of activity and silence in corticothalamic networks. Both activity and silence are stable network states, but the mechanisms of their alternation remain unknown. We show, using simultaneous multisite intracellular recordings in cats, that slow rhythm involves all neocortical neurons and that both activity and silence started almost synchronously in cells located up to 12 mm apart. Activity appeared predominantly at the area 5/7 border and spread in both anterior and posterior directions. The activity started earlier in fast-spiking cells and intrinsically bursting cells than in regular-spiking neurons. These results provide direct evidencefortwo mechanisms of active state generation: spread of activityfrom a localfocus and synchronization of weaker activity, originating at multiple locations. Surprisingly, onsets of silent states were synchronized even more precisely than the onsets of activity, showing no latency bias for location or cell type. This most intriguing finding exposes a major gap in understanding the nature of state alternation. We suggest that it is the synchronous termination of activity and occurrence of silent states of the neuronal network that makes the EEG picture during slow-wave sleep so characteristic. Synchronous onset of silence in distant neurons cannot rely exclusively on properties of individual cells and synapses, such as adaptation of neuronalfiring or synaptic depression; instead, it implies the existence of a network mechanism. Revealing this yet unknown large-scale mechanism, which switches network activity to silence, will aid our understanding of the origin of brain rhythms in normal function and pathology

Age dependency of trauma-induced neocortical epileptogenesis

Trauma and brain infection are the primary sources of acquired epilepsy, which can occur at any age and may account for a high incidence of epilepsy in developing countries. We have explored the hypothesis that penetrating cortical wounds cause deafferentation of the neocortex, which triggers homeostatic plasticity and lead to epileptogenesis (Houweling et al., 2005). In partial deafferentation experiments of adult cats, acute seizures occurred in most preparations and chronic seizures occurred weeks to months after the operation in 65% of the animals (Nita et al., 2006, 2007; Nita and Timofeev, 2007). Similar deafferentation of young cats (age 8–12 months) led to some acute seizures, but we never observed chronic seizure activity even though there was enhanced slow-wave activity in the partially deafferented hemisphere during quiet wakefulness. This suggests that despite a major trauma, the homeostatic plasticity in young animals was able to restore normal levels of cortical excitability, but in fully adult cats the mechanisms underlying homeostatic plasticity may lead to an unstable cortical state. To test this hypothesis we made an undercut in the cortex of an elderly cat. After several weeks this animal developed seizure activity. These observations may lead to an intervention after brain trauma that prevents epileptogenesis from occurring in adults

Modeling of age-dependent epileptogenesis by differential homeostatic synaptic scaling

Homeostatic synaptic plasticity (HSP) has been implicated in the development of hyperexcitability and epileptic seizures following traumatic brain injury (TBI). Our in vivo experimental studies in cats revealed that the severity of TBI-mediated epileptogenesis depends on the age of the animal. To characterize mechanisms of these differences, we studied the properties of the TBI-induced epileptogenesis in a biophysically realistic cortical network model with dynamic ion concentrations. After deafferentation, which was induced by dissection of the afferent inputs, there was a reduction of the network activity and upregulation of excitatory connections leading to spontaneous spike-and-wave type seizures. When axonal sprouting was implemented, the seizure threshold increased in the model of young but not the older animals, which had slower or unidirectional homeostatic processes. Our study suggests that age-related changes in the HSP mechanisms are sufficient to explain the difference in the likelihood of seizure onset in young versus older animals

Origin of Active States in Local Neocortical Networks during Slow Sleep Oscillation

Slow-wave sleep is characterized by spontaneous alternations of activity and silence in corticothalamic networks, but the causes of transition from silence to activity remain unknown. We investigated local mechanisms underlying initiation of activity, using simultaneous multisite field potential, multiunit recordings, and intracellular recordings from 2 to 4 nearby neurons in naturally sleeping or anesthetized cats. We demonstrate that activity may start in any neuron or recording location, with tens of milliseconds delay in other cells and sites. Typically, however, activity originated at deep locations, then involved some superficial cells, but appeared later in the middle of the cortex. Neuronal firing was also found to begin, after the onset of active states, at depths that correspond to cortical layer V. These results support the hypothesis that switch from silence to activity is mediated by spontaneous synaptic events, whereby any neuron may become active first. Due to probabilistic nature of activity onset, the large pyramidal cells from deep cortical layers, which are equipped with the most numerous synaptic inputs and large projection fields, are best suited for switching the whole network into active state

Origin of Active States in Local Neocortical Networks during Slow Sleep Oscillation

Slow-wave sleep is characterized by spontaneous alternations of activity and silence in corticothalamic networks, but the causes of transition from silence to activity remain unknown. We investigated local mechanisms underlying initiation of activity, using simultaneous multisite field potential, multiunit recordings, and intracellular recordings from 2 to 4 nearby neurons in naturally sleeping or anesthetized cats. We demonstrate that activity may start in any neuron or recording location, with tens of milliseconds delay in other cells and sites. Typically, however, activity originated at deep locations, then involved some superficial cells, but appeared later in the middle of the cortex. Neuronal firing was also found to begin, after the onset of active states, at depths that correspond to cortical layer V. These results support the hypothesis that switch from silence to activity is mediated by spontaneous synaptic events, whereby any neuron may become active first. Due to probabilistic nature of activity onset, the large pyramidal cells from deep cortical layers, which are equipped with the most numerous synaptic inputs and large projection fields, are best suited for switching the whole network into active state

The spindles : are they still thalamic?

Commentary on Ayoub et al. Differential effects on fast and slow spindle activity, and the sleep slow oscillation in humans with carbamazepine and flunarizine to antagonize voltage-dependent Na+ and Ca2+ channel activity