191 |
The neuropathology of the social cognitive network in autismMcKavanagh, Rebecca January 2014 (has links)
Potential differences in developmental trajectory were investigated in autism at both the macro- and micro-scopic scale, using regional volumetric measurements from in-vivo scans and measurements of minicolumnar organisation of the cortex in post-mortem tissue. In addition, a study was carried out to investigate the sensitivity of measures of cortical diffusion to cortical architecture. Three key regions of interest were studied throughout this thesis, orbital frontal cortex (BA11), primary auditory cortex (BA41) and part of the inferior parietal lobe (BA40). Subjects with ASD showed increases in grey matter in left parietal cortex and decreases in left BA11 compared to controls. In addition, subjects with ASD showed increased grey matter volume with age in both BA41 and the inferior parietal lobe, whereas controls only showed a negative correlation between grey matter volume in BA41 and age. Wider minicolumns were found in ASD in all regions, suggesting pathology is not restricted to higher order association areas. Differences seemed more pronounced at younger ages suggesting an altered developmental trajectory in ASD. Such an increase in minicolumnar width arguably underlies the feature-based processing style seen in ASD. A pilot study using post-mortem DTI scans of MS brains revealed a relationship between measures of the directionality of diffusion and the width of axonal bundles in the cortex, an aspect of the minicolumnar arrangement. When extending this investigation to a set of ASD and control brains, evidence was found for different relationships between axon bundle width and measures of the directionality of diffusion in the cortex, suggesting that although differences in axon bundle width were not seen between groups, there may be differences in the composition of the axon bundles between ASD and control groups.
|
192 |
Structural and functional brain abnormalities in children with subclinical depressionMancini-Marïe, Adham January 2007 (has links)
Mémoire numérisé par la Division de la gestion de documents et des archives de l'Université de Montréal.
|
193 |
Emotional processing of natural visual images in brief exposures and compound stimuli : fMRI and behavioural studiesShaw, Lynda Joan January 2009 (has links)
Can the brain register the emotional valence of brief exposures of complex natural stimuli under conditions of forward and backward masking, and under conditions of attentional competition between foveal and peripheral stimuli? To address this question, three experiments were conducted. The first, a behavioural experiment, measured subjective valence of response (pleasant vs unpleasant) to test the perception of the valence of natural images in brief, masked exposures in a forward and backward masking paradigm. Images were chosen from the International Affective Picture System (IAPS) series. After correction for response bias, responses to the majority of target stimuli were concordant with the IAPS ratings at better than chance, even when the presence of the target was undetected. Using functional magnetic resonance imaging (fMRI), the effects of IAPS valence and stimulus category were objectively measured on nine regions of interest (ROIs) using the same strict temporal restrictions in a similar masking design. Evidence of affective processing close to or below conscious threshold was apparent in some of the ROIs. To further this line of enquiry, a second fMRI experiment mapping the same ROIs and using the same stimuli were presented in a foveal (‘attended’) peripheral (‘to-be-ignored’) paradigm (small image superimposed in the centre of a large image of the same category, but opposite valence) to investigate spatial parameters and limitations of attention. Results are interpreted as showing both valence and category specific effects of ‘to-be-ignored’ images in the periphery. These results are discussed in light of theories of the limitations of attentional capacity and the speed in which we process natural images, providing new evidence of the breadth of variety in the types of affective visual stimuli we are able to process close to the threshold of conscious perception.
|
194 |
Software tool for modelling coding and processing of information in auditory cortex of mice / Software tool for modelling coding and processing of information in auditory cortex of micePopelová, Markéta January 2013 (has links)
Autor Markéta Popelová Název práce Software tool for modelling coding and processing of information in auditory cortex of mice Abstrakt Porozumění zpracovávání a kódování informací ve sluchové k·ře (AC) je stále ne- dostatečné. Z několika r·zných d·vod· by bylo užitečné mít výpočetní model AC, například z d·vodu vysvětlení, či ujasnění procesu kódování informací v AC. Prv- ním cílem této práce bylo vytvořit softwarový nástroj (simulátor SUSNOMAC), zaměřený na modelování AC. Druhým cílem bylo navrhnout výpočetní model AC s následujícími vlastnostmi: Izhikevich·v model neuronu, dlouhodobá plasticita ve formě Spike-timing-dependent plasticity (STDP), šestivrstvá architektura, pa- rametrizované typy neuron·, hustota neuron· a pravděpodobnost vzniku synapsí. Navržený model byl testován v desítkách experiment·, s r·znými sadami para- metr· a v r·zných velikostech (až 100 000 neuron· s takřka 21 milióny synapsí). Experimenty byly analyzovány a jejich výsledky srovnány s pozorováním skutečné AC. V práci popisujeme a analyzujeme několik zajímavých pozorování o aktivitě modelované sítě a vzniku tonotopického uspořádání AC. 1
|
195 |
Role of cortical parvalbumin interneurons in fear behaviour / Rôle des interneurones corticaux parvalbuminergiques dans les comportements de peurCourtin, Julien 13 December 2013 (has links)
Les processus d'apprentissage et de mémoire sont contrôlés par des circuits et éléments neuronaux spécifiques. De nombreuses études ont récemment mis en évidence que les circuits corticaux jouent un rôle important dans la régulation des comportements de peur, cependant, leurs caractéristiques anatomiques et fonctionnelles restent encore largement inconnues. Au cours de ma thèse, en utilisant des enregistrements unitaires et des approches optogénétiques chez la souris libre de se comporter, nous avons pu montrer que les interneurones inhibiteurs du cortex auditif et du cortex préfrontal médian forment un microcircuit désinhibiteur permettant respectivement l'acquisition et l'expression de la mémoire de peur conditionnée. Dans les deux cas, les interneurones parvalbuminergiques constituent l'élément central du circuit et sont inhibés de façon phasique. D’un point de vue fonctionnel, nous avons démontré que cette inhibition était associée à la désinhibition des neurones pyramidaux par un mécanisme de réduction de l'inhibition continue exercée par les interneurones parvalbuminergiques. Ainsi, les interneurones parvalbuminergiques peuvent contrôler temporellement l'excitabilité des neurones pyramidaux. En particulier, nous avons montré que l'acquisition de la mémoire de peur conditionnée dépend du recrutement d'un microcircuit désinhibiteur localisé dans le cortex auditif. En effet, au cours du conditionnement de peur, la présentation du choc électrique induit l'inhibition des interneurones parvalbuminergiques, ce qui a pour conséquence de désinhiber les neurones pyramidaux du cortex auditif et de permettre l’apprentissage du conditionnement de peur. Dans leur ensemble, ces données suggèrent que la désinhibition est un mécanisme important dans l'apprentissage et le traitement de l'information dans les circuits corticaux. Dans un second temps, nous avons montré que l'expression de la peur conditionnée requière l'inhibition phasique des interneurones parvalbuminergiques du cortex préfrontal médian. En effet, leur inhibition désinhibe les cellules pyramidales préfrontales et synchronise leur activité en réinitialisant les oscillations thêta locales. Ces résultats mettent en évidence deux mécanismes neuronaux complémentaires induits par les interneurones parvalbuminergiques qui coordonnent et organisent avec précision l’activité neuronale des neurones pyramidaux du cortex préfrontal pour contrôler l'expression de la peur conditionnée. Ensemble, nos données montrent que la désinhibition joue un rôle important dans les comportements de peur en permettant l’association entre des informations comportementalement pertinentes, en sélectionnant les éléments spécifiques du circuit et en orchestrant l'activité neuronale des cellules pyramidales. / Learning and memory processes are controlled by specific neuronal circuits and elements. Numerous recent reports highlighted the important role of cortical circuits in the regulation of fear behaviour, however, the anatomical and functional characteristics of their neuronal components remain largely unknown. During my thesis, we used single unit recordings and optogenetic manipulations of specific neuronal elements in behaving mice, to show that both the auditory cortex and the medial prefrontal cortex contain a disinhibitory microcircuit required respectively for the acquisition and the expression of conditioned fear memory. In both cases, parvalbumin-expressing interneurons constitute the central element of the circuit and are phasically inhibited during the presentation of the conditioned tone. From a functional point of view, we demonstrated that this inhibition induced the disinhibition of cortical pyramidal neurons by releasing the ongoing perisomatic inhibition mediated by parvalbumin-expressing interneurons onto pyramidal neurons. Thereby, this disinhibition allows the precise temporal regulation of pyramidal neurons excitability. In particular, we showed that the acquisition of associative fear memories depend on the recruitment of a disinhibitory microcircuit in the auditory cortex. Fear-conditioning-associated disinhibition in auditory cortex is driven by foot-shock-mediated inhibition of parvalbumin-expressing interneurons. Importantly, pharmacological or optogenetic blockade of pyramidal neuron disinhibition abolishes fear learning. Together, these data suggest that disinhibition is an important mechanism underlying learning and information processing in cortical circuits. Secondly, in the medial prefrontal cortex, we demonstrated that expression of fear behaviour is causally related to the phasic inhibition of prefrontal parvalbumin-expressing interneurons. Inhibition of parvalbumin-expressing interneuron activity disinhibits prefrontal pyramidal neurons and synchronizes their firing by resetting local theta oscillations, leading to fear expression. These results identify two complementary neuronal mechanisms both mediated by prefrontal parvalbumin-expressing interneurons that precisely coordinate and enhance the neuronal efficiency of prefrontal pyramidal neurons to drive fear expression. Together these data highlighted the important role played by neuronal disinhibition in fear behaviour by binding behavioural relevant information, selecting specific circuit elements and orchestrating pyramidal neurons activity.
|
196 |
Modeling the emergence of perceptual color space in the primary visual cortexBall, Christopher Edward January 2015 (has links)
Humans’ perceptual experience of color is very different from what one might expect, given the light reaching the eye. Identical patterns of light are often perceived as different colors, and different patterns of light are often perceived as the same color. Even more strikingly, our perceptual experience is that hues are arranged circularly (with red similar to violet), even though single-wavelength lights giving rise to perceptions of red and violet are at opposite ends of the wavelength spectrum. The goal of this thesis is to understand how perceptual color space arises in the brain, focusing on the arrangement of hue. To do this, we use computational modeling to integrate findings about light, physiology of the visual system, and color representation in the brain. Recent experimental work shows that alongside spatially contiguous orientation preference maps, macaque primary visual cortex (V1) represents color in isolated patches, and within those patches hue appears to be spatially organized according to perceptual color space. We construct a model of the early visual system that develops based on natural input, and we demonstrate that several factors interact to prevent this first model from developing a realistic representation of hue. We show these factors as independent dimensions and relate them to problems the brain must be overcoming in building a representation of perceptual color space: physiological and environmental variabilities to which the brain is relatively insensitive (surprisingly, given the importance of input in driving development). We subsequently show that a model with a certain position on each dimension develops a hue representation matching the range and spatial organization found in macaque V1—the first time a model has done so. We also show that the realistic results are part of a spectrum of possible results, indicating other organizations of color and orientation that could be found in animals, depending on physiological and environmental factors. Finally, by analyzing how the models work, we hypothesize that well-accepted biological mechanisms such as adaptation, typically omitted from models of both luminance and color processing, can allow the models to overcome these variabilities, as the brain does. These results help understand how V1 can develop a stable, consistent representation of color despite variabilities in the underlying physiology and input statistics. This in turn suggests how the brain can build useful, stable representations in general based on visual experience, despite irrelevant variabilities in input and physiology. The resulting models form a platform to investigate various adult color visual phenomena, as well as to predict results of rearing experiments.
|
197 |
Modelling microcircuits of grid cells and theta-nested gamma oscillations in the medial entorhinal cortexSolanka, Lukas January 2015 (has links)
The relationship between structure, dynamics, and function of neural networks in nervous systems is still an open question in the neuroscience community. Nevertheless, for certain areas of the mammalian nervous system we do have sufficient data to impose constraints on the organisation of the network structure. One of these areas is the medial entorhinal cortex which contains cells with hexagonally repeating spatial receptive fields, called grid cells. Another intriguing property of entorhinal cortex and other cortical regions is a population oscillatory activity, with frequency in the theta (4-10 Hz) and gamma (30-100 Hz) range. This leads to a question, whether these oscillations are a common circuit mechanism that is functionally relevant and how the oscillatory activity interacts with the computation performed by grid cells. This thesis deals with applying the continuous attractor network theory to modelling of the microcircuit of layer II in the medial entorhinal cortex. Based on recent experimental evidence on connectivity between stellate cells, and fast spiking interneurons, I first develop a two-population spiking attractor network model that is capable of reproducing the activity of a population of grid cells in layer II. The network was implemented with exponential integrate and fire neurons that allowed me to address both the attractor states and the oscillatory activity in this region. Subsequently, I show that the network can produce theta-nested gamma oscillations with properties that are similar to the cross-frequency coupling observed in vivo and in vitro in entorhinal cortex, and that these theta-nested gamma oscillations can co-exist with grid-like receptive fields generated by the network. I also show that the connectivity inspired by anatomical evidence produces a number of directly testable predictions about the firing fields of interneurons in layer II of the medial entorhinal cortex. The excitatory-inhibitory attractor network, together with the theta-nested gamma oscillations, allowed me to explore potential relationships between nested gamma oscillations and grid field computations. I show, by varying the overall level of excitatory and inhibitory synaptic strengths, and levels of noise, in the network, that this relationship is complex, and not easily predictable. Specifically, I show that noise promotes generation of grid firing fields and theta-nested gamma oscillations by the model. I subsequently demonstrate that theta-nested gamma oscillations are dissociable from the grid field computations performed by the network. By changing the relative strengths of interactions between excitatory and inhibitory neurons in the network, the power and frequency of the gamma oscillations changes without disrupting the rate-coded grid field computations. Since grid cells have been suggested to be a part of the spatial cognitive circuit in the brain, these results have potential implications for several cognitive disorders, including autism and schizophrenia, as well as theories that propose a cognitive role for gamma oscillations.
|
198 |
Étude per-opératoire par stimulation électrique directe des représentation sensorimotrices corticales et cérébelleuses chez l'homme / Per-operative investigation with direct electrical stimulation of cortical and cerebellar sensorimotor representations in humansMottolese, Carmine 21 December 2013 (has links)
Durant les dernières décennies, le système moteur a été largement étudié. Pourtant, bien des zones d'incertitudes persistent concernant d'une part la nature des circuits neuronaux de haut niveau impliqués dans l'émergence des sentiments d'intention ou de conscience motrice et d'autre part l'organisation des structures cérébrales de bas-niveau impliquées dans l'expression de ces sentiments. Il a été suggéré que le cortex pariétal et l'aire motrice supplémentaire pourraient jouer un rôle dans la génération des intentions motrices, alors que le cortex prémoteur pourrait plutôt sous-tendre la conscience du geste. Cela étant, les processus exacts implémentés dans chacune de ces régions, la façon dont elles interagissent fonctionnellement et la nature des signaux qu'elles échangent avec les structures sensorimotrices considérées de bas-niveau demeurent méconnus. Il est établi que ces structures bas-niveau, dont le cortex moteur primaire et le cervelet, contiennent des cartes sensorimotrices organisées de manière topographique. Cependant, l'organisation fine de cette topographie et la nature des interactions entre les différentes cartes restent à définir. Dans ce travail de thèse, j'ai utilisé la stimulation électrique directe chez des patients opérés de tumeurs et malformations cérébrales pour explorer la manière dont les multiples représentations motrices sont organisées et pour identifier les régions responsables de l'émergence des sentiments d'intention et de conscience motrice. J'ai alors pu montrer, en particulier, l'existence de cartes motrices multiples au sein des cortex moteur primaire et cérébelleux. Par ailleurs, j'ai pu identifier le rôle critique du cortex pariétal pour l'émergence du sentiment d'intention motrice et -sur la base de processus prédictifs- de la conscience d'agir. Par rapport à ce point, j'ai aussi pu mettre en évidence que le cortex prémoteur était impliqué, à travers un contrôle continu des prédictions pariétales, dans l'émergence d'une conscience d'agir non plus inférée mais véritable / During the last five decades, the motor system has been widely studied. Yet, little is known about the neural substrate of high-level aspects of movement such as intention and awareness and how these functions are related to low-level movement execution processes. It has been suggested that the parietal cortex and supplementary motor area are involved in generating motor intentions, while premotor cortex may play a role in the emergence of motor awareness. However, the precise mechanisms implemented within each of these areas, the way they interact functionally and the nature of the signals conveyed to primary sensory and motor regions is far from being understood. Furthermore, intention and awareness of movement are also influenced by peripheral information coming from the skin, muscles and joints, and this information must be integrated to produce smooth, accurate and coordinated motor actions. Cortical and subcortical structures such as the primary motor cortex and the cerebellum are known to contain motor maps thought to contribute to motor control, learning and plasticity, but the intrinsic organization of these maps and the nature of their reciprocal relations are still unknown. In this thesis I used Direct Electrical Stimulation in patients undergoing brain surgeries to investigate how multiple motor representations are organized and identify the regions responsible for the emergence of conscious motor intention and awareness. I showed, in particular, the existence of multiple efferent maps within the cerebellum and the precentral gyrus. Furthermore, I identified the critical role of the parietal cortex for the emergence of conscious intention and -based on predictive processes- motor awareness. I also provided evidence that the premotor cortex is involved in "checking" parietal estimations, thus leading to a sense of "veridical awareness"
|
199 |
Präfrontale Hirnoxygenierung während einer Aufgabe zum Arbeitsgedächtnis bei Patienten mit einer unipolaren Depression / Prefrontal brain oxygenation during a working memory task of patients with a unipolar depressionJay, Johanna Tharsilla January 2010 (has links) (PDF)
Patienten mit Depression zeigen typischerweise eine Beeinträchtigung kognitiver Funktionen, vor allem im Bereich der exekutiven Funktionen. Als neuroanatomisches Korrelat konnte den exekutiven Funktionen der präfrontale Kortex zugeordnet werden. In den bisherigen bildgebenden Untersuchungen bei depressiven Patienten konnte vor allem eine Hypofrontalität festgestellt werden. Durch verschiedene neuropsychologische Tests konnten kognitive Defizite vor allem im visuell-räumlichen Arbeitsgedächtnis gezeigt werden. Als neuroanatomisches Korrelat konnte dem Arbeitsgedächtnis der DLPFC zugeordnet werden. Die bisher durchgeführten kombinierten Untersuchungen bei depressiven Patienten lieferten jedoch keine einheitlichen Ergebnisse. Mittelpunkt unserer Untersuchung war es deshalb mittels NIRS während der Durchführung eines Tests für das visuell-räumliche und das objektbezogene Arbeitsgedächtnis sowohl bei einer Patientengruppe mit unipolarer Depression als auch bei einer gesunden Kontrollgruppe die Aktivierungsmuster des präfrontalen Kortex zu ermitteln. Für den Zusammenhang zwischen der Hirnaktivierung und der Schwere der depressiven Erkrankung konnten keine signifikanten Korrelationen gezeigt werden. Dies spricht gegen den „state“-Charakter und für den „trait“-Charakter der Hypofrontalität bei einer depressiven Erkrankung. Die bezüglich der Verhaltensdaten gerechneten Varianzanalysen zeigten eine deutliche Schwierigkeitsabstufung zwischen den drei Bedingungen (OWM>VWM>KON). Der fehlende Interaktionseffekt Gruppe x Bedingung, also eine höhere Reaktionszeit der Patienten während allen Aufgaben und nicht nur während OWM und VWM deutet auf eine allgemeine Verlangsamung im Sinne einer psychomotorischen Verlangsamung hin und nicht wie erwartet auf ein besonderes Defizit im Bereich kognitiver Funktionen. Interaktionseffekte bei den bildgebenden Daten bei gleichzeitig fehlenden Interaktionsnachweisen bei den Verhaltensdaten deuten an, dass die funktionellen Daten unabhängig von den Verhaltensdaten interpretiert werden können. Ein kognitives Defizit für beide Komponenten des visuell-räumlichen Arbeitsgedächtnisses bei Patienten mit einer depressiven Erkrankung zeigt sich in unserer Untersuchung also weniger über die Verhaltensdaten als vielmehr über die verminderte Hirnaktivierung während OWM und VWM. Im Gruppenvergleich konnte in den ROI-Analysen für OWM und VWM wie erwartet ein spezieller Arbeitsgedächtniseffekt gezeigt werden, also eine höhere Aktivierung der Kontrollgruppe speziell für die Arbeitsgedächtnisaufgaben. Es wurde also insgesamt in unserer Untersuchung eine präfrontale Hypoaktivierung bei Patienten mit einer depressiven Erkrankung festgestellt. / Patients suffering from depression typically show an impairment of cognitive functions, especially concerning the executive functions. The pre-frontal cortex was determined to be the neuroanatomical correlate of the executive functions. In previous imaging examinations of patients suffering from depression, a hypofrontality was demonstrated. By using different neuropsychological tests, cognitive deficits, especially for the visual-spatial working memory, could be demonstrated. The DLPFC could be shown to be the neuroanatomical correlate of the working memory. The previous combined examinations of patients suffering from depression had, however, failed to show consistent results. The focus of our examination therefore was to detect the pattern of brain activation of patients with a unipolar depression and healthy controls during a visual-spatial (VWM) and visual-object (OWM) working memory task by using Near-infrared Spectroscopy. Significant correlations concerning the connnection between brain activation and the severity of the depressive disease could not be demonstrated. This favors the “trait”-character rather than the “state”-character of the hypofrontality of a depressive disease. The analyses of variance of the behavioral data showed a clear grading of the difficulties among the three conditions (OWM>VWM>KON). The missing effect of interaction group x condition, meaning higher reaction times of the patients during all tasks and not just during OWM and VWM, implies a general slowing down in terms of a psychomotoric slowing down and not – different from what we had expected- a special deficit in the area of the cognitive functions. The effects of interaction of the imaging data combined with the missing effects of the behavioral data imply that the functional data can be interpreted independently from the behavioral data. In our examination, the cognitive deficit for both components of the visual-spatial working memory of patients with a unipolar disease can be demonstrated to a lesser degree through the behavioral data than through the attenuated brain activation during OWM and VWM. As we expected, in the comparison of the groups a special effect for working memory could be demonstrated in the ROI-analyses for OWM and VWM, meaning a higher activation of the control group, especially for the working memory tasks. Therefore, in general, our examination demonstrated a prefrontal hypoactivation of patients suffering from a depressive disease.
|
200 |
Are there order specific patterns of cortical gyrification and if so why?Pillay, Praneshri 10 December 2008 (has links)
Abstract (for Chapter 2)
Objective: The aim was to test the hypothesis that the order is a significant phylogenetic
grouping in terms of quantifiable gyrification indices. Method: The gyrification index
(GI) was measured from serial sections of the brain of twenty five different mammalian
species, representing the different orders i.e. primates, carnivores, artiodactyls and
rodents. Image J analysis was used to measure the contours of the cerebral cortex and the
GI was calculated using three different methods of analysis i.e. complete vs outer; gyral
vs sulcal and outer vs inner surface contours. The measurements were then computed
against the brain weights of each species within the order. Results: An increasing GI
correlates with an increasing brain weight in all the mammalian orders. Each order has its
own specific allometric patterns that are significantly different from the other orders
examined. The artiodactyls were the mammals with the most gyrencephalic brains, these
species being significantly more gyrencephalic than all other mammals when species of
similar brain weights are compared. The North American beaver has an atypically
lissencephalic brain for its size, differing from the trend for increased gyrencephaly found
in the other rodent species examined. Conclusions: Our results show definite trends and
patterns specific to each order. So it would seem that the order is a significant
phylogenetic grouping in terms of this neural parameter, from which we can predict with
a reasonable degree of certainty, the GI of any species of a particular order, if we know
the brain weight.
Abstract (for Chapter 3)
The mammalian order has proven to be a significant phylogenetic grouping in terms of
gyrification from which we can predict with a reasonable degree of certainty, the GI of
any species of a particular order, if we know the brain weight. We have attempted in the
present study to identify potential causes for gyrification at the class level by
investigating relationships at the level of the order. It appears that clues to the extent and
pattern of gyrification in the different mammalian orders might be related to the bones
that constitute the braincase. The external surface areas of the bones of the cranial vault
of seventeen different mammalian species were measured using a microscribe digitiser.
These values were plotted against brain weight from which we could then calculate
residual values, determining if there was more or less external cranial vault area than
expected for the size of the brain. These residuals were then plotted against the
gyrification indices determined in a previous study for the species examined. Results
indicated that for the primates and artiodactyls the skull may potentially be considered as
a limiting factor on the expansion of the cerebral cortex; however, the carnivore and
rodent orders show conflicting results which suggest that the relative surface area of the
skull appears to have no effect on the quantitative extent of gyrencephaly. These
inconclusive findings suggest that causes contributing to the quantitative extent of
gyrification across mammals may be multifactorial, and more parameters may need to be
included in the analysis to arrive at an answer.
|
Page generated in 0.049 seconds