Dissertations / Theses on the topic 'Declarative; Functional'

Thesis (Ph. D.)--University of California, San Diego, 2006.
Title from first page of PDF file (viewed May 18, 2006). Available via ProQuest Digital Dissertations. Vita. Includes bibliographical references (p. 125-138).

The Edinburgh High Risk Study recruited 162 young adults with at least one first or second degree relative with schizophrenia and 43 closely matched controls. A broad neuropsychological (NP) and clinical assessment battery was administered every 18-24 months over 10 years, while participants underwent between 1 and 3 functional magnetic resonance imaging (fMRI) scans during a verbal memory and executive function task over 5 years. Methods: Baseline predictors of schizophrenia, performance changes over 2 NP assessments, and the influence of genetic liability were examined in high risk participants with (HR+) and without psychotic symptoms (HR-), those who are now ill (Scz) and controls (C ), using one-way ANOVAs and repeated measures ANCOVAs. Aspects of verbal and non-verbal memory were also compared between the HR and C in the first 100 participants to undergo an fMRI scan using one-way ANOVAs. In the same participants, differences between groups in blood oxygen level dependent (BOLD) fMRI brain responses during an event related verbal encoding (word classification) and retrieval task were investigated using fixed and random effects general linear models. Results: On a test of verbal learning at baseline, Scz performed significantly less well than HR. However, there were no significant interactions of time by group, and HR showed stable impairments relative to C on immediate and delayed prose recall, delayed list recall and response suppression across both assessments before and after controlling for IQ. Measures of genetic liability were inversely correlated with delayed prose recall over time. HR showed poorer cued delayed recall, and less word retention between short and long delay recall trials on a verbal learning test. A visual recognition test also significantly discriminated between HR and C. Behavioural analysis of the fMRI verbal memory task revealed no differences between groups in reaction time or accuracy. However, during encoding there was a greater BOLD response in the right inferior frontal lobe (BA45/44) in HR relative to C, and in the right inferior parietal lobule (BA7/40) in HR+ relative to C and HR-. During correct recognition compared to correct rejection responses there was a greater bilateral cerebellar and left inferior frontal response in HR relative to C, and an increased thalamus response in HR-relative to HR+. Conclusions: Stable differences in NP performance over time suggest a trait deficit, which is relatively unaffected by the presence of psychotic symptoms and schizophrenia onset, although small numbers might be have been precluded detection significant time by group interactions. Poorer verbal memory performance overall in Scz suggests that this deficit is more pronounced in those who go on to develop schizophrenia. Non-verbal learning impairments reflect encoding deficits, while verbal learning impairments reflect encoding and retention difficulties in the HR group.

La Polarité Cellulaire Planaire (PCP) est une voie de signalisation originellement identifiée chez les invertébrés pour son rôle dans l’établissement d’une asymétrie cellulaire perpendiculaire à l’axe apico‐basal. Elle définit une polarité dans le plan d’un épithélium et coordonne cette polarité dans tout l'épithélium. L'activation de la voie PCP conduit à une réorganisation ducyto squelette en passant par une modulation des zones d'adhésion, régulant ainsi la forme et les mouvements des cellules. La voie de signalisation de la PCP est conservée tout au long de l'évolution jusqu'au mammifères, et contrôle la morphogénèse de divers tissus dont les tissus épithéliaux et mésenchymateux, ainsi que pour les tissues cardiaques, osseux, pulmonaire ou encore rénaux, mais aussi le système nerveux pour n'en citer que quelques‐uns.Afin d'identifier le rôle de vangl2, un des gènes centraux de la PCP, dans la mise en place de la circuiterie hippocampale, nous avons créé un modèle murin où vangl2 est supprimé de façon conditionnelle (cKO) dans le télencéphale à des stades précoces de l’embryogénèse. J’ai d'abord montré que Vangl2 est enrichi dans les neurones immatures de la zone sous granulaire du DG, ainsi que dans l’arborisation des neurites (axones et dendrites) des cellules granulaires (CG) du gyrus denté (DG) de l’hippocampe. Ainsi, Vangl2 est enrichi dans le stratum lucidum (sl), une région dense en contacts synaptiques entre le DG et le CA3. Dans cette région a lieu une synapse très particulière entre l'axone des CG, la fibre moussue (Mf) qui forme des boutons géants (MfB) et les excroissances épineuse (TE) issues de la partie proximale des dendrites apicaux. L'analyse structurale et ultra structurale de ces épines démontre que l'élargissement et la complexification de la synapse MfB/TE est bloquée dans nos mutants, alors que les zones actives (PSD) des épines sont présentes, mais réorganisées. De façon intéressante,dans une zone plus distale des dendrites des neurones du CA3 (sl), les épines sont, elles, plus grosses, suggérant un remodelage complexe du réseau en l'absence de vangl2. Enfin, j’ai pu montrer que ces défauts morphologiques étaient corrélés à des problèmes de mémoire complexe (mémoire déclarative) qui dépendent de l’hippocampe mais aussi du cortex. Cette étude montre pour la première fois l’importance du signal PCP dans maturation in vivo d’un circuit hippocampique spécifique ainsi que ces conséquences cognitives. D'autres résultats in vitro montrent que la suppression de vangl2 augmente la vitesse de déplacement des cônes de croissance sur des substrats de N‐cadhérine. J’ai utilisé la microscopie en super résolution spt‐PALM‐TIRF pour montrer que cette augmentation de croissance est inversement proportionnelle à la vitesse du flux rétrograde d’actine. Des expériences de FRAP permettent de suggérer que les molécules de N‐cadhérine engagées dans des interactions hémophiliques (adhésion) est plus importante dans les mutants vangl2 Je propose que Vangl2 contrôle le recyclage et la stabilité des protéines N‐cadhérine dans les sites d’adhésion afin de réguler localement les dynamiques d’actine et par conséquent la croissance neuronale
Planar Cell Polarity (PCP) is a signaling pathway originally known for its role in the establishment of cellular asymmetry perpendicular to the apico‐basal axis, in the plane of an epithelium. PCPsignaling has been shown to be crucial for many tissue patterning, including epithelial and mesenchymal tissue, but also cardiac, lung, bone, or kidney tissues, to cite a few. PCP signaling controls the regulation of cellular movement via the control of adhesion turnover and cytoskeleton reorganization. Vangl2 is one of the most upstream core PCP proteins that has been implicated in the recent years in various neuronal mechanisms, such as axonal guidance, dendrite morphogenesis or synaptogenesis. However, most of these studies rely on acute downregulation of the gene in vitro or in the use of a mouse presenting a spontaneous mutation of this gene, called Loop‐tail (Vangl2Lp) which causes the death of the embryo at birth. Moreover, the Vangl2Lp form of this protein has been described has a dominant‐negative form, making it difficult to untangle the molecular mechanism leading to the many phenotypes (included neuronal ones) reported inhomozygotes Looptail mice. To bypass this problem we created a conditional knockout (cKO) mouse in which vangl2 is deleted in the telencephalon during early embryogenesis. First, I analyzed the profile of expression of the protein during the first 3 weeks after birth, and I show that Vangl2 is specifically targeted to the arborization of granular cells (GC) of the dentate gyrus (DG) of the hippocampus, and excluded from cell bodies. Also, the protein was highly enriched in immature neurons of the subgranular zone of the DG, and in the stratum lucidum, a region of high‐density contacts between the GC and the CA3. In this region, a special type of synapse is formed: the Mossy Fiber Bouton (MfB) / Thorny Excrescence (TE) synapse. These synapses are bigger and more complex than conventional synapses. I then performed a structural and ultrastructural analysis of the DG/CA3 circuit in the Vangl2 cKO mice in order to understand the role of Vangl2 in the hippocampus maturation. For this, I used stereotaxic mice infection viruses, and Serial block face scanning electron microscopy (SBFsEM) with 3D reconstruction. Results show that in cKO mice, Mfs fasciculation is mildly impacted, and that the enlargement and complexification of the MfB/TE synapse is arrested, with TEs almost absent. I was able to link these morphological abnormalities to deficits in complex hippocampal‐dependent learning tasks. This work demonstrates for the first time the importance of PCP signaling for the in vivo maturation of a specific hippocampal circuit and its specific cognitive consequences. Next, I attempted to identify the functional consequences of vangl2 deletion on young hippocampal neuron maturation. My results confirm that Vangl2 is expressed in young hippocampal neurons and that the deletion of the gene affected neurite outgrowth on Ncadherin substrate. I used spt‐PALM‐TIRF super‐resolution microscopy to show that this increased neurite outgrowth was inversely proportional to a decrease in actin retrograde flowand to a decrease in the number of directed actin trajectories. These results strongly suggest that N‐cadherin adhesions are affected by Vangl2 deletion. FRAP experiments demonstratedthat in Vangl2 cKO neurons the recovery of N‐cadherin molecules engaged in homophilicbindings (adhesion) was decreased, suggesting that the turnover of N‐cadherin involved inadhesion is reduced. Altogether, I propose that Vangl2 controls the turnover/stability of Ncadherin proteins at adhesion sites to regulate local actin dynamics and consequently neuronal outgrowth

Recent research, that has been focused on recognition memory, has revealed that two processes contribute to recognition of previously encountered items: recollection and familiarity (Aggleton & Brown, 1999; Eichenbaum, 2006; Eichenbaum, Yonelinas, & Ranganath, 2007; Rugg & Yonelinas, 2003; Skinner & Fernandes, 2007; Squire, Stark, & Clark, 2004; Wixted, 2007a; Yonelinas, 2001a; Yonelinas, 2002). The findings of neural correlates of recollection and familiarity lead to the assumption that there are different brain regions activated in either process, but there are, to the best of my knowledge, no studies assessing how these brain regions are working together in a recollection or a familiarity network, respectively. Additionally, there are almost no studies to date, which directly searched for overlapping regions. Therefore, in study I of the current thesis, brain regions associated to both recognition processes are searched investigated. Additionally, a connectivity analysis will search for functional correlated brain activations that either build a recollection or a familiarity network. It is undoubtable that the Brain Derived Neurotrophic Factor (BDNF) is strongly involved in synaptic plasticity in the hippocampus (Bramham & Messaoudi, 2005) and there is evidence that a genetic variant of this neurotrophin (BDNF 66Met) is related to poorer memory performance (Egan, et al., 2003). Therefore, in study II of the current thesis, the effect of BDNF Val66Met on recollection and familiarity performance and related brain activations is investigated. Finally, one could summarize, that serotonin, like BDNF, is strongly involved in brain development and plasticity as well as in learning and memory processes (Vizi, 2008). More precisely, there is evidence for alterations in the structure of brain regions, which are known to be involved in emotional memory formation and retrieval, like amygdala and hippocampus (Frodl, et al., 2008; Munafo, Brown, & Hariri, 2008; Pezawas, et al., 2005). One study found an slight epistatic effect of BDNF and 5-HTTLPR on the grey matter volume of the amygdala (Pezawas, et al., 2008). Therefore, in study III, it is investigated if such an interaction effect could be substantiated for the amygdala and additionally revealed for the hippocampus. The results of the current thesis allow further comprehension of recollection, hence episodic memory, and point to a special role of the BDNF in temporal and prefrontal brain regions. Additionally, the finding of an epistatic effect between BDNF and serotonin transporter function point to the need of analyzing interactions between genes and also between genes and environmental factors which reveals more information than the study of main effects alone. In conclusion, analyzing behavioral and neural correlates of episodic memory reveal allowed insights in brain functions that may serve as guideline for future studies in clinical populations with memory deficits, including susceptibility factors such as good or bad environment, as well as promising gene variants that influence episodic memory.

This thesis aimed to examine the effects of glucose drink administration on sensorimotor function (studies 1 - 3) and declarative memory (study 4). Glucose had no effect on a modified version of the Hick task in study 1. However in study 2 we observed that glucose slowed reaction times (RTs) during the initial performance of the Eriksen flanker task. One possible reason for this effect is that glucose only slows sensorimotor function when a response is weakly associated with a stimulus, such as at the beginning of task performance. In study 1 stimulus-response (S-R) associations may have been too strong to observe a glucose slowing effect. Here participants performed a greater number of training trials and stimuli were arguably mapped more directly to a response compared to study 2. In study 3 we tested the hypothesis that glucose slows sensorimotor function when S-R associations are weak. Here we used a letter version of the Eriksen flanker task and kept S-R association consistently low by changing the stimulus set to a novel pair of letters every 80 trials. We found that glucose constantly slowed RTs for the duration of this task, a result which is congruent with the hypothesis that glucose slows sensorimotor function when S-R associations are weak. In study 4 we focused on the effects of glucose administration on declarative memory function and sought to determine whether glucose affected the encoding of stimuli in a word recognition task. Here we used ERPs as an online measure of encoding processes. Our findings were that glucose enhanced recognition performance, replicating the well established effect that glucose- facilitates declarative memory. Furthermore, during encoding, glucose affected ERP components associated with early sensory processing, visual word-form generation, lexical/semantic access and long-term memory encoding/consolidation. Furthermore there was a correlation between recognition performance and the degree to which glucose amplified the N400 component, an ERP potential associated with lexical/semantic access. The results of this study therefore indicate that glucose modulates encoding processes and that these effects may, at least partially, underlie the glucose facilitation of declarative memory.

This paper concerns itself with possibilities of declarative programming in the new version of Java 8 language, specifically using elements adopted from the domain of functional programming languages: function as a value and lazy streams of data. The goal of this paper is to demonstrate possibilities of declarative programming using these elements, analyze its implementation and design own extensions. The contribution lies particularly in showing possibilities of the new elements, implementation analysis and design of a new functionality. The output can be used by a Czech reader, who is at least slightly advanced in the field of information technologies. The paper is divided into a theoretical and practical parts. Theoretical part is covered by chapters 3-8. Theoretical part describes motivation for introduction of the new elements, describes functional programming and its basic principles, then it shows basic principles of the newly introducted elements and ends with the description of the java.util.stream package. Pactical part is covered by chapters 9 and 10. Practical part concerns with stream oper-ations and extension design of existing functionality.

Les fonctions cognitives reposent sur la communication dynamique de régions cérébrales interconnectées. Dans la maladie d’Alzheimer (MA), les travaux antérieurs suggèrent que le processus neuropathologique cible de façon précoce un ou plusieurs systèmes anatomo-fonctionnels spécifiques. La dysfonction du réseau par défaut a été objectivée de façon consistante. Cependant, ses relations avec les symptômes cliniques et avec l’atteinte des régions du lobe temporal interne qui lui sont fonctionnellement connectées restent à clarifier. L’IRM fonctionnelle de repos est une technique pertinente pour caractériser in vivo chez l’Homme la connectivité cérébrale.Par une approche des systèmes neuraux, ce travail de thèse a pour objectif de caractériser la réorganisation fonctionnelle neuronale dans la MA, ses corrélats cliniques, ainsi que l’influence de l’âge de début des symptômes. Par le recueil et l’analyse des données neuropsychologiques, en IRMf de repos et en IRM structurale, acquises chez des sujets avec des troubles de la mémoire et avec une forme mnésique légère de MA, notre travail apporte des éclairages : i) sur l’implication du réseau temporal antérieur dans la mémoire déclarative décontextualisée et ses modifications dans le cours de la MA ; ii) sur les similitudes et spécificités des systèmes anatomo-fonctionnels ciblés dans les deux formes cliniques distinctes - à début précoce et tardif - de la MA ; iii) sur la réorganisation de l’organisation topologique cérébrale dans son ensemble de ces deux formes de la maladie
Cognitive functions rely on the dynamic interplay of connected brain regions. Previous studies suggest that in Alzheimer disease (AD), early pathological changes target one or several specific anatomo-functional networks. Dysfunction of the default mode network is a consistent finding. However, its relationship with clinical symptoms and interconnected medial temporal regions remains to be clarified. Resting state functional MRI (fMRI) is an emerging method aimed at characterizing in vivo brain connectivity in the Human.Using a neural system approach, the aim of this thesis was to characterize neuronal functional reorganization in AD, its clinical correlates, and to determine the influence of age at onset. Neuropsychological data, structural and fMRI were obtained in subjects with early memory impairment and mild “amnestic” AD. This work provides new insights into : i) the functional role of the anterior temporal network in context-free declarative memory and its changes throughout the course of AD; ii) the common and specific features in targeted anatomo-functional networks between early and late onset AD ; iii) the reorganization of whole brain topological properties in the two forms of the disease

Les problèmes d’optimisation combinatoire sont devenus la cible de nombreuses recherches scientifiques pour leur importance dans la résolution de problèmes académiques et de problèmes réels rencontrés dans le domaine de l’ingénierie et dans l’industrie. La résolution de ces problèmes par des méthodes exactes ne peut être envisagée à cause des délais de traitement souvent exorbitants que nécessiteraient ces méthodes pour atteindre la (les) solution(s) optimale(s). Dans cette thèse, nous nous sommes intéressés au contexte algorithmique de résolution des problèmes combinatoires, et au contexte de modélisation de ces problèmes. Au niveau algorithmique, nous avons appréhendé les méthodes hybrides qui excellent par leur capacité à faire coopérer les méthodes exactes et les méthodes approchées afin de produire rapidement des solutions. Au niveau modélisation, nous avons travaillé sur la spécification et la résolution exacte des problématiques complexes de fouille des ensembles de motifs en étudiant tout particulièrement le passage à l’échelle sur des bases de données de grande taille. D'une part, nous avons proposé une première parallélisation de l'algorithme DGVNS, appelée CPDGVNS, qui explore en parallèle les différents clusters fournis par la décomposition arborescente en partageant la meilleure solution trouvée sur un modèle maître-travailleur. Deux autres stratégies, appelées RADGVNS et RSDGVNS, ont été proposées qui améliorent la fréquence d'échange des solutions intermédiaires entre les différents processus. Les expérimentations effectuées sur des problèmes combinatoires difficiles montrent l'adéquation et l'efficacité de nos méthodes parallèles. D'autre part, nous avons proposé une approche hybride combinant à la fois les techniques de programmation linéaire en nombres entiers (PLNE) et la fouille de motifs. Notre approche est complète et tire profit du cadre général de la PLNE (en procurant un haut niveau de flexibilité et d’expressivité) et des heuristiques spécialisées pour l’exploration et l’extraction de données (pour améliorer les temps de calcul). Outre le cadre général de l’extraction des ensembles de motifs, nous avons étudié plus particulièrement deux problèmes : le clustering conceptuel et le problème de tuilage (tiling). Les expérimentations menées ont montré l’apport de notre proposition par rapport aux approches à base de contraintes et aux heuristiques spécialisées
Combinatorial optimization problems have become the target of many scientific researches for their importance in solving academic problems and real problems encountered in the field of engineering and industry. Solving these problems by exact methods is often intractable because of the exorbitant time processing that these methods would require to reach the optimal solution(s). In this thesis, we were interested in the algorithmic context of solving combinatorial problems, and the modeling context of these problems. At the algorithmic level, we have explored the hybrid methods which excel in their ability to cooperate exact methods and approximate methods in order to produce rapidly solutions of best quality. At the modeling level, we worked on the specification and the exact resolution of complex problems in pattern set mining, in particular, by studying scaling issues in large databases. On the one hand, we proposed a first parallelization of the DGVNS algorithm, called CPDGVNS, which explores in parallel the different clusters of the tree decomposition by sharing the best overall solution on a master-worker model. Two other strategies, called RADGVNS and RSDGVNS, have been proposed which improve the frequency of exchanging intermediate solutions between the different processes. Experiments carried out on difficult combinatorial problems show the effectiveness of our parallel methods. On the other hand, we proposed a hybrid approach combining techniques of both Integer Linear Programming (ILP) and pattern mining. Our approach is comprehensive and takes advantage of the general ILP framework (by providing a high level of flexibility and expressiveness) and specialized heuristics for data mining (to improve computing time). In addition to the general framework for the pattern set mining, two problems were studied: conceptual clustering and the tiling problem. The experiments carried out showed the contribution of our proposition in relation to constraint-based approaches and specialized heuristics

Recent research, that has been focused on recognition memory, has revealed that two processes contribute to recognition of previously encountered items: recollection and familiarity (Aggleton & Brown, 1999; Eichenbaum, 2006; Eichenbaum, Yonelinas, & Ranganath, 2007; Rugg & Yonelinas, 2003; Skinner & Fernandes, 2007; Squire, Stark, & Clark, 2004; Wixted, 2007a; Yonelinas, 2001a; Yonelinas, 2002). The findings of neural correlates of recollection and familiarity lead to the assumption that there are different brain regions activated in either process, but there are, to the best of my knowledge, no studies assessing how these brain regions are working together in a recollection or a familiarity network, respectively. Additionally, there are almost no studies to date, which directly searched for overlapping regions. Therefore, in study I of the current thesis, brain regions associated to both recognition processes are searched investigated. Additionally, a connectivity analysis will search for functional correlated brain activations that either build a recollection or a familiarity network. It is undoubtable that the Brain Derived Neurotrophic Factor (BDNF) is strongly involved in synaptic plasticity in the hippocampus (Bramham & Messaoudi, 2005) and there is evidence that a genetic variant of this neurotrophin (BDNF 66Met) is related to poorer memory performance (Egan, et al., 2003). Therefore, in study II of the current thesis, the effect of BDNF Val66Met on recollection and familiarity performance and related brain activations is investigated. Finally, one could summarize, that serotonin, like BDNF, is strongly involved in brain development and plasticity as well as in learning and memory processes (Vizi, 2008). More precisely, there is evidence for alterations in the structure of brain regions, which are known to be involved in emotional memory formation and retrieval, like amygdala and hippocampus (Frodl, et al., 2008; Munafo, Brown, & Hariri, 2008; Pezawas, et al., 2005). One study found an slight epistatic effect of BDNF and 5-HTTLPR on the grey matter volume of the amygdala (Pezawas, et al., 2008). Therefore, in study III, it is investigated if such an interaction effect could be substantiated for the amygdala and additionally revealed for the hippocampus. The results of the current thesis allow further comprehension of recollection, hence episodic memory, and point to a special role of the BDNF in temporal and prefrontal brain regions. Additionally, the finding of an epistatic effect between BDNF and serotonin transporter function point to the need of analyzing interactions between genes and also between genes and environmental factors which reveals more information than the study of main effects alone. In conclusion, analyzing behavioral and neural correlates of episodic memory reveal allowed insights in brain functions that may serve as guideline for future studies in clinical populations with memory deficits, including susceptibility factors such as good or bad environment, as well as promising gene variants that influence episodic memory.

В диссертации рассматриваются механизмы перепроектирования деятельности таможенного поста в условиях особой экономической зоны. Применение метода организационного моделирования и функционального анализа позволило автору разработать новую организационную архитектуру Верхнесалдинского таможенного поста в условиях особой экономической зоны «Титановая долина». Реализация проекта реорганизации Верхнесалдинского таможенного поста оптимизирует управленческие процессы таможенной деятельности и ставит управление самой особой эконмической зоны на более высокий уровень реализации региональных инвестиционных проектов.
The thesis deals with mechanisms of re-projecting a customs office within the special economic zone. The author develops new organizational architecture for Vyerkhnyaya Salda customs office within the Titan Valley special economic zone, applying the methods of organizational modelling and functional analysis. Realizing the reorganizational project for Vyerkhnyaya Salda customs office optimizes the administrative process in the customs activity and brings up the special economic zone administration to a higher level of realizing the regional investment projects.

A bill of Exchange was originally used as payment instrument. Recently, it is mostly used as securing instrument. This purpose was mainly evolved by legal practice and its legislation could be problematic and unclear for laymen. The main aim of this thesis is to analyze a bill of exchange as a securing instrument. Further attention is paid to the function of payment. However, the bill of exchange and check are both regulated in identical law, so to some of its institutes I also describe a checks. The main attention of my thesis is devoted to the securing purpose of the bill of exchange. There I describe the specifics of this instrument in the comparison of other civil securing instruments. Due to this contrast, it can be said, that the bill of exchange gives the creditor some significant advantage on one hand, but finds some insuperable limits on the other hand. My thesis is divided into five chapters. The first chapter describes the historical development of bills of exchange and check, and the circumstances under which these institutions were created. The second chapter deals with the exchange and check law, their rules, the systematic inclusion of this branch of law and the basic peculiarities are defined. The third chapter is devoted to a general definition of the bill of exchange, describes...