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Étude de la variation de phase des fimbriae F1651, Pap et CS31A et de l'impact des régulateurs homologues de PapILavoie, Rémi 04 1900 (has links)
Les Escherichia coli pathogènes extra-intestinaux (ExPEC) sont responsables d’une grande variété de maladies. Plus particulièrement, certaines souches ExPEC, du sous-groupe d’E. coli uropathogènes, sont porteuses de fimbriae de type P. Cette famille d’adhésines est soumise à une régulation transcriptionnelle appelée variation de phase; un mécanisme du tout ou rien. Il s’agit d’une compétition entre deux protéines régulatrices : la Dam méthylase et la nucléoprotéine Lrp. Ce mécanisme est aussi soumis à l’influence des régulateurs locaux PapB et PapI, deux régulateurs essentiels. Afin d’étudier PapI et ses homologues ainsi que leur impact sur la variation de phase des fimbriae F1651, Pap et CS31A. Grâce à une fusion chromosomique entre la région régulatrice de clp et les gènes lacZYA, nous avons étudié l’effet, en trans, de PapI et FooI qui ont pu restaurer la variation de phase avec une forte tendance pour la phase OFF. Pour étudier l’action de ces protéines sur foo et pap, nous avons utilisé un système utilisant gfp comme gène rapporteur de l’activité des promoteurs des opérons pap et foo. Cela a permis d’observer la variation de phase au niveau cellulaire par cytométrie en flux et en temps réel par microscopie à fluorescence. Ces expériences ont confirmé que la population de cellules F1651 positives a un phénotype d’expression de F1651 partielle alors que les cellules Pap sont en majorité en phase OFF. PapI et FooI n’ont pas la même influence sur la variation de phase, puisque FooI favorise une plus grande fréquence de variation de phase. / Escherichia coli extra-intestinal pathogenic (ExPEC) are responsible for a wide variety of diseases. Particularly ExPEC strains from the subset called uropathogenic E.coli (UPEC) are carrying fimbriae type P. This adhesin family is subject to transcriptional regulation called phase variation, an all or nothing mechanism. It is a competition between two regulatory proteins: the Dam methylase and the nucleoprotein Lrp. This mechanism is also under the influence of the local regulators PapB and PapI. These two regulators are essential to the phase variation. We therefore sought to investigate PapI and its homologs and their impact on the phase variation of fimbriae F1651, Pap, and CS31A. By means of a chromosomal fusion between the regulatory region of clp gene and lacZYA, we studied the effect in trans of PapI and FooI which could restore the phase variation with a strong tendency to phase OFF. To study the action of PapI and FooI, we used a system with gfp as a reporter gene in operons pap and foo. This allowed the observation of the phase variation at the cellular level by flow cytometry and real-time fluorescence microscopy. These experiments confirmed that the population of F165 positive cells have a partial expression state whereas Pap cells mostly have an OFF expression state. We also confirmed that FooI and PapI do not have the same influence on phase variation and that FooI promotes greater frequency of phase variation.
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Training components of face cognitionDolzycka, Dominika 15 April 2013 (has links)
Gesichterkognition ist eine wichtige Fähigkeit für soziale Interaktionen. Obwohl große interindividuelle Unterschiede in der Gesichterkognition festgestellt wurden, gibt es bisher wenige Bestrebungen, diese Fertigkeit zu trainieren. In den vorliegenden Studien habe ich Trainingsverfahren für das Gesichtergedächtnis und die Geschwindigkeit der Gesichterkognition entwickelt und untersucht, welche auf dem Modell von Wilhelm et al. (2010) beruhen. In Studie 1 wurden Trainingseffekte bei gesunden Probanden mittleren Alters behavioral untersucht. Das Training des Gesichtergedächtnisses zeigte einen Trend zur Leistungsverbesserung in der trainierten Aufgabe. Das Training der Geschwindigkeit der Gesichterkognition verkürzte signifikant die Reaktionszeiten in allen Geschwindigkeitsaufgaben der Gesichterkognition, der Objektkognition sowie der mentalen Geschwindigkeit. Daher wird angenommen, dass das Geschwindigkeitstraining eine allgemeine Fähigkeit, komplexe visuelle Stimuli zu verarbeiten, beeinflusst hat. In Studie 2 wurden nach einem Re-Training die psychophysiologischen Grundlagen der trainingsbedingten Veränderungen untersucht. Das Geschwindigkeitstraining verkürzte zwar die Reaktionszeiten im Verlauf des Re-Trainings, jedoch unterschieden sich die beiden Trainingsgruppen nicht im folgenden Posttest. Die Auswertung der ereigniskorrelierten Potentiale wies auf eine Reduktion der strukturellen Repräsentationen aus dem Langzeitgedächtnis zur Erkennung von Individuen (N250r) durch das Geschwindigkeitstraining und auf eine Verstärkung der semantischen Verarbeitung von bekannten Gesichtern (N400) durch das Gedächtnistraining hin. Die vorliegende Arbeit zeigt die Plastizität der Verarbeitungsgeschwindigkeit für komplexe visuelle Stimuli auf. / Face cognition is a crucial skill for social interaction. Large individual differences in face cognition have been shown for healthy adults, suggesting that there might be a need for improvement, yet training of this ability has seldom been attempted. In the present studies, I developed and tested training procedures for face memory and for speed of face cognition, based on the model developed by Wilhelm et al. (2010). In Study 1, training effects were studied with healthy middle-aged participants at the behavioural level. Both training procedures enhanced performance over the course of the training. For facial speed, this improvement was significant as were the faster reaction times on all tasks for facial speed, for object speed, and for general processing speed. Thus, training of facial speed influenced a more general ability to process complex visual stimuli more quickly. Study 2 was conducted to investigate the psychophysiological underpinnings of training effects after a re-training. The facial speed training enhanced performance over the course of the re-training. In the post-test conducted directly after the re-training, the two groups did not differ in reaction times. Results within event-related components suggested that the facial speed training reduced the contributions of structural representations from long-term memory to identity recognition (N250r) and that face memory training enhanced the semantic processing of familiar faces (N400). This dissertation demonstrates the plasticity of the speed of processing complex visual stimuli. The versatility of the results and the limitations of the studies are discussed along with suggestions for future research.
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Étude de l'influence du récepteur LRP-1 sur le potentiel invasif de cellules tumorales : mesures nanomécaniques et d'adhérence par microscopie à force atomique / Study of the influence of the LRP-1 receptor on the invasive potential of cancer cells : nanomechanical and adhesion measurements by atomic force microscopyLe cigne, Anthony 01 July 2016 (has links)
Le récepteur low-density lipoprotein receptor-related protein 1 (LRP-1) est capable d’internaliser des protéases impliquées dans la progression du cancer, et constitue donc une cible thérapeutique prometteuse. Cependant, LRP-1 peut également réguler certaines protéines membranaires. Son ciblage dans une stratégie de modulation de la protéolyse pourrait donc affecter l’adhésion et la dynamique du cytosquelette. Dans ce travail, nous avons étudié l’influence de l’invalidation de LRP-1 sur des paramètres originaux corrélés au potentiel invasif de cellules cancéreuses par microscopie à force atomique (AFM). Cette invalidation induit des changements dans la dynamique d’adhérence des cellules et dans la morphologie, tels qu’un renforcement des fibres de stress et un étalement plus prononcé, causant une augmentation de la surface et de la circularité cellulaires. L’analyse des propriétés mécaniques par AFM a montré que ces différences sont acccompagnées par une augmentation du module d’Young. De plus, les mesures montrent une diminution globale de la motilité cellulaire et une perturbation de la persistance directionnelle. Une augmentation de la force d’adhésion entre cellules invalidées pour LRP-1 et une bille fonctionnalisée à la gélatine a également été observée. Enfin, nos données de spectroscopie de force enregistrées à l’aide d’une pointe fonctionnalisée par un anticorps anti-sous-unité d’intégrine β1 montrent que l’invalidation de LRP-1 modifie la dynamique des intégrines. Dans leur ensemble, nos résultats montrent que des techniques classiquement utilisées dans l’investigation de cellules cancéreuses peuvent être couplées à l’AFM pour ouvrir l’accès à des paramètres complémentaires, pouvant faciliter la discrimination entre différents degrés de potentiel invasif. / The low-density lipoprotein receptor-related protein 1 (LRP-1) can internalize proteases involved in cancer progression and is thus considered a promising therapeutic target. However, it has been demonstrated that LRP-1 is also able to regulate membrane-anchored proteins. Thus, strategies that target LRP-1 to modulate proteolysis could also affect adhesion and cytoskeleton dynamics. Here, we investigated the effect of LRP-1 silencing on parameters reflecting cancer cells’ invasiveness by atomic force microscopy (AFM). The results show that LRP-1 silencing induces changes in the cells’ adhesion behavior, particularly the dynamics of cell attachment. Clear alterations in morphology, such as more pronounced stress fibers and increased spreading, leading to increased area and circularity, were also observed. The determination of the cells’ mechanical properties by AFM showed that these differences are correlated with an increase in Young’s modulus. Moreover, the measurements show an overall decrease in cell motility and modifications of directional persistence. An overall increase in the adhesion force between the LRP-1-silenced cells and a gelatin-coated bead was also observed. Ultimately, our AFM-based force spectroscopy data, recorded using an antibody directed against the β1 integrin subunit, provide evidence that LRP-1 silencing modifies integrin dynamics. Together, our results show that techniques traditionally used for the investigation of cancer cells can be coupled with AFM to gain access to complementary phenotypic parameters that can help discriminate between specific phenotypes associated with different degrees of invasiveness.
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Étude de la variation de phase des fimbriae F1651, Pap et CS31A et de l'impact des régulateurs homologues de PapILavoie, Rémi 04 1900 (has links)
No description available.
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Experimental studies in brain tumours : with special regard to multidrug resistance and the ErbB-familyAndersson, Ulrika January 2005 (has links)
Primary brain tumours, and especially the most common form malignant gliomas, usually display a pronounced resistance to other treatment modalities when surgery fails to cure. Growth factors, such as EGF and its receptor, frequently amplified and overexpressed in malignant gliomas, and factors associated with multidrug resistance have been suggested to at least partially explain the poor outcome. The aim of this thesis was to characterise factors in primary brain tumours associated with the development of resistance with focus on the epidermal growth factor receptor (ErbB) family, and multidrug resistance (MDR). Influences of irradiation on the expression and activity of P-glycoprotein (Pgp) in malignant gliomas was evaluated. The effects showed that irradiation increased the efflux activity of Pgp in rat brain vascular endothelial cells, but not in glioma cells. In the intracranial BT4C glioma model, Pgp was detected in the capillary endothelium in the tumour tissue but not in glioma cells. Expression of several factors coupled to MDR (Pgp, MRP1, LRP, and MGMT) in primary brain tumours were analysed and correlated to clinical data. In gliomas, Pgp and MRP1 were predominantly observed in capillary endothelium and in scattered tumour cells, whereas LRP occurred only in tumour cells. In meningiomas, expression of the analysed markers was demonstrated in the capillary endothelium, with a higher expression of Pgp and MRP1 in transitional compared to meningothelial meningiomas. A pronounced expression of MGMT was found independently of the histopathological grade or tumour type. Survival analysis indicated a shorter overall survival for patients suffering from low-grade gliomas with high expression of Pgp. To explore the importance of the epidermal growth factor receptor (EGFR), expression levels of the family members (EGFR, ErbB2-4) were analysed and their relations to various clinical parameters were evaluated in gliomas and meningiomas. In gliomas, the highest EGFR expression was observed in high-grade tumours, while ErbB4 expression was most pronounced in low-grade tumours. In meningiomas, expression of EGFR, ErbB2, and ErbB4 was observed in the majority of the tumours. An intriguing observation in low-grade gliomas was a significantly decreased overall survival for patients with high EGFR protein expression. The effects of different time schedules for administration of the selective EGFR inhibitor ZD1839 in relation to irradiation of glioma cells were analysed. The analyses showed a heterogeneity in the cytotoxic effects of ZD1839 between cell lines, and it was obvious that some of the cell lines showed sensitivity to ZD1839 despite no or low expression of EGFR. The study also demonstrated the importance of timing of ZD1839 administration when this agent is combined with irradiation. In conclusion, in order to enhance the efficacy of radiotherapy by various drugs in malignant gliomas it may be essential to inhibit drug efflux activity in endothelial cells and to deliver drugs in an optimal timing in relation to radiotherapy. The heterogeneity in expression of drug resistance markers, as well as the ErbB family reflects the complexity in classification of primary brain tumours, and indicates that subgroups of patients with low-grade gliomas expressing Pgp and EGFR might benefit from more aggressive and individualised treatment.
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Neural Correlates of Speed-Accuracy Tradeoff: An Electrophysiological AnalysisHeitz, Richard Philip 29 March 2007 (has links)
Recent computational models and physiological studies suggest that simple, two-alternative forced-choice decision making can be conceptualized as the gradual accumulation of sensory evidence. Accordingly, information is sampled over time from a sensory stimulus, giving rise to an activation function. A response is emitted when this function reaches a criterion level of activity. Critically, the phenomenon known as speed-accuracy tradeoff (SAT) is modeled as a shift in the response boundaries (criterion). As speed stress increases and criterion is lowered, the information function travels less distance before reaching threshold. This leads to faster overall responses, but also an increase in error rate, given that less information is accumulated. Psychophysiological data using EEG and single-unit recordings from monkey cortex suggest that these accumulator models are biologically plausible. The present work is an effort to strengthen this position. Specifically, it seeks to demonstrate a neural correlate of criterion and demonstrate its relationship to behavior. To do so, subjects performed a letter discrimination paradigm under three levels of speed stress. At the same time, electroencephalogram (EEG) was used to derive a measure known as the lateralized readiness potential, which is known to reflect ongoing motor preparation in motor cortex. In Experiment 1, the amplitude of the LRP was related to speed stress: as subjects were forced to respond more quickly, less information was accumulated before making a response. In other words, criterion lowered. These data are complicated by Experiment 2, which found that there are boundary conditions for this effect to obtain.
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MULTIVARIATE CHARACTERIZATION OF LIGNOCELLULOSIC BIOMASS AND GRAFT MODIFICATION OF NATURAL POLYMERSKRASZNAI, DANIEL 29 February 2012 (has links)
The plant cell wall contains significant quantities of renewable polymers in the form of cellulose, hemicellulose, and lignin. These three renewable polymers have the potential to complement or replace synthetic polymers in a variety of applications. Rapidly determining the quantities of these polysaccharides in lignocellulosic biomass is important yet difficult since plant biomass is recalcitrant and highly variable in composition.
Part of this contribution outlines a novel compositional analysis protocol using infrared spectroscopy and multivariate regression techniques that is rapid and inexpensive. Multivariate regression models based on calibration mixtures can be used to discern between populations of lignocellulosic biomass or to predict cellulose, hemicellulose, and lignin quantities. Thus, the compositional analysis step can be expedited so that other processes, like fractionation of the lignocellulose polymers, can be tuned accordingly to maximize the value of the final product.
Hybrid materials were also generated using a variety of polymerization techniques and post-polymerization modifications. A novel controlled/living radical polymerization initiator was synthesized (2-bromo-2-methylpropane hydrazide) containing a hydrazide functionality that was covalently linked to the reducing-end of dextran. Despite the rapid coupling of the hydrazide- based initiator to the reducing-end of dextran, the instability of the alkyl bromide bond resulted in several unsuccessful attempts at Cu(0)-mediated controlled/living radical polymerization. Recommendations were given to improve the stability of this compound; however, an alternative approach to synthesizing hybrid copolymers was also investigated in parallel.
Hyperbranched polymers were synthesized using commercially available vinyl and divinyl monomers in the presence of a cobalt(II) complex that enabled control over the size, architecture, and mol% of pendant vinyl groups amenable to post-polymerization modification. Modifying the ratio of divinyl monomer to cobalt(II) complex provided a series of hyperbranched polymers with variable morphology and mol% pendant vinyl groups. The pendant vinyl bonds were subsequently converted to amines via thiol additions with cysteamine. These amine functionalized hyperbranched polymers were then used in a subsequent reductive amination reaction with the reducing-end of dextran to produce the amphiphilic core-shell copolymer poly(methyl methacrylate-co-ethylene glycol dimethacrylate)-b-dextran. These amphiphilic copolymers mimicked the colloidal behaviour of conventional block copolymer micelles without requiring difficult syntheses or tedious self-assembly steps. / Thesis (Master, Chemical Engineering) -- Queen's University, 2012-02-28 11:20:01.568
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Comparative Functional Analysis and Identification of Regulatory Control in Gene Networks Using the Leucine-Responsive Regulatory protein and its Regulon as a Model SystemLintner, Robert E. 14 May 2007 (has links)
No description available.
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Électrophysiologie cognitive et motrice du syndrome Gilles de la TouretteThibault, Geneviève January 2009 (has links)
Thèse numérisée par la Division de la gestion de documents et des archives de l'Université de Montréal.
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Électrophysiologie cognitive et motrice du syndrome Gilles de la TouretteThibault, Geneviève January 2009 (has links)
Thèse numérisée par la Division de la gestion de documents et des archives de l'Université de Montréal
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