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331	Évaluation de la pénétration cutanée des ingrédients de systèmes dispersés : utilisation combinée des cellules de diffusion et de la microscopie confocale Raman / Percutaneous penetration evaluation of disperse systeme ingredients via a combination of diffusion cells and confocal Raman microscopy Förster, Matthias 21 December 2010 (has links) L'objet de cette thèse est l'étude de la pénétration des actifs cosmétiques dans la peau. Les axes d'investigation principaux ont concerné l'influence des propriétés physicochimiques des actifs et des ingrédients de la formule sur les mécanismes de pénétration. Les actifs cosmétiques choisis sont le rétinol, actif lipophile, et la caféine, actif hydrophile. Les formulations investiguées sont des émulsions de type huile dans eau, comparées aux solutions de tensioactifs correspondantes. Trois huiles cosmétiques ont été utilisées: Butylène glycol de cocoate, Octyldodecyl myristate et la Paraffine liquide, stabilisées en émulsion avec des tensioactifs ester de polyéthylène glycol (PEG20 et PEG6) possédant des longueurs de chaîne carbonées variables (C8, C12, C18 et C18:1). La pénétration percutanée a été mesurée quantitativement en utilisant la méthode des cellules de diffusion de Franz en fonctionnement statique et dynamique et qualitativement par la microscopie confocale Raman. Avec cette combinaison de techniques analytiques, il est possible, de mesurer la pénétration et d’évaluer l'impact de chaque composant de la formulation sur la pénétration cutanée d'un actif. Une corrélation a pu être établie entre l’effet fluidifiant d’une huile et l’augmentation de la pénétration du rétinol. Par ailleurs les tensioactifs, même s’ils ont montré un effet moindre en terme de fluidification conduisent également à une augmentation de la pénétration en raison d’une variation du coefficient de partage de l’actif entre la formule et la peau. Concernant la caféine, l’influence de la structure des tensioactifs et en particulier de la longueur de chaîne carbonée a été mise en évidence / The purpose of this thesis is to study the penetration of cosmetics actives into the skin. The main lines of investigation concerned the influence of actives and formulation components physicochemical properties on the penetration mechanisms. The selected cosmetic actives are retinol, lipophilic, and caffeine, hydrophilic. The investigated formulations are oil in water emulsions, compared to their corresponding surfactant solutions. Three cosmetic oils were used: Butylene glycol cocoate, Octyldodecyl myristate and liquid paraffin. Emulsions are stabilized with polyethylene glycol ester surfactants (PEG20 and PEG6) having variable carbon chain lengths (C8, C12, C18 and C18: 1). Percutaneous penetration was measured quantitatively using Franz diffusion cells in a static and dynamic way and qualitatively by confocal Raman microscopy. With this combination of analytical techniques, it is possible to measure the penetration and evaluate the impact of each formulation component on skin penetration of an active. A correlation could be established between the fluidizing effect of an oil and the increase in retinol penetration. Moreover, the surfactants, although they showed less effect in terms of fluidizing also lead to an increase in penetration due to a variation of the active partition coefficient between the formula and the skin. Regarding caffeine, the influence of the surfactant structure and in particular the carbon chain length has been pointed out Confocal Raman microscopie Peau Pénétration cutanée Rétinol Caféine Émulsion Esters de polyéthylène glycol Cellules de Franz Confocal Raman microscopy Skin Cutaneous penetration Retinol Caffeine Emulsion Polyethylene glycol ester Franz cells 612.79
332	Efeitos dos inibidores de NF Kappa-B e Rho Quinase em um modelo de asma animal: comparação com o tratamento com corticosteroides / Effects of NFkB and rho-quinase inhibitors in an animal asthma model: comparison to corticosteroid treatment Flávia Castro Ribas de Souza 15 December 2017 (has links) Embora a grande maioria dos pacientes com asma tenha controle com o padrão de tratamento com corticosteroides, 5 a 10% destes asmáticos ainda desenvolvem algumas formas graves da doença e são considerados pacientes difíceis de controlar. A ativação do NFkB contribui para a manutenção e desenvolvimento de inflamação pulmonar crônica na fisiopatologia da asma. O éster fenetilico do ácido cafeico (CAPE), um componente ativo de própolis das colmeias de abelhas, é conhecido por ter propriedades antiinflamatórias e imunomoduladoras. É conhecido como um potente e um inibidor específico da ativação de NFk B. Nós anteriormente mostramos que Y27632, um inibidor de Rho quinase, atenuou a resposta pulmonar das vias aéreas, inflamação e remodelamento. Para o nosso conhecimento, tratamentos com os inibidores de NFk B ou Rho-quinase em comparação com o uso de corticosteroides não foram previamente investigados em um modelo animal de inflamação pulmonar crônica alérgica. MÉTODOS: Trinta camundongos BALB/C machos (20 a 25g) foram divididos em cinco grupos (n=6 em cada grupo): SAL (instilado com solução salina), OVA (expostos à ovalbumina), OVA-CAPE (expostos à ovalbumina e tratados com CAPE), OVA-RHO (expostos à ovalbumina e tratados com inibidor de Rho), OVA-CORT (expostos à ovalbumina e tratados com corticosteróide). Os animais foram sensibilizados para ovalbumina durante 28 dias e os controles receberam solução salina. A administração de corticosteróide (1mg/Kg/dia) e CAPE (10mg/Kg/dia) foi feita por via intraperitoneal e Y-27632 (10 mg/kg) administrado por via intranasal, todos nos dias 22, 24, 26 e 28 do protocolo experimental. Vinte e quatro horas após a conclusão do protocolo experimental, os animais foram submetidos a uma avaliação da curva de resposta à dose à metacolina, consideramos as respostas máximas da Resistência ao Sistema Respiratório (Rrs) e Elastância (Ers) às 24 horas após o último desafio com ovalbumina (respostas basais e máximas após a metacolina desafio 3, 30 e 300mg/mL). Posteriormente, os pulmões foram removidos e a análise histológica foi realizada usando morfometria. RESULTADOS: não houve diferenças nos valores basais de todos os grupos. expostos à ovalbumina Houve um aumento em Rrs e Ers após o desafio da metacolina em comparação com o grupo SAL (p < 0,05). No grupo exposto ao OVA, os tratamentos com CAPE, CORT e RHO reduziram a resposta máxima de Ers em relação ao OVA (p < 0,05). Em relação ao tratamento com somente CAPE atenuou a resposta máxima de Rrs em relação ao OVA (p < 0,05). Houve diminuição nos eosinófilos, conteúdo de fibras de colágeno, células positivas para iNOS, MMP-9, TIMP-1 em grupos OVA-CAPE, OVA-CORT e OVA-RHO em comparação com os animais sensibilizados (grupo OVA) (p < 0,05). CONCLUSÃO: a inibição de NFkB e Rho-quinase contribuiu para o controle da hiperresponsividade, inflamação, processo de remodelamento da matriz extracelular e ativação do estresse oxidativo. Embora os inibidores de NFkB e Rho-quinase sejam uma alternativa ao tratamento da asma, são necessários mais estudos / Although the great majority of asthma patients obtain control with the gold standard treatment using corticosteroids, 5 to 10% of these asthmatics still develop some severe forms of the disease, called difficult to control patients. Activation of NFk B contributes to the maintenance and development of chronic lung inflammation in pathophysiology of asthma. Caffeic acid phenethyl ester (CAPE), an active component of propolis from honeybee hives, is known to have anti-inflammatory and immunomodulatory properties. It is known as a potent and a specific inhibitor of NFk B activation. We previously have shown that Y27632, a Rho-quinase inhibitor, attenuated airway lung responsiveness, inflammation and remodeling. To our knowledge, treatments with the NFk B or Rho-kinase inhibitors compared to the use of corticosteroids have not been previously investigated in an animal model of chronic allergic lung inflammation. METHODS: Thirty male BALB/c mice (20 to 25g) were divided into five groups (n=6 in each group): SAL (saline-instilled), OVA (exposed-ovalbumin), OVA-CAPE (exposedovalbumin and treated with CAPE), OVA-RHO (exposed-ovalbumin and treated with Rho inhibitor), OVA-CORT (exposed-ovalbumin and treated with corticosteroid). The BALB/c mice were sensitized to ovalbumin for 28 days and controls received saline. The administration of corticosteroid (1mg/Kg/day) and CAPE (10mg/Kg/day) was made intraperitoneally and Y-27632 (10mg/kg) was intranasally, all on days 22, 24, 26 and 28 of the experimental protocol. Twentyfour hours after completion of the experimental protocol, animals were subject to an evaluation of dose response curve to methacholine. We considered the maximal responses of respiratory system resistance (Rrs) and elastance (Ers) 24 hours after the last challenge with ovalbumin (baseline and maximal responses after metacholine challenge 3, 30 and 300mg/mL). Afterwards, lungs were removed and histological analysis was performed using morphometry. RESULTS: There were no differences on baseline values of all groups. Ovalbumin-exposed mice had an increase in Rrs and Ers after methacholine challenge compared to SAL group (p < 0.05). In OVA-exposed groups, the treatments with CAPE, CORT and RHO reduced maximal response of %Ers compared to OVA (p < 0.05). In relation to %Rrs only CAPE treatment attenuated the maximal response compared to OVA (p < 0.05). There was a decrease in eosinophils, collagen fibers content, iNOS, MMP-9, TIMP-1 positive cells in OVACAPE, OVA-CORT and OVA-RHO groups compared to only sensitized animals (OVA group) (p < 0.05). CONCLUSION: NFkB and Rho-quinase inhibition contributes to the control of hyperresponsiveness, inflammation, extracellular matrix remodeling process and oxidative stress activation. Although NFkB and Rho-quinase inhibitors were an alternative to asthma treatment, more studies are needed Asma Camundongos Corticosteroides Éster fenetilico do ácido cafeico Quinases associadas a rho Remodelação das vias aéreas Adrenal cortex hormones Airway remodeling Asthma Caffeic acid phenethyl ester Mice Rho-associated kinases
333	De la dose à l'effet clinique : utilisation de la modélisation dans les différentes étapes du processus de prédiction du critère clinique : Exemple avec un nouveau médicament en prévention secondaire de la morbidité-mortalité cardiovasculaire / From dose to clinical effect : use of modeling through drug development to predict clinical benefit : Example of a new drug in secondary prevention of coronary heart disease Hourcade-Potelleret, Florence 15 November 2012 (has links) Les données épidémiologiques montrent une association inverse entre les taux de HDL-cholestérol (HDL-C) et le risque d'évènements cardiovasculaires. Des traitements ayant montré une augmentation significative du HDL-C, comme les inhibiteurs de la protéine de transfert des esters de cholestérol, devraient donc permettre de réduire le risque cardio-vasculaire. En utilisant différentes techniques de modélisation, nous avons tenté de quantifier l'efficacité attendue sur les événements cardiovasculaires de l'un d'entre eux, le dalcétrapib, ne disposant que de données pharmacocinétiques et pharmacodynamiques. Tout d’abord, afin d'établir la relation pharmacocinétique / pharmacodynamique entre les concentrations et la modification de HDL-C, nous avons analysé les données individuelles des patients dyslipidémiques par une approche de population. Une hausse moyenne de HDL-C de 26.4 % par rapport au placebo était alors anticipée. Nous avons ensuite tenté de corréler l'effet observé sur l'HDL-C et l'effet clinique à partir de données d'autres études par méta-régression des essais évaluant l'effet des principaux hypolipémiants en prévention secondaire. Cette modélisation n'a pas permis de montrer de corrélation entre le changement de l’HDL-C (P5 P95 :-3.0 et 36 %) et la réduction du risque cardiovasculaire. Une analyse de sensibilité par type de traitement suggère qu'une même hausse de HDL-C entre deux classes thérapeutiques pourrait se traduire par un effet clinique dissemblable, indiquant que HDL-C ne peut pas être utilisé comme critère intermédiaire puisqu'il ne serait pas un prédicteur indépendant du risque cardiovasculaire / Epidemiological data demonstrate an inverse correlation between HDL-cholesterol (HDL-C) levels and cardiovascular risk. Therefore, drugs as cholesteryl ester transfer protein (CETP) inhibitors that lead to a significant HDL-C increase are believed to reduce the occurrence of coronary events. We aimed to evaluate the clinical efficacy of one CETP inhibitor, dalcetrapib, by using various modeling techniques while only pharmacokinetic (PK) and pharmacodynamlc (PD) data were available. First, we analyzed individual data from dyslipidemic patients using a population approach in order to establish the PK/PD relationship between dalcetrapib concentrations and HDL-C change. The results show that an average raise of 26.4 % is expected in comparison to placebo with the 5th (P5) and 95th (P95) percentile of the mean average at 20.7 % and 31.9 % respectively. The increase in HDL-C is explained by a delayed catabolism following the transfer inhibition of cholesterol ester from HDL to Apo-B rich lipoproteins. We endeavored then to correlate HDL-C increase to coronary events by using a meta-regression analysis on randomized trials that evaluated the clinical efficacy of main dyslipidemic drugs on coronary events in secondary prevention. The modeling did not show a statistical association between HDL-C change (P5-P95:-3.0 and 36 %) and coronary risk reduction. A sensitivity analysis by drug class suggests that the same HDL-C increase resulting from different mechanisms of action may not impact the cardiovascular risk in the same way. This would indicate that HDL-C could not be used as a risk marker since it might not be an independent predictor of cardiovascular risk Maladie d'artère coronaire Méta-analyse Inhibiteurs de l'HMG-Coa réductase Acides fibriques Acides nicotiniques Pharmacocinétique Pharmacodynamique Cholesterol ester transfer proteins Coronary artery disease Meta-analysis Fibric acids Nicotinic acids Pharmacokinetics Pharmacodynamics
334	Wear and friction torque in thrust ball and roller bearings lubricated with "windmill gear oils" Marinho, Albano Manuel Gonçalves January 2011 (has links) Tese de mestrado integrado. Engenharia Mecânica. Faculdade de Engenharia. Universidade do Porto. 2011 Transmissões mecânicas Consumo energético Produtos biodegradáveis Óleo mineral Óleo pao Óleo ester Ferrografia analítica Ferrografia de leitura direta Análise das partículas de desgaste Óleos lubrificantes Lubrificação elastohidrodinâmica
335	Recherche et évaluation d'antalgiques originaux : les activateurs des canaux potassiques TREK-1 Rodrigues, Nuno 02 December 2011 (has links) Les antalgiques utilisés aujourd’hui sont des produits anciens et plusieurs d’entre eux datent du 19ème siècle. La morphine demeure l’antalgique de référence pour les douleurs dites par excès de nociception, mais elle est à l’origine d’effets indésirables gênants et graves. Il a été démontré que l’effet antalgique de la morphine passait par l’activation des canaux potassiques TREK-1. Les travaux de recherche ont donc comme objectif la recherche d’antalgiques originaux activateurs de TREK-1. Nous avons synthétisé des activateurs de TREK-1 décrits dans la littérature puis nous avons évalué leur activité antalgique in vivo (writhing test) ce qui nous a permis d’identifier le CDC comme molécule « lead ». Nous avons ensuite synthétisé 43 analogues du CDC que nous avons évalué pour leur effet antalgique ainsi que leur capacité à activer les canaux TREK-1 (électrophysiologie). Ces molécules ont été préparées en 3 à 12 étapes avec des rendements de 3 à 72 % en utilisant des réactions telles que : aldolisation, oléfination de Watsworth et Horner, Peterson, estérification …Des résultats très prometteurs ont émergé de cette étude de relation structure-activité avec 8 molécules qui se démarquent avec un très bon effet antalgique (>50% inhibition de la douleur) ainsi qu’une bonne activation des canaux TREK-1 (R>2). Enfin nous avons analysé les résultats de cette étude par modélisation moléculaire (QSAR) ce qui nous a permis d’identifier les caractéristiques structurales essentielles de ces molécules. / Analgesics used today are old products and several of them date from the 19th century. Morphine remains the analgesics of reference for pains called by excess of nociception, but it is at the origin of awkward and serious side effects. It was shown that the analgesic effect of morphine passed by the activation of potassium channels TREK-1. The objective of this work is thus to develop original analgesics, activators of TREK-1. We synthesized activators of TREK-1 described in the literature and we evaluated their analgesic activity in vivo (writhing test) which enabled us to identify CDC as a lead molecule. We then synthesized 43 analogues of CDC which we evaluated for their analgesic effect and their ability to activate TREK-1 channels (electrophysiology). These molecules were prepared in 3 to 12 steps with yields ranging from 3 to 72 % by using reactions such as : aldol reaction, Watsworth and Horner’s olefination, Peterson’s olefination, esterification … Very promising results emerged from this structure-activity relationship study with 8 molecules which display a very good analgesic effect (>50% inhibition of pain) as well as a good activation of TREK-1 channels (R> 2). Finally we analyzed the results of this study by molecular modeling (QSAR) which enabled us to identify the essential structural characteristics of these molecules. Douleur Antalgiques Canaux potassiques TREK-1 CDC Dérivé d’ester caféique Aldolisation Oléfination QSAR Writhing test Électrophysiologie Pain Analgesics Potassium channels TREK-1 CDC Analogues of caffeic ester Aldol reaction Olefination QSAR Writhing test Electrophysiology
336	Application de la LIF de molécules aromatiques au dosage de carburants fossiles et biocarburants Ledier, Constantin 13 December 2011 (has links) (PDF) Les industries automobile et aéronautique sont confrontées dans le futur proche à une raréfaction des carburants fossiles, ainsi qu'au problème de pollution de l'environnement émis par les systèmes propulsifs. Pour s'affranchir de ces problèmes, l'utilisation de carburants alternatifs censés apporter rendement et préservation de l'environnement, s'est considérablement développée ces derniers temps. Cependant, leurs impacts sur la pollution, consommation et rendement de combustion ne sont toujours pas clairement établis. En particulier, il est nécessaire de quantifier leurs effets sur les phénomènes physiques clés à la base des processus que sont l'évaporation du carburant liquide et le mélange carburant vapeur/air. L'analyse expérimentale de ces processus physiques nécessite alors l'emploi de diagnostics lasers non-intrusifs et quantitatifs, permettant de mesurer des grandeurs physiques comme les distributions spatiales instantanées de température et de concentration du carburant en phase vapeur. Parmi les techniques optiques les plus attrayantes, l'imagerie de fluorescence induite par laser (PLIF) offre de nombreux avantages. L'objectif de la thèse a été, dans un premier temps, de caractériser les propriétés spectroscopiques de quatre carburants multi-composants, le kérosène (Jet A1), le Biomass-to-Liquid (BtL), le Diesel et l'Ester Méthylique Huile Végétale (EMHV) qui, mis à part le premier, possèdent des propriétés spectroscopiques encore peu connues. L'exploitation de leurs propriétés de fluorescence a ensuite permis d'évaluer leurs capacités à fournir des signaux autorisant la mesure de la température et de la concentration du carburant en phase vapeur. Dans un second temps, un étude exhaustive des propriétés de fluorescence de plusieurs cétones (3-pentanone, benzophénone) et aromatiques (fluoranthène, acénaphtène, naphtalène, 1,2,4-triméthylbenzène...) en fonction de la température et du quenching de l'oxygène moléculaire, a été réalisée à pression atmosphérique pour identifier les traceurs fluorescents potentiellement adaptés au dosage optique des quatre carburants. Les données photophysiques collectées ont ensuite été utilisées pour parfaire l'établissement des couples carburants/traceurs fluorescents ainsi que les stratégies de mesures de température et de concentration de carburant associées. L'exploitation des données acquises lors de différentes campagnes de mesures a ainsi mis en évidence la possibilité de détecter simultanément la fluorescence de plusieurs molécules aromatiques (mono-, di- et/ou tri-aromatique) naturellement présentes ou ajoutées artificiellement dans les carburants. Le cas du Diesel a nécessité le développement d'un carburant modèle pour permettre une étude de son évaporation. L'application de cette nouvelle approche PLIF a été validée sur un injecteur hélicoptère LPP de nouvelle génération fonctionnant avec trois carburants spécifiques que sont le Jet A1, le BtL et un mélange Jet A1/BtL Diagnostic laser Spectroscopie Fluorescence induite par laser Aromatiques Biocarburants Carburants fossiles Jet A1 Diesel Biomass-to-liquid Ester PLIF Système d'injection LPP Température Concentration Quenching Oxygène moléculaire Pression atmosphérique
337	Transition Metal Mediated Transformations of Carboranes Eriksson, Ludvig January 2003 (has links) <p>This thesis describes the use of copper and palladium to mediate transformations of carboranes, especially <i>p</i>-carborane.</p><p>1-(1-<i>p</i>-carboranyl)-<i>N</i>-methyl-<i>N</i>-(2-butyl)-3-isoquinolinecarboxamide, a carborane containing analogue of the peripheral benzodiazepine receptor (PBR) ligand PK11195, has been synthesised. A key step in the reaction is the copper (I) mediated coupling of p-carborane with ethyl 1-bromo-isoquinoline-3-carboxylate. </p><p><i>p</i>-Carborane has been arylated on the 2-<i>B</i>-atom in high yields, using the Suzuki–Miyaura reaction. Thus the reaction between 2-I-<i>p</i>-carborane and various arylboronic acids [1-naphthyl-, phenyl-, 4-MeO-C<sub>6</sub>H<sub>4</sub>-, 3-CH<sub>3</sub>CONH-C<sub>6</sub>H<sub>4</sub>-, 4-NC-C<sub>6</sub>H<sub>4</sub>-, 3-NO<sub>2</sub>-C<sub>6</sub>H<sub>4</sub>-], gave the corresponding 2-aryl-<i>p</i>-carboranes in DME solution when reacted in the presence of cesium fluoride and the catalytic Pd<sub>2</sub>(dba)<sub>3</sub>–dppb system. Under the same conditions, the boron-boron bond forming reaction of two <i>p</i>-carboranylboronic esters (2-[(pinacolato)boron]-<i>p</i>-carborane and 2-[(neopentyl glycolato)boron]-p-carborane) was also shown feasible.</p><p><i>p</i>-Carborane has been vinylated on the 2-<i>B</i>-atom in high yields by use of the Heck reaction. The coupling between 2-I-<i>p</i>-carborane and various styrenes [4-H-, 4-C<sub>6</sub>H<sub>4</sub>-, 4-Cl , 4-Br-, 4-NO<sub>2</sub>-, 4-CH3O- and 4 CH<sub>3</sub> ] resulted in the formation of the corresponding<i>trans</i>-β-(2-<i>B</i>-<i>p</i>-carboranyl) styrene in DMF solution when reacted in the presence of silver phosphate and the palladacycle Herrmann´s catalyst. The reaction was shown to proceed at higher rate with electron rich than with electron deficient olefins.</p><p>The feasibility of palladium-catalysed isotopic exchange of an iodinated closo-carborane with a radioisotope of iodine has been studied. 2-I-<i>p</i>-carborane was selected as a model compound. It was shown, that such isotopic exchange is possible and provides a high yield (83 ± 4.2 %) during 40 min long reaction. The reaction conditions were optimised, and it was demonstrated that presence of the tetra n-butylammonium hydrogensulphate is important in order to stabilise catalyst and provide reproducibility of labelling. In this work we have modified the methodology and extended the application to a wider range of iodinated carboranes. By the use of Herrmann’s catalyst in toluene at 100 °C this [<sup>125</sup>I]-iodide labelling could be improved and extended. 2-I-<i>p</i>- 9-I-<i>m</i>-, 9-I-<i>o</i>-, 3-I-<i>o</i>-carborane, 1-phenyl-3-I-<i>o</i>-carborane and 1,2-diphenyl-3-I-<i>o</i>-carborane could be [<sup>125</sup>I]-iodide labelled in high to excellent yields within 5 minutes.This reported palladium catalyzed radio-iodination of the uncharged closo-carboranes might find use in pharmacokinetic studies of carborane derivatives.</p> Chemistry carborane isoquinoline PK11195 peripheral bensodiazepine receptor Cu (I) Iodide iodinated carborane palladium isotopic exchange Herrmann’s Catalyst Heck reaction Suzuki-Miyaura reaction cross coupling arylation olefination 125-iodine radiolabelling carboraneboronic ester BNCT 2-iodo- Kemi Chemistry Kemi
338	Lichtinduzierte Generierung von optisch anisotropen Filmen auf der Basis von multi-funktionalen Polymeren Rosenhauer, Regina January 2004 (has links) Gegenstand der Arbeit ist die lichtinduzierte Orientierung von multifunktionalen Polymeren, die u.a. für die Herstellung von optischen Schichten in Flüssigkristalldisplays verwendet werden können. Dafür wurden Polymere entwickelt, die wenigstens eine mesogene und eine lichtsensitive Gruppe enthalten. Diese Gruppen zeigen Eigenschaften, die für die Orientierung der kompletten Polymerfilme verantwortlich sind. Das Material wird dafür zunächst in einem ersten Schritt kurz mit linear polarisiertem Licht bestrahlt, wobei richtungsabhängig eine photochemische Reaktion an der lichtsensitiven Gruppe erfolgt und dadurch ein "Orientierungskeim" gelegt wird. Durch die thermische Ausrichtung der mesogenen Gruppen an den photochemisch generierten "Orientierungskeimen" erfolgt die komplette Orientierung des Filmes in einem zweiten Schritt. Dadurch wird eine hohe optische Anisotropie erhalten. Dieses Verfahren wurde als Zwei-Stufen-Bulk-Orientierungsprozess bezeichnet. <br><br> In der vorliegenden Arbeit wurden die Photoreaktionen verschiedener lichtsensitiver Gruppen, wie z. B. Azobenzen, Stilben und Zimtsäureester und deren Orientierungsfähigkeit in flüssigkristallinen Polymeren untersucht. Der Orientierungsprozess wurde durch die Wahl geeigneter Bestrahlungsbedingungen optimiert. Die Effizienz der Orientierung wurde anhand der sich verändernden winkelabhängigen Absorptionseigenschaften und der Doppelbrechung des Materials analysiert. Es wurde gezeigt, dass eine effiziente lichtinduzierte Orientierung bei einer Vielzahl von flüssigkristallinen Polymeren realisierbar ist. So wurde z. B. erstmalig gefunden, dass durch eine Photo-Fries-Orientierung eine hohe optische Anisotropie erhalten werden kann. Außerdem wurde eine neue lichtsensitive Gruppe auf der Basis von Donor-Akzeptor-substituiertem Ethen entwickelt, die farbneutral ist und durch polarisiertes UV-Licht sowohl orientiert als auch re-orientiert werden kann. <br><br> Es wurden weiterhin Polymere entwickelt, die zusätzlich zu den photosensitiven und flüssigkristallinen Einheiten, fluoreszierende Gruppen enthalten. Die Auswahl geeigneter Fluoreszenzverbindungen erfolgte aufgrund ihrer anisometrischen Form, ihrer Ordnungsparameter in einer niedermolekularen Flüssigkristallmischung und ihrer Photostabilität. Das Orientierungsverhalten von ausgewählten Fluorophoren wurde in sechs Ter- und zwei Copolymeren untersucht. Das Prinzip der Orientierung beruht auf einer kooperativen Ausrichtung der Seitengruppen. Aus diesem Grund kommt dem Nachweis der Kooperativität in der vorliegenden Arbeit eine besondere Stellung zu. <br><br> Durch lichtinduzierte Bulk-Orientierung wurden Filme erhalten, welche durch eine richtungsabhängige Fluoreszenz und Absorption im sichtbaren- oder UV-Bereich charakterisiert sind. Die Fluoreszenz wird durch einige lichtsensitive Verbindungen komplett gelöscht. Die wahlweise erhaltenen anisotropen Filme von farbigen, fluoreszierenden oder farbneutralen Verbindungen, die zudem in kleinen Pixeln von wenigen Mikrometern orientiert werden können, eröffnen vielfältige Möglichkeiten für den Einsatz von multi-funktionalen Polymeren als optische Schichten in Flüssigkristalldisplays. / The work presents the light-induced orientation of multifunctional polymers, which can be used for the preparation of optical films in liquid crystal displays (LCDs). Polymers which contain at least one mesogenic and one photosensitive side group were developed for this approach. The side groups of the specially designed polymers show properties which allow for the orientation of the whole polymer film. Isotropic films of the polymeric material were shortly irradiated with linearly polarised light in a first step. So, a photochemical reaction on the light-sensitive group takes place and results in the generation of "orientational seeds". The complete orientation of the polymer film takes place applying a secondary thermal step which aligns the mesogenic groups near to these "orientational seeds". In this way highly anisotropic films are generated. This method was called two-step-bulk-orientation process. <br><br> The photoreaction of different light-sensitive groups, such as azobenzene, stilbene, cinnamic ester and their ability to orient liquid crystalline polymers were investigated in this thesis. The orientation process was optimised using suitable irradiation conditions. The efficiency of the orientation was analysed measuring the angular dependent absorbance and the birefringence of the material due to the ordering procedure. It was shown, that a light-induced orientation is practicable in a high amount of different liquid crystalline polymers. So, for the first time it was found, that the generation of a high optical anisotropy is achieved as result of the rearrangement of the Photo-Fries-Reaction. Moreover, a new light-sensitive group based on donor-acceptor substituted ethylene was developed, which is colourless and allow the orientation and reorientation using polarised UV light. <br><br> Moreover, polymers were developed, which contain fluorescent groups in addition to the photo-sensitive and mesogenic units. The selection of suitable fluorophores was carried out with respect to their anisometric shape, their order parameter in a low molecular liquid crystalline mixture and their photostability. The orientational behaviour of selected fluorophores in six terpolymers and in two copolymers were investigated. The principle of the ordering is based on the cooperative orientation of the side groups. In this way the verification of the cooperativity of the process plays an important role in this work. <br><br> It was shown, that films can be fabricated by means of the light-induced bulk-orientation, which is characterised by an angular selective fluorescence and absorption in the UV or visible region. The fluorescence was completely quenched by some light-sensitive groups. In this way the anisotropic films became optional coloured, fluorescent or colourless and can be patterned in small anisotropic pixels of some micrometers. So, the developed multifunctional materials and the ordering method open new possibilities for the generation of different types of optical films in LCDs. multifunktionale Polymere Anisotropie Chemistry and allied sciences
339	Structure-Property Relationships of Surfactants at Interfaces and Polyelectrolyte-Surfactant Aggregates Kjellin, Mikael January 2002 (has links) The first part of this thesis is concerned with thestructure-property relationships in nonionic surfactantsystems. The main aim was to investigate how the surfactantstructure influences the adsorption at interfaces andinteractions between surfactant coated interfaces.Particularly, the effect of the structure of the surfactantheadgroups was investigated. These were sugar-based headgroupwith varying size and flexibility and poly(ethylene oxide)based headgroups with or without an additional amide or estergroup. The hydrophobic part of the surfactant consisted mostlyof straight alkyl chains, except for one type of poly(ethyleneoxide) based surfactant with a dehydroabietic hydrophobe. The main technique that was used is the surface forcetechnique, with which the forces acting between two adsorbedsurfactant layers on hydrophilic or hydrophobic surfaces can bemeasured. These forces are important for e.g. the stability ofdispersions. The hydrophilic surfaces employed were glass andmica, whereas the hydrophobic surfaces were silanized glass andhydrophobized mica. The adsorption behavior on hydrophilicsurfaces is highly dependent on the type of headgroup andsurface, whereas similar results were obtained on the two typesof hydrophobic surfaces. To better understand how the surfaceforces are affected by the surfactant structure, measurementsof adsorbed amount and theoretical mean-field latticecalculations were carried out. The results show that the sugarsurfactant layers and poly(ethylene oxide) surfactant layersgive rise to very different surface forces, but that the forcesare more similar within each group. The structure-propertyrelationships for many other physical properties have beenstudied as well. These include equilibrium and dynamicadsorption at the liquid-vapor interface, micelle size, micelledynamics, and wetting. The second part in this thesis is about the aggregationbetween cationic polyelectrolytes and an anionic surfactant.The surface force technique was used to study the adsorption ofa low charged cationic polyelectrolyte on mica, and theaggregation between the adsorbed polyelectrolyte with theanionic surfactant. The aggregation in bulk was studied withturbidimetry, small angle neutron scattering (SANS), and smallangle x-ray scattering (SAXS). An internal hexagonal aggregatestructure was found for some of the bulk aggregates. <b>Keywords:</b>nonionic surfactant, sugar surfactant,poly(ethylene oxide), amide, ester, polyelectrolyte, SDS,hydrophobic surface, glass surface, mica, adsorption,aggregation, micelle size, surface forces, wetting, dynamicsurface tension, NMR, TRFQ, SANS, SAXS, mean-field latticecalculations. nonionic surfactant sugar surfactant poly(ethylene oxide) amide ester polyelectrolyte SDS hydrophobic surface glass surface mica adsorption aggregation micelle size surface forces wetting dynamic surface tension NMR TRFQ SANS SAXS,
340	Transition Metal Mediated Transformations of Carboranes Eriksson, Ludvig January 2003 (has links) This thesis describes the use of copper and palladium to mediate transformations of carboranes, especially p-carborane. 1-(1-p-carboranyl)-N-methyl-N-(2-butyl)-3-isoquinolinecarboxamide, a carborane containing analogue of the peripheral benzodiazepine receptor (PBR) ligand PK11195, has been synthesised. A key step in the reaction is the copper (I) mediated coupling of p-carborane with ethyl 1-bromo-isoquinoline-3-carboxylate. p-Carborane has been arylated on the 2-B-atom in high yields, using the Suzuki–Miyaura reaction. Thus the reaction between 2-I-p-carborane and various arylboronic acids [1-naphthyl-, phenyl-, 4-MeO-C6H4-, 3-CH3CONH-C6H4-, 4-NC-C6H4-, 3-NO2-C6H4-], gave the corresponding 2-aryl-p-carboranes in DME solution when reacted in the presence of cesium fluoride and the catalytic Pd2(dba)3–dppb system. Under the same conditions, the boron-boron bond forming reaction of two p-carboranylboronic esters (2-[(pinacolato)boron]-p-carborane and 2-[(neopentyl glycolato)boron]-p-carborane) was also shown feasible. p-Carborane has been vinylated on the 2-B-atom in high yields by use of the Heck reaction. The coupling between 2-I-p-carborane and various styrenes [4-H-, 4-C6H4-, 4-Cl , 4-Br-, 4-NO2-, 4-CH3O- and 4 CH3 ] resulted in the formation of the correspondingtrans-β-(2-B-p-carboranyl) styrene in DMF solution when reacted in the presence of silver phosphate and the palladacycle Herrmann´s catalyst. The reaction was shown to proceed at higher rate with electron rich than with electron deficient olefins. The feasibility of palladium-catalysed isotopic exchange of an iodinated closo-carborane with a radioisotope of iodine has been studied. 2-I-p-carborane was selected as a model compound. It was shown, that such isotopic exchange is possible and provides a high yield (83 ± 4.2 %) during 40 min long reaction. The reaction conditions were optimised, and it was demonstrated that presence of the tetra n-butylammonium hydrogensulphate is important in order to stabilise catalyst and provide reproducibility of labelling. In this work we have modified the methodology and extended the application to a wider range of iodinated carboranes. By the use of Herrmann’s catalyst in toluene at 100 °C this [125I]-iodide labelling could be improved and extended. 2-I-p- 9-I-m-, 9-I-o-, 3-I-o-carborane, 1-phenyl-3-I-o-carborane and 1,2-diphenyl-3-I-o-carborane could be [125I]-iodide labelled in high to excellent yields within 5 minutes.This reported palladium catalyzed radio-iodination of the uncharged closo-carboranes might find use in pharmacokinetic studies of carborane derivatives. Chemistry carborane isoquinoline PK11195 peripheral bensodiazepine receptor Cu (I) Iodide iodinated carborane palladium isotopic exchange Herrmann’s Catalyst Heck reaction Suzuki-Miyaura reaction cross coupling arylation olefination 125-iodine radiolabelling carboraneboronic ester BNCT 2-iodo- Kemi Chemistry Kemi

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