Global ETD Search

111	Formation and electrolysis of disubstituted alkali-metal amides Korn, Gerhard Gunter 26 April 2010 (has links) The purpose of this investigation was to determine the products of the electrolysis of dimethyl lithium amide. / Master of Science LD5655.V855 1955.K676 Amides Electrochemical analysis Electrolysis
112	Structural studies of titanium(IV) picolinamide alkoxide and oxide derivatives Lord, Rianne M., Lord, S.M., Pask, C.M., McGowan, P.C. 27 April 2016 (has links) Yes / Reactions have been carried out using the titanium(IV) precursors TiCl4 and Ti(OiPr)4, with addition of two equivalents of a functionalized picolinamide ligand. The reactions with TiCl4 led to the formation of either a mononuclear titanium species, [Ti(N,O)Cl2X2] or a dinuclear titanium species [Ti(N,O)X3]2[l- O] (X = OMe or Cl), with incorporation of one picolinamide ligand. The ligand is bound to the titanium centre as the protonated amide. The reactions with Ti(OiPr)4 resulted in the formation of mononuclear titanium bis-picolinamide species [Ti(N,O)2(OiPr)2], and also dinuclear and trinuclear products, [(N,O)Ti (OiPr)2][l-OiPr]2 and [(N,O)Ti(OiPr)2]2[l-OiPr]2[(OiPr)2Ti][l3-O] respectively. In these cases the picolinamide ligand was found to be deprotonated and bound to the titanium as the iminolate. These molecules have been characterized by X-ray crystallographic analysis and structural characteristics are discussed. Titanium Amides Iminolates Isopropoxide Catalysis Titanium(IV) picolinamide alkoxide Structure
113	Total synthesis of eucophylline : a free-radical approach towards total synthesis of cytotoxic leucophyllidine / Synthèse totale de l'eucophylline : approches radicalaires vers la synthèse totale de la leucophyllidine Hassan, Haitham 23 September 2016 (has links) La thèse décrit la première synthèse totale de l'Eucophylline, le fragment sud de l'alcaloïde Leucophyllidine récemment isolé à partir de Leuconotisgriffithii et L. eugenifolius. La synthèse en 10 étapes comprend une nouvelle méthode d’accès au squelette azabicyclo[3.3.1]nonane par un processus de carbooximation radicalaire d'oléfines à trois composants. Au cours de ces études, nous avons également isolé des énamines présentant des stabilités inhabituelles résultant de leur conformation bicyclique tendue. La synthèse de la partie éburnane, le fragment nord de la Leucophyllidine, a été réalisée grâce à une nouvelle réaction radicalaire de carbo-cyanation à trois composants. Cette réaction radicalaire s'est révélée efficace pour installer le groupement fonctionnel nitrile sur des oléfines, et éventuellement former des centres quaternaires, notamment dans des structures complexes, puisqu'une bonne tolérance aux différents groupes fonctionnels a été observée. Le couplage biomimétique entre le squelette éburnane et l'Eucophylline a finalement été étudié en utilisant des modèles de structure similaire. Les résultats préliminaires de cette étude ont montré que l'absence d'effet gem-diméthyle dans le modèle éburnane empêche probablement la formation de l'imine cyclique,intermédiaire-clé dans le couplage désiré. / The thesis describes the first total synthesis of Eucophylline, the south fragment of the Leucophyllidine alkaloid recently isolated from Leuconotis griffithiiand L. eugenifolius. The 10-step synthesis encompasses a new straight forward method to access to the azabicyclo[3.3.1]nonane skeleton through a free-radical three-component olefinic carbo-oximation process. During these studies, we also isolated enamines exhibiting unusual stabilities resulting from their strained bicyclicconformation. The synthesis of the Eburnane part, the north fragment of Leucophyllidine, was developed relying on a new free-radical three-component Carbo-Cyanation reaction. This new reaction showed high tolerance toward different functional groups and provided an efficient mean to install the nitrile group in complex structures and to introduce quaternary centers. The biomimetic coupling between the Eburnane and Eucophylline fragments was finally studied using structurally similar models. Preliminary results of this model study showed that absence of a gemdimethyleffect in the Eburnane model probably prevents the formation of the cyclicimine, key intermediate for the desired coupling. Eucophylline Synthèse totale Alcaloïdes bisindoliques Carbocyanation Amides contraints Eucophylline Total synthesis Bisindole alkaloids Carbo-Cyanation Twisted amides
114	Utilisation des propriétés des N-alkoxyamides pour la synthèse de γ- et δ- lactames hautement fonctionnalisés par des processus domino / Use of the N-alkoxy amide properties in domino reactions for the synthesis of highly functionalized γ- and δ-lactams Champetter, Philippe 22 December 2017 (has links) Les hétérocycles azotés occupent une place importante en chimie organique et médicinale et, à ce titre, constituent des cibles de choix pour le développement de réactions toujours plus efficaces et faciles d’emploi. Les travaux antérieurs, réalisés au laboratoire URCOM sur l’accès aux γ-lactames, ont servi de base pour développer une méthodologie impliquant des conditions douces qui ont mis en évidence les propriétés spécifiques des N-alkoxy amides pour accéder aux γ- et δ-lactames hautement fonctionnalisés de manière hautement diastéréosélective selon un processus domino. Cette méthodologie a aussi pu être étendue aux hydantoïnes, 2-imino-thiazolidin-4-ones et thiazinan-4-ones qui constituent également des molécules étudiées en chimie médicinale. En parallèle, une comparaison de réactivité entre N-alkoxy amides et N-alkyl amides a montré la meilleure réactivité des composés N-alkoxylés pour l’obtention de ces différents hétérocycles azotés. Cette différence de réactivité a été attribuée à la possible chélation du contre anion alcalins des bases minérales utilisées dans notre approche par les N-alkoxy amides. Les conditions douces ont permis d’envisager des versions organocatalysées énantiosélectives ou multicomposantes des réactions précédentes conduisant à des résultats préliminaires intéressants. / Nitrogen-containing heterocycles are key compounds in organic and medicinal chemistry and continue to attract synthetic effort for the development of more efficient and convenient reaction. Previous work carried out at the URCOM laboratory for the access to γ-lactams has provided the basis for developing a highly diastereoselective methodology under mild conditions that has demonstrated the specific properties of N-alkoxy amides, allowing the access to γ- and δ-lactams following a domino process. This methodology also allowed the access to hydantoïns, 2-imino thiazolidin-4-ones and thiazinan-4-ones which are compounds of importance in medicinal chemistry. In parallel, a comparison of reactivity between N-alkoxy and N-alkyl amides was carried out in order to demonstrate the better reactivity of the N-alkoxy amide compounds. This better reactivity was attributed to a possible chelation of the alkali metal counter anion of the mineral bases used in our conditions by the N-alkoxy amides. These mild conditions allowed organocatalyzed enantioselective or multicomponents approaches providing interesting preliminary results. Hétérocycles azotés Γ- et δ- lactames N-alkoxy amides N-heterocycles Γ- et δ- lactams Domino process N-alkoxy amides Methodology
115	Extended Molecular Mechanics Investigations Of Some Simple Alkyl Amides And Thioamides Ganeshsrinivas, E 11 1900 (has links) (PDF) No description available. Molecular Dynamics Amides - Infrared Spectra Amides Vibrational Frequency Amines Thioamides Molecular Mechanics Acetamide Thioacetamide Thioformamide Organic Chemistry
116	The use of levobupivacaine and ropivacaine in spinal anaesthesia for lower limb and urological surgery. / CUHK electronic theses & dissertations collection January 2011 (has links) I found that 2.6ml of 0.5% levobupivacaine had similar clinical characteristics as the same volume of 0.5% bupivacaine in spinal anaesthesia. Both were effective for spinal anaesthesia in urological surgery, when a sensory block up to at least T10 dermatome was required. In comparing the use of levobupivacaine alone and levobupivacaine with fentanyl, there were no significant differences in haemodynamic changes and quality of sensory and motor block, when 2.6ml of levobupivacaine alone or 2.3ml of levobupivacaine with fentanyl 15mcg (0.3ml) were used in spinal anaesthesia. Both were effective for spinal anaesthesia in urological surgery. In comparing the use of ropivacaine 10mg and bupivacaine 10mg, both with fentanyl 15mcg in spinal anaesthesia for urological surgery, all the patients achieved adequate level of sensory block up to T10 dermatome or higher. The two drugs were similar in the onset time of motor block, the characteristics of sensory block and haemodynamic changes; however, the duration of motor block was shorter with ropivacaine. I concluded that both studied solutions, ropivacaine-fentanyl and bupivacaine-fentanyl, were effective for spinal anaesthesia in urological surgery and the duration of motor block was shorter with the ropivacaine-fentanyl solution. The dose-response relationship of ropivacaine in spinal anaesthesia for lower limb surgery requiring a sensory block up to at least the T12 dermatome was defined. Anaesthesia was successful in 0, 0, 42, 83 and 100% when ropivacaine at doses of 2, 4, 7, 10 and 14mg respectively were given. The derived values for ED50 and ED95 were 7.6mg and 11.4mg respectively. The cephalic level of sensory block and the degree of motor block increased with larger doses of ropivacaine. Finally, the median effective dose (ED50) of bupivacaine, levobupivacaine and ropivacaine in spinal anaesthesia for lower limb surgery were defined as 5.50mg (95% CI: 4.90--6.10mg), 5.68mg (95% CI: 4.92--6.44mg), and 8.41mg (95% CI: 7.15--9.67mg) respectively. The relative potency ratios were 0.97 (95% CI: 0.81--1.17) for levobupivacaine/bupivacaine, 0.65 (95% CI: 0.54--0.80) for ropivacaine/bupivacaine and 0.68 (95% CI: 0.55--0.84) for ropivacainellevobupivacaine. / In this series of studies, I have shown that levobupivacaine and ropivacaine are effective local anaesthetic agents for spinal anaesthesia in lower limb and urological surgery. This proved my hypothesis. Both are suitable alternatives to bupivacaine for spinal anaesthesia. Furthermore, these studies showed that ropivacaine is less potent than levobupivacaine and bupivacaine and the potency is similar between levobupivacaine and bupivacaine at median effective dose. / Levobupivacaine and ropivacaine are two relatively new local anaesthetics which were developed in view of their potential for less cardiotoxicity in comparison with bupivacaine, the most common local anaesthetic used in spinal anaesthesia for many years. Both are produced in pure S(-) enantiomer form in contrast to bupivacaine which is a racemic mixture. They have been shown to be effective in peripheral nerve blocks, and epidural analgesia and anaesthesia; nevertheless, experience of their use in spinal anaesthesia is limited. The objective of this thesis was to evaluate their use in spinal anaesthesia for surgery in non-obstetric patients. My hypothesis was that levobupivacaine and ropivacaine are effective local anaesthetic agents for spinal anaesthesia in lower limb and urological surgery. In order to test this hypothesis, I conducted five clinical studies on 269 patients who had urological surgery or lower limb surgery under spinal or combined spinal-epidural anaesthesia. First, I investigated the efficacy and clinical characteristics of levobupivacaine and the mixture of levobupivacaine with fentanyl in spinal anaesthesia. Next, I compared the use of ropivacaine-fentanyl with bupivacaine-fentanyl in spinal anaesthesia. Finally, I defined the dose-response relationship of ropivacaine in spinal anaesthesia using traditional dose-response methodology and defined the relative potency among levobupivacaine, ropivacaine and bupivacaine by comparing the defined ED50 in spinal anaesthesia using up-down sequential allocation method. / Lee, Ying Yin. / Source: Dissertation Abstracts International, Volume: 73-06, Section: B, page: . / Thesis (M.D.)--Chinese University of Hong Kong, 2011. / Includes bibliographical references (leaves 133-150). / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Electronic reproduction. [Ann Arbor, MI] : ProQuest Information and Learning, [201-] System requirements: Adobe Acrobat Reader. Available via World Wide Web. Amides Genitourinary organs--Surgery Leg--Surgery Spinal anesthesia Amides Anesthesia, Spinal--methods Bupivacaine--analogs & derivatives Lower Extremity--surgery Urologic Diseases--surgery
117	Rôle de la programmation maternelle et du rythme circannuel sur le contrôle neuroendocrine de la physiologie saisonnière / The role of photoperiodic history and internal long‐term timing in seasonal neuroendocrinology Saenz De Miera Patin, Cristina 25 November 2014 (has links) La régulation endogène de la physiologie saisonnière, comme les rythmes circannuels et l’histoire photopériodique vécue pendant la gestation, permet aux individus d’anticiper à l’arrivée des saisons. L’objectif de cette thèse a été l’étude de l’effet de ces deux phénomènes à long terme sur les voies neuroendocrines contrôlant la physiologie saisonnière. Ces études montrent que les rythmes circannuels sont initiés au niveau de l’expression de la thyréostimuline dans la pars tuberalis et celle-ci est transmisse à l’hypothalamus où elle contrôle les niveaux d’hormone thyroïdienne et de neuropeptides. De façon similaire, la photopériode vécue pendant la gestation semble programmer l’expression des déiodinases dans l’hypothalamus des rongeurs adultes. Dans l’ensemble, ces résultats montrent la conservation du rôle de la pars tuberalis en tant que site central pour l’intégration des signaux impliqués dans le contrôle de la physiologie saisonnière. / Internal long-term timing strategies, like circannual rhythms and photoperiodic history, allow changes in physiology in anticipation to the seasons. In this project I investigated the effects of both types of history dependent timing on the neuro endocrine pathways for regulation of seasonal physiology. My work revealed that internal circannual timing is initiated through the control of thyroid stimulating hormone at the pars tuberalis and is integrated into the regulation of hypothalamic thyroid hormone levels and neuropeptides.Similarly, history-dependent expression in hypothalamic deiodinases was observed in adult rodents based on their gestational photoperiodic experience. Overall, my results highlight the pars tuberalis as a conserved central site in mammals for the integration of multiple seasonal cues, which via differential control of thyroid hormone levels in the hypothalamus dictates the timing in seasonal physiology. Saisonnalité Circannuel Programmation maternelle Déiodinases Pars tuberalis RF-amides Seasonality Circannual Maternal programming Deiodinases Pars tuberalis RF-amides 571.8 573.8 612.02
118	New methodologies for the introduction of the SCF3 and Cl groups by C(sp3)-H bond functionalization and the design of original fluorinated electrophilic reagents / Nouvelles méthodologies pour l'introduction des groupements SCF3 et CI par la fonctionnalisation de liaisons C(sp3)-H et l'élaboration de réactifs électrophiles fluorés originaux Xiong, Heng-Ying 22 March 2017 (has links) Le domaine de recherche de la chimie du fluor a connu un essor considérable. En particulier, le motif SCF3 et plus récemment les groupements SCF2R (R = H, SO2Ph, SAr, COAr, Rf) ont fait l'objet d'une attention particulière de la part de la communauté scientifique du fait de leurs propriétés remarquables. Dans ce contexte, le développement de nouvelles méthodologies et de réactifs originaux pour l'introduction de ces groupements fluorés a suscité un fort intérêt. En conséquence, les objectifs de cette thèse ont été 1) de développer de nouvelles méthodologies pour la fonctionnalisation de liaisons C(sp3)-H par l'introduction directe d'un motif SCF3 catalysée par des métaux de transition, et son extension à d'autres groupements fonctionnels ainsi que 2) de concevoir et étudier de nouveaux réactifs fluorés électrophiles. La première partie de cette thèse a été dédiée au développement d'une réaction de trifluorométhylthiolation d'amides aliphatiques catalysée au palladium, une transformation inédite (Chapitre 2). Puis, la chloration d'amides aliphatiques catalysée au palladium, dans des conditions douces, a été étudiée (Chapitre 3). Enfin, une nouvelle voie de synthèse pour accéder aux sulfénamides trifluorométhylés a été développée (Chapitre 4). Cette approche a été étendue à la préparation d'un nouveau réactif électrophile pour l'introduction du groupement SCN. De plus, un réactif électrophile original, source du motif SCF2PO(OEt)2, a été synthétisé et appliqué à la construction de liaisons C-SCF2PO(OEt)2, N-SCF2PO(OEt)2 et S-SCF2PO(OEt)2 ainsi qu'à la synthèse d'un composé d'intérêt biologique (Chapitre 4). / The organofluorine chemistry field has witnessed a very fast expansion. In particular, the SCF3 moiety and more recently the SCF2R groups (R = H, SO2Ph, SAr, COAr, Rf) have attracted a special interest from the scientific community because of their remarkable properties. In this context, the development of new methodologies and original reagents for the introduction of such fluorinated groups is particularly appealing. Therefore, the goals of this thesis were 1) to develop a new methodology for the direct introduction of the SCF3 group by transition metal-catalyzed C(sp3)-H bond functionalization and its extension to other functional groups as well as 2) to design and study new electrophilic fluorinated reagents.The first part of this Ph.D. thesis was dedicated to the development of an unprecedented Pd-catalyzed trifluoromethylthiolation of aliphatic amides by C-H bond functionalization (Chapter 2). Then, the Pd-catalyzed chlorination of aliphatic amides by C-H bond functionalization under mild conditions was investigated (Chapter 3). Finally, a newly designed strategy for the synthesis of trifluoromethanesulfenamides was elaborated (Chapter 4). This approach was extended to the preparation of a new electrophilic reagent for the thiocyanation reaction. In addition, an original electrophilic SCF2PO(OEt)2 reagent was designed and applied to the construction of C-SCF2PO(OEt)2, N-SCF2PO(OEt)2 and S-SCF2PO(OEt)2 bonds as well as to the synthesis of a biorelevant compound (Chapter 4). Fonctionnalisation de liaisons C-H Trifluoromethylthiolation Amides aliphatiques Réactifs électrophiles originaux Réactif de thiocyanation C-H bond functionalization Aliphatic amides Chlorination Original electrophilic reagents Thiocyanating reagent
119	Hypervalent Iodine Reagents in Metal-Free Arylations and Vinylations : Investigation of Suitable Coupling Partners and Synthesis of New Reagents Stridfeldt, Elin January 2017 (has links) This thesis concerns the development of metal-free reactions to obtain carbon-heteroatom and carbon-carbon bonds. This is achieved by transferring carbon ligands from hypervalent iodine reagents to suitable nucleophiles. The bulk of the work presented herein concerns arylation of oxygen and nitrogen nucleophiles, using the well-known diaryliodonium salts as aryl sources. In the first project, O-arylation of the oxime ethyl acetohydroxamate was studied. It was found that electron-poor as well as electron-rich aryl moieties could be transferred successfully to this nucleophile. Furthermore, the protocol could be extended to a sequential one-pot synthesis of benzo[b]furans. This method allowed for a fast synthesis of the natural product stemofuran A and formal syntheses of other natural products. In a successive project, O-arylation of hydroxide and aliphatic alkoxides was investigated. It is known that electron-poor aryl moieties can be transferred to these nucleophiles in moderate to high yields. However, combined with more electron-rich diaryliodonium salts, a large amount of side products were formed. These were suppressed upon addition of aryne traps, suggesting that aryne pathways are competing with the desired ligand coupling. It was also observed that secondary alcohols were oxidized to the corresponding ketones. The mechanism for this oxidation was investigated and aryne pathways could be excluded. Instead we suggest that the carbinol hydrogen gets deprotonated via an internal mechanism, after the alkoxide has coordinated to the iodonium salt. Highly sterically congested alkyl aryl ethers could be obtained in high yields by combining tertiary alcohols with ortho-blocked diaryliodonium salts. Next, N-arylation of secondary acyclic amides was studied using acetanilide as the model substrate. This procedure was suitable for transfer of electron-poor as well as ortho-substituted aryl moieties, but attempts to transfer very electron-rich aryl groups were unsuccessful. On the other hand, the amides displayed a complementary reactivity, allowing phenylation of electron-rich amides. In the final project, a one-pot synthesis of the cyclic iodonium reagent vinylbenziodoxolone is presented. These compounds have not been explored as reagents earlier. Initial screenings showed that the vinyl moiety could be transferred to nitrocyclohexane with opposite regioselectivity compared to the acyclic analogue of the reagent. / <p>At the time of the doctoral defense, the following paper was unpublished and had a status as follows: Paper 2: Manuscript.</p> Diaryliodonium Salts Benzofurans Aryl Ethers Secondary Amides Vinylbenziodoxolones Organic Chemistry Organisk kemi
120	Design, Synthesis and Glioblastoma Activity of 1,3-Diazinane Based Aryl Amides and Benzo Fused Heterocycles Hron, Rebecca 19 May 2017 (has links) The development of novel targeted therapeutics for the treatment of cancer remains difficult due to the complex nature of the disease itself as well as the challenges associated with the synthesis of these therapeutics. Impediments to the discovery of novel drug candidates include lack of available starting materials and access to well-developed syntheses which are both convenient and economically feasible. Semicarbazides, for instance, are a critical synthon for the manufacture of numerous biologically important molecules. Historically, convenient methods for the synthesis of semicarbazides and their derivatives did not exist. Recently, a facile and efficient method for the preparation of semicarbazides via their corresponding phenyl carbamates was developed. These phenyl carbamate intermediates may also be used to prepare a wide variety of other derivatives such as substituted ureas as well as the aryl carbamoyl derivatives of 1,3-diazinane-5-carboxamide. While exploring the preparation of the aryl carbamoyl derivatives of 1,3-diazinane-5-carboxamide, it was found that these compounds possess anti-cancer activity against the glioblastoma LN-229 cell line. Intrigued by these results, additional analogues were designed, leading to the development of a small library of chromenopyrimidinedione and pyrimidinequinolinedione compounds as potential anti-cancer agents. Indeed, these two classes of compounds, with many of the derivatives novel, produced a selection of interesting molecules with potent anti-cancer activity against the glioblastoma cell line LN-229 at biologically relevant concentrations. Taken together, these results provide a unique approach not only to the design but also towards the synthesis of novel therapeutics intended for use as anti-cancer agents. Medicinal-Pharmaceutical Chemistry Organic Chemistry

Search results