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Showing 91 to 97 of 97 (0.202 seconds)| 91 |
Nové regulační mechanismy nukleace mikrotubulů / New regulatory mechanisms of microtubule nucleationČernohorská, Markéta January 2016 (has links)
MT nucleation from γ-tubulin complexes, located at centrosome, is an essential step in the formation of MT cytoskeleton. In mammalian cells, -tubulin is encoded by two genes. We functionally characterized two γ-tubulin proteins and have found that both are functionally equivalent. γ-Tubulin 2 is able to substitute for γ-tubulin 1 in MT nucleation. However, we revealed that unlike TUBG1, TUBG2 expression is downregulated in mouse preimplantation development. Mast cells represent effectors of the allergy reaction. Their activation by antigen induces number of cellular processes such as degranulation, proliferation and cytoskeleton rearrangements. The regulatory mechanisms of MT reorganization during mast cell activation are unknown. We identified new signaling proteins, GIT1 and PIX that interact with - tubulin. Depletion of GIT1 or PIX leads to changes in MT nucleation. GIT1 is phosphorylated on tyrosine and associates with γ-tubulin in a Ca2+ -dependent manner. Our data suggested a novel signaling pathway for MT rearrangement in mast cells where tyrosine kinase-activated GIT1 and βPIX work in concert with Ca2+ signaling to regulate MT nucleation. We tested the capability of GIT1 and PIX to influence -tubulin function in more cell types. We found out that GIT1/βPIX signaling proteins together...
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Dynamique et contrôle optique des molécules froides / Dynamic and optical control of cold moleculesVexiau, Romain 10 December 2012 (has links)
Le travail théorique présenté dans cette thèse concerne la formation de molécules ultra-froides bialcalines et le contrôle de leurs degrés de liberté externes et internes. Cette étude est motivée par les nombreuses expériences en cours visant à l'obtention d'un gaz quantique dégénéré de molécules dans leur état fondamental absolu. Le schéma de formation étudié repose sur le processus de transfert adiabatique stimulé (STIRAP) réalisé en présence d'un potentiel optique de piégeage (réseau optique) des atomes et des molécules.Nous avons déterminé les paramètres du réseau optique (intensité et fréquence du champ laser) qui permettent de piéger efficacement des dimères d'alcalins en évaluant la polarisabilité dynamique acquise par les molécules soumises à un champ externe. Ces calculs reposent en particulier sur la connaissance détaillée de la structure électronique des molécules. Nous avons identifié des plages de longueur d'ondes dites « magiques » où la polarisabilité est la même pour chaque niveau peuplé au cours du transfert adiabatique, permettant ainsi un transfert optimal. Ce formalisme nous a également permis d'obtenir les coefficients Van der Waals de l'interaction à longue portée nécessaires pour étudier les taux de collisions entre molécules.Nous avons réalisé une étude plus détaillée de la molécule RbCs. En étudiant précisément la probabilité de transition de la molécule vers un niveau excité, nous avons proposé un schéma STIRAP pour transférer des molécules de RbCs, initialement dans un niveau vibrationnel excité, vers leur état rovibrationnel fondamental.Ces travaux ont montré l'importance de la connaissance précise de la structure hyperfine de l'état électronique moléculaire excité pour réaliser un gaz dégénéré de molécules dans un état quantique bien défini. Un modèle asymptotique nous a permis d'obtenir une première estimation de la structure hyperfine des courbes d'énergies potentielles des premiers états moléculaires excités des molécules Cs2 et RbCs. / The theoretical work presented in this thesis is focused on the formation of ultracold bialcaline molecules and on the control of their external and internal degrees of freedom. This study is motivated by the increasing number of experiments aiming at obtaining a quantum degenerate gas of molecules in their absolute ground state. The formation scheme we worked on is based on the Stimulated Raman Adiabatic Passage (STIRAP) technique operated while molecules are trapped inside an optical lattice.We have determined the parameters of the optical lattice (intensity and wavelength of the laser) that allow for an efficient trapping of the alkali dimers by evaluating the dynamic polarizability of molecules in the presence of an external field. Such calculations require the accurate knowledge of the electronic structure of the molecules. We have identified the so-called ``magic'' wavelength for which all levels populated during the STIRAP sequence have the same polarizability, thus ensuring an optimal transfer. The same approach has also been used to compute the strength of the long-range interaction between polar bialkali molecules needed to evaluate collision rates.The particular case of the RbCs molecule has been investigated. We have selected a radiative transition allowing for an efficient STIRAP scheme yielding molecules in their rovibrational ground state. These works have raised the need for the precise knowledge of the hyperfine structure of the excited electronic molecular state involved in the STIRAP scheme. We have developed an asymptotic model to obtain a first estimate of the hyperfine structure for the potential curves of the lowest excited states of Cs2 and RbCs.
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RNAi-mediated knockdown of the endogenous TCR improves safety of immunotherapy with TCR gene-modified T cellsBunse, Mario 11 March 2015 (has links)
Durch den Transfer der Gene des heterodimeren T-Zellrezeptors (TZR) mithilfe viraler Vektoren können T-Zellen programmiert werden, ein ausgewähltes Antigen spezifisch zu erkennen. In klinischen Studien wurden solche T-Zellen bereits mit Erfolg zur Immuntherapie von Krebs und viralen Infektionen eingesetzt. Genmodifizierte T-Zellen unterscheiden sich jedoch von normalen T-Zellen, weil sie neben den beiden zelleigenen auch die zwei übertragenen TZR-Gene exprimieren. Diese Situation erlaubt die Bildung vier verschiedener TZR-Heterodimere: der zelleigene TZR, der übertragene TZR und zwei gemischte TZR, bestehend aus je einer übertragenen und einer zelleigenen TZR-Kette. Gemischte TZR bergen das Risiko von Nebenwirkungen, weil sie durch Zufall gesundes Körpergewebe erkennen und so Autoimmunität auslösen könnten. In dieser Arbeit wurden deshalb virale Vektoren entwickelt, die gleichzeitig mit der Übertragung von neuen TZR-Genen den zelleigenen TZR durch RNA Interferenz (RNAi) unterdrücken. Mikro-RNA (miRNA), die in den Vektor MP71 eingefügt wurden, reduzierten den zelleigenen TZR in Maus-T-Zellen um mehr als 85%. Dies hatte zur Folge, dass beide Ketten des übertragenen P14-TZR in gleicher Menge auf der Zelloberfläche exprimiert wurden und die Bildung von gemischten TZR reduziert wurde. In einem Mausmodell der adoptiven T-Zelltherapie verhinderte die Unterdrückung des zelleigenen TZR die Entstehung von Autoimmunität, die andernfalls durch gemischte TZR verursacht wurde. Im Gegensatz dazu führte die Anwendung von gentechnisch optimierten P14-TZR-Genen weder zur angeglichenen Oberflächenexpression der P14-TZR Ketten noch zu weniger Autoimmunität im Mausmodell. Ein anderes Tierexperiment zeigte, dass die miRNA die Funktion der genmodifizierten T-Zellen nicht beeinträchtigte. Schließlich wurde ein viraler Vektor entwickelt und getestet, der die Expression des zelleigenen TZR in menschlichen T-Zellen effektiv unterdrückte und die Bildung von gemischten TZR reduzieren konnte. / T cells can be genetically modified using viral vectors. The transfer of genes encoding both chains of the heterodimeric T cell receptor (TCR) programs T cells to specifically react towards an antigen of choice. Such TCR gene-modified T cells were already successfully applied in clinical studies to treat cancer and viral infections. However, in contrast to nonmanipulated T cells these cells express the transferred TCR in addition to the endogenous TCR and this situation allows the assembly of four different TCR heterodimers: the endogenous TCR, the transferred TCR, and two mixed TCR dimers, composed of one endogenous and one transferred TCR chain. The formation of mixed TCR dimers represents a safety issue because they may by chance recognize self-antigens and thereby cause autoimmune side effects. To overcome this problem, an RNAi-TCR replacement vector was developed that simultaneously silences the endogenous TCR and expresses an RNAi-resistant therapeutic TCR. The expression of miRNA encoded by a retroviral MP71 vector in transduced mouse T cells reduced the surface levels of the endogenous TCR by more than 85%. The knockdown of the endogenous TCR in turn resulted in equal surface expression levels of both transferred P14 TCR chains and prevented the formation of mixed TCR dimers. Accordingly, the development of lethal mixed TCR dimer-dependent autoimmunity (TI-GVHD) in a mouse model of adoptive T cell therapy was dramatically reduced by the knockdown of the endogenous TCR. In contrast, the usage of genetically optimized TCR genes neither resulted in equal surface levels of both P14 TCR chains nor in reduced autoimmunity. A second mouse model demonstrated that the in vivo functionality of the transduced T cells was not negatively influenced by the expression of the miRNA. Finally, an RNAi-TCR replacement vector for human T cells was developed that effectively reduced the expression of the endogenous TCR and prevented the formation of mixed TCR dimers.
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The Ecological Function of Fish MucusMaxi Eckes Unknown Date (has links)
Ultraviolet light is damaging but fish have evolved protective mechanisms, which allows them to live in shallow water reefs, high in UV radiation. This thesis details my investigation into the physiological ecology of solar ultraviolet (UV) absorbing compounds, known as mycosporine-like amino acids found in the external epithelial mucus, and examines the supporting role potentially played by a UV-induced DNA repair mechanism in coral reef fish of the Indo-Pacific. Using reverse phase chromatography and UV spectrophotometry, I examined whether the distribution of MAA compounds across different areas of the body is correlated with differential UV exposure. Comparisons were made between the MAA content and the absorbance spectra of mucus from the dorsal, ventral, caudal and head body surface areas in five species of Scaridae (Chlorurus sordidus, Scarus schlegeli, S. niger, S. psittacus and S. globiceps) from Ningaloo Reef, Coral Bay, Western Australia. All fish analysed had at least five MAAs present, and results showed that fish had increased UV absorbance in mucus over the dorsal area, which receives the brunt of UV radiation. Little UV protection was found in mucus from the ventral area, which receives the lower level of UV radiation mostly via reflection of the sand and reef surfaces. Furthermore, UV absorbance per mg dry mucus versus standard fish length showed that there is a positive relationship in C. sordidus with increasing size. I examined whether there is a difference in the quantity of UV screening compounds found in the mucus of fish along a longitudinal geographical gradient from inshore reefs (Lizard Island, Great Barrier Reef) to the outer edge reefs to oceanic reefs (Osprey Reef). MAA absorbance increased with longitudinal distance from the mainland landmass of Australia to more oligotrophic outer reefs, where UV attenuation is reduced and the ocean is more transparent to UV wavelength. I determined that fish living on inshore, more turbid reefs where UV attenuation in shallow waters is high have lower levels of MAA protection than fish from clear oceanic reefs. Furthermore, there seems to be a direct relationship between light attenuation and exposure with the quantity of protective sunscreening found in the mucus of reef fish. It is know that UV irradiation decreases with water depth and that mucus from fish with deep habitats absorbs less UV than that of fish from shallow habitats. It is unknown however, whether this UV protection is variable within the same individuals and if so, how fast changes 11 occur. To test this, I relocated 9 ambon damselfish from a deep reef (18 m) to a shallow reef (1.5 m) to expose fish to increased levels of UV and relocated another 7 fish from a shallow to a deep reef to expose fish to decreased levels of UV. One week after relocation, all fish were returned to their original reef site to determine whether MAA levels would return to their initial levels. Fish relocated to a shallower depth were recovered and had a 60% (SD+/-2%) increase in mucus UV absorbance. Conversely, the fish relocated to a deeper depth were recovered and had a 41% (SD+/-1%) decrease mucus UV absorbance. No difference was found between UV absorbance of relocated and original fish at both depth. Six days after fish were returned to their original reef, mucus UV absorbance levels had returned to 67% +/- 4% of the original level. These results show that mucus UV absorbance is variable in individual ambon damselfish and that the sunscreen protection typical for a certain depth is reached in relocated fish within just a few days of relocation. The rate of MAA loss is higher than the accumulation of MAAs suggesting that diet is not the sole determining factor involved in the sequestration of MAAs to mucus. The cleaner fish Labroides dimidiatus performs a mutualistic service by removing ectoparasites such as gnathiid isopods as well other dead infected tissue from its clients. Cleaner fish however are also known to feed on client mucus. The benefits of eating mucus until recently were unclear. In this study, we analysed the mucus of several cleaner fish clients to determine whether mucus feeding has a nutritional advantage over gnathiids and whether cleaner fish obtain their own MAA protection through this dietary mucus ingestion. Results show that host fish that are infected with gnathiids of poor nutritional value, in contrast to those that harbour gnathiids with higher nutritional value, continuously exude mucus that has both high nutritional value and high MAA content. These findings support the conclusion that in a competitive market for cleaners some host fish are forced to offer more than parasites to cleaners. Ultraviolet light that is not filtered by UV absorbing compounds such as MAA may still lead to DNA damage such as the formation of cyclobutane pyrimidine dimers (CPDs) or 6-4 photoproducts (6-4 PPs). However, coral reef fish have alternative mechanisms to overcome UV induced damage via the photolyase DNA repair mechanisms. We experimentally demonstrated for the first time that a coral reef fish species, the moon wrasse Thalassoma lunare has the ability to repair DNA damage via photoreactivation. Fish both with and without MAA protection were irradiated with UVB wavelength to induce DNA lesions. Half of the experimental fish were then exposed to photoreactivating wavelength to induce DNA repair 12 while the other fish were blocked from the repair mechanisms. Fish which had undergone DNA repair had the lowest number of lesions regardless of mucus MAA protection. When fish were blocked from photoreactivation wavelengths MAA sunscreens clearly served a photoprotective role. The amount of damage was greatest in fish which both lacked MAAs and which were also blocked from photoreactivating wavelengths. Thus for the overall UV protection of fish both the MAA sunscreens as well as the DNA repair system play a significant role in counteracting UV damage. Ultraviolet protection by MAA sunscreens is ubiquitous in marine fish. To date the same 5 MAA compounds (palythine (λmax 320 nm), asterina (λmax 330 nm), palythinol (λmax 332 nm), usujirene (λmax 357 nm) and palythene (λmax 360nm) have been identified in the mucus of several different species of reef fish from Australia. Here we report the first evidence of the presence of additional UV absorbing compounds found in the mucus of fish from Indonesia. Using UV spectroscopy the mucus of four species of fish was compared between both geographical regions. The presence of an additional peak between 294-296 nm wavelengths suggests the presence of gadusol and/or deoxygadusol, which are photoprotective compounds, thought to be the precursors of MAAs. Thus, UV protecting compounds in the mucus of fish may not be as conserved between different regions as previously assumed. Our knowledge concerning the effect of UV radiation has advanced considerably in the past decade and my research findings contribute to the better understanding of protective mechanisms of marine fish. The correlations I have found between UV attenuation/exposure, depth, and longitude of sampled individuals lead me to believe that mucus UV absorbing MAA compounds are a highly efficient adaptive defence.
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MECHANISTIC STUDIES ON THE PHOTOTOXICITY OF ROSUVASTATIN, ITRACONAZOLE AND IMATINIBNardi, Giacomo 31 March 2015 (has links)
Photosensitizing effects of xenobiotics are of increasing concern in public health
since modern lifestyle often associates sunlight exposure with the presence of chemical
substances in the skin. An important number of chemicals like perfumes, sunscreen
components, or therapeutic agents have been reported as photosensitizers.
In this context, a considerable effort has been made to design a model system for
photosafety assessment. Indeed, screening for phototoxicity is necessary at the
early phase of drug discovery process, even before introducing drugs and chemicals
into clinical therapy, to prevent undesired photoreactions in humans. In the case
of new pharmaceuticals, their phototoxic potential has to be tested when they absorb
in the regions corresponding to the solar spectrum, that is, for wavelengths
>290 nm. So, there is an obvious need for a screening strategy based on in vitro
experiments. The goal of the present thesis was the photochemical study of different
photoactive drugs to investigate the key molecular aspects responsible for their
photosensitivity side effects.
In a first stage, rosuvastatin was considered in chapter 3 as representative
compound of the statin family. This lipid-lowering drug, also known as “superstatin”,
contains a 2-vinylbiphenyl-like moiety and has been previously described
to decompose under solar irradiation, yielding stable dihydrophenanthrene analogues.
During photophysical characterization of rosuvastatin, only a long-lived
transient at ca. 550 nm was observed and assigned to the primary photocyclization
intermediate. Thus, the absence of detectable triplet-triplet absorption and
the low yield of fluorescence ruled out the role of the parent drug as an efficient
sensitizer. In this context, the attention was placed on the rosuvastatin main photoproduct
(ppRSV). Indeed, the photobehavior of this dihydrophenanthrene-like
compound presented the essential components needed for an efficient biomolecule
photosensitizer i.e. (i) a high intersystem crossing quantum yield (ΦISC =0.8), (ii)
a triplet excited state energy of ca. 67 kcal mol−1
, and (iii) a quantum yield of singlet oxygen formation (Φ∆) of 0.3. Furthermore, laser flash photolysis studies
revealed a triplet-triplet energy transfer from the triplet excited state of ppRSV
to thymidine, leading to the formation of cyclobutane thymidine dimers, an important
type of DNA lesion. Finally, tryptophan was used as a probe to investigate the
Type I and/or Type II character of ppRSV-mediated oxidation. In this way, both
an electron transfer process giving rise to the tryptophanyl radical and a singlet
oxygen mediated oxidation were observed. On the basis of the obtained results,
rosuvastatin, through its major photoproduct ppRSV, should be considered as a
potential sensitizer.
Then, itraconazole (ITZ), a broad-spectrum antifungal agent, was chosen as
main character of chapter 4. Its photochemical properties were investigated in connection
with its reported skin photosensitivity disorders. Steady state photolysis,
fluorescence and phosphorescence experiments were performed to understand ITZ
photoreactivity in biological media. The drug is unstable under UVB irradiation,
suffering a primary dehalogenation of the 2,4-dichlorophenyl moiety that occurs
mainly at the ortho-position. In poorly H-donating solvents, as acetonitrile, the
major photoproduct arises from intramolecular attack of the initially generated
aryl radical to the triazole ring. In addition, reduced compounds resulting from
homolytic cleavage of the C-Cl bond in ortho or para positions and subsequent Habstraction
from the medium are obtained to a lesser extent. In good H-donating
solvents, such as ethanol, the main photoproducts are formed by reductive dehalogenation.
Furthermore, irradiation of a model dyad containing a tryptophan unit
and the reactive 2,4-dichlorophenyl moiety of itraconazole leads to formation of
a new covalent link between these two substructures revealing that homolysis of
the C-Cl bond of ITZ can result in alkylation of reactive amino acid residues of
proteins, leading to formation of covalent photoadducts. Therefore, it has been established
that the key process in the photosensitization by itraconazole is cleavage
of the carbon-halogen bond, which leads to aryl radicals and chlorine atoms. These
highly reactive species might be responsible for extensive free radical-mediated biological
damage, including lipid peroxidation or photobinding to proteins.
In chapter 5, photobehavior of imatinib (IMT) was addressed. This is a
promising tyrosine kinase inhibitor used in the treatment of some types of human
cancer, which constitutes a successful example of rational drug design based on the
optimization of the chemical structure to reach an improved pharmacological activity.
Cutaneous reactions, such as increased photosensitivity or pseudoporphyria,
are among the most common nonhematological IMT side effects; however, the
molecular bases of these clinical observations have not been unveiled yet. Thus,
to gain insight into the IMT photosensitizing properties, its photobehavior was
studied together with that of its potentially photoactive anilino-pyrimidine and
pyridyl-pyrimidine fragments. In this context, steady-state and time resolved fluorescence,
as well as laser flash photolysis experiments were run, and the DNA
photosensitization potential was investigated by means of single strand breaks
detection using agarose gel electrophoresis. The obtained results revealed that the drug itself and its anilino-pyrimidine fragment are not DNA-photosensitizers.
By contrast, the pyridyl-pyrimidine substructure displayed a marked photogenotoxic
potential, which was associated with the generation of a long-lived triplet
excited state. Interestingly, this reactive species was efficiently quenched by benzanilide,
another molecular fragment of IMT. Clearly, integration of the photoactive
pyridyl-pyrimidine moiety in a more complex structure strongly modifies its
photobehavior, which in this case is fortunate as it leads to an improved toxicological
profile. Thus, on the bases of the experimental results, direct in vivo
photosensitization by IMT seems unlikely. Instead, the reported photosensitivity
disorders could be related to indirect processes, such as the previously suggested
impairment of melanogenesis or the accumulation of endogenous porphyrins.
Finally, a possible source of errors in the TEMPO/EPR method for singlet
oxygen detection was analyzed. For many biological and biomedical studies, it is essential
to detect the production of 1O2 and to quantify its production yield. Among
the available methods, detection of the characteristic 1270 nm phosphorescence of
singlet oxygen by time-resolved near infrared (TRNIR) emission constitutes the
most direct and unambiguous approach. An alternative indirect method is electron
paramagnetic resonance (EPR) in combination with trapping. This is based on
the detection of the TEMPO free radical formed after oxidation of TEMP (2,2,6,6-
tetramethylpiperidine) by singlet oxygen. Although the TEMPO/EPR method has
been largely employed, it can produce misleading data. This was demonstrated by
the present study, where the quantum yields of singlet oxygen formation obtained
by TRNIR emission and by the TEMPO/EPR method were compared for a set of
well-known photosensitizers. The results revealed that the TEMPO/EPR method
leads to significant overestimation of singlet oxygen yield when the singlet or triplet
excited state of the photosensitizers were efficiently quenched by TEMP, acting as
electron donor. In such case, generation of the TEMP+•
radical cation, followed by
deprotonation and reaction with molecular oxygen gives rise to a EPR detectable
TEMPO signal that is not associated with singlet oxygen production. This knowledge
is essential for an appropriate and error-free application of the TEMPO/EPR
method in chemical, biological and medical studies. / Nardi, G. (2014). MECHANISTIC STUDIES ON THE PHOTOTOXICITY OF ROSUVASTATIN, ITRACONAZOLE AND IMATINIB [Tesis doctoral no publicada]. Universitat Politècnica de València. https://doi.org/10.4995/Thesis/10251/48535 / TESIS
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Étude mécanistique computationnelle des réactions d’amination catalysées par des dimères de rhodiumAzek, Emna 01 1900 (has links)
Catalytic amination reactions are a powerful tool in organic synthesis. They aim to introduce nitrogen atom to alkane, alkene or thioether moieties, giving rise to amine products that have various medical and industrial applications. The Lebel group has developed catalytic amination reactions in the presence of rhodium dimers using N-sulfonyloxycarbamates as nitrene precursors. In the presence of a base, N-sulfonyloxycarbamates presumably afforded rhodium nitrenes which underwent C-H insertions, C=C additions or reactions with the sulfur atom of thioethers resulting in acyclic and cyclic carbamates, aziridines and sulfilimines respectively. In addition, good diastereoselectivities were observed in the presence of a chiral N-sulfonyloxycarbamate reagent and a chiral rhodium dimer for all three reactions.
In this dissertation, we are interested in the mechanistic aspects of these amination reactions. Given the absence of experimental proofs of in-situ generated rhodium nitrene species, playing the role of the amination agent, nor of its precomplex, the rhodium nitrenoid, the different amination reactions mechanisms remain uncertain. Our approach is based on the scan of the potential energy surfaces of different mechanistic paths, for each of the amination reactions, well established on the experimental level, by resorting to the Functional Theory of Density (DFT).
The Ernzerhof research group is expert on the development of exchange-correlation functionals, therefore relevant strict criteria have been considered when choosing and validating the theoretical model used during the mechanistic studies. The correlation exchange functional developed by Perdew-Burke-Ernzerhof (PBE) was established as the best to study reactions involving rhodium dimers where the electronic correlation is strong. We studied the formation and reactivity of rhodium nitrene species considering their two lower energy spin states. Singlet rhodium nitrenes appeared to be the most reactive intermediates for the C-H amination reaction. In addition, singlet rhodium nitrenes were shown responsible for the formation of secondary products such as carbonyls and primary carbamates derived from the corresponding N-mesyloxycarbamates. In sharp contrast, in the aziridination reaction, both singlet and triplet rhodium nitrene species acted as aminating agents in a process involving an intersystem spin crossover. To further rationalize the asymmetric induction of catalytic aziridination reactions, we have undertaken the calculation of the diastereoselectivity ratios in the presence of the chiral catalyst Rh2[(S)-nttl]4. An exhaustive study was performed and it revealed that the asymmetric induction was due to a reactive conformation of rhodium nitrene species in which the ligand adopts C4 symmetry.
Up to now, no mechanistic study involving DFT calculations have been reported in the literature for the amination of thioethers, no matter what catalytic system is used. To study catalytic sulfimidation reactions, we calculated the different mechanistic paths of rhodium catalyzed thioanisole imidation with and without DMAP and bis(DMAP)CH2Cl2 additives. The study showed a 'classical' insertion mechanism of rhodium nitrene species into the thioether in absence of bis(DMAP)CH2Cl2. In the presence of the latter, the mechanism diverged to a thioether insertion/salt (bis(DMAP)CH2Cl-OMs) elimination reaction where the rhodium nitrenoid complex was, henceforth, the imidation reagent. / Les réactions d’amination catalytiques sont un outil très efficace en synthèse organique.
Elles consistent à introduire un azote sur différents composés organiques, permettant de
synthétiser des produits aminés qui peuvent être utilisés pour différentes applications
médicales et industrielles. Le groupe de recherche du Pr Lebel a développé des réactions
d’amination faisant appel aux dimères de rhodium comme catalyseurs et en utilisant les Nsulfonyloxycarbamates,
comme précurseurs de nitrènes métalliques. En effet, en présence
d’une base, les N-sulfonyloxycarbamates forment possiblement un intermédiaire de type
nitrène de rhodium qui peuvent s’insérer dans un lien C-H, s’additionner sur un lien C=C ou
réagir avec un atome de soufre d’un thioéther. On peut ainsi préparer des carbamates cycliques
et acycliques, des aziridines et des sulfilimines respectivement. Dans le cas où les réactions
d’amination sont catalysées par des dimères de rhodium chiraux, on obtient de bonnes
diastéréosélectivités en présence d’un réactif N-sulfonyloxycarbamate chiral.
Dans cette dissertation, nous nous sommes intéressés aux aspects mécanistiques de ces
réactions d’amination. À défaut de preuves expérimentales solides pour prouver la génération
in-situ des espèces nitrènes de rhodium, lesquelles sont les agents d’amination clés, ni de celle
du pré-complexe, nitrénoïde de rhodium, des incertitudes subsistaient toujours concernant les
mécanismes des différentes réactions d’amination. Notre approche se base sur l’étude des
surfaces d’énergies potentielles de différents chemins mécanistiques possibles pour chacune
des réactions d’amination, bien établie sur le plan expérimental, en faisant recours à la Théorie
des Fonctionnelles de la Densité (DFT).
Le groupe de recherche du Pr Ernzerhof est expert dans le développement des
fonctionnelles d’échange-corrélation. Pour ce, des critères strictes et pertinents ont été pris en
compte lors du choix et de la validation du modèle théorique utilisé dans ces études
mécanistiques. La fonctionnelle d’échange corrélation développée par Perdew–Burke–
Ernzerhof (PBE) s’est révélé être la meilleure pour décrire ces systèmes réactionnels faisant
intervenir les dimères de rhodium dont la corrélation électronique est forte. À l’aide de cette
fonctionnelle pure, nous avons étudié la formation et la réactivité des espèces nitrènes de
rhodium en fonction de leurs deux états de spin de plus basse énergie. Les nitrènes de rhodium
singulet se sont révélés être les intermédiaires les plus réactifs dans l`amination de liens C-H.
De plus, les nitrènes de rhodium à l’état singulet sont responsables de la formation des
produits secondaires tels que les carbonyles et les carbamates primaires dérivés des Nmésyloxycarbamates
correspondants. Dans la réaction d’aziridination, les espèces nitrènes de
rhodium à l’état singulet et triplet peuvent toutes les deux agir comme agents d'amination et
les processus font intervenir un croisement intersystème de spin. Afin de rationaliser
l’induction asymétrique des réactions d’aziridination catalytiques, nous avons entrepris le
calcul des ratios de diastéréosélectivités en présence du catalyseur chiral Rh2[(S)-nttl]4.
L’étude exhaustive de cette réaction a permis de déterminer que l’induction asymétrique
provient d’une conformation réactive de l’espèce nitrène de rhodium de symétrie C4.
Aucune étude mécanistique s’appuyant sur la chimie computationnelle n’a été rapportée
dans la littérature pour la réaction d’amination de thioéthers et ce peu importe le système
catalytique. Afin d’étudier les réactions de sulfimidation catalytiques, nous avons calculé les
différents chemins mécanistiques de l’imidation du thioanisole catalysée par un complexe de
rhodium avec et sans les additifs DMAP et bis(DMAP)CH2Cl2. L’étude montre que le
mécanisme procède via une insertion ‘classique’ des espèces nitrènes de rhodium dans le
thioéther en absence de bis(DMAP)CH2Cl2. En présence de ce dernier, le mécanisme diverge
vers une réaction d’insertion du thioéther/élimination d’un sel (bis(DMAP)CH2Cl-OMs) où le
complexe nitrénoïde de rhodium devient, désormais, l’agent d’imidation.
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Phytochemical investigation of Acronychia species using NMR and LC-MS based dereplication and metabolomics approaches / Etude phytochimique d’espèces du genre Acronychia en utilisant des approches de déréplication et métabolomique basées sur des techniques RMN et SMKouloura, Eirini 28 November 2014 (has links)
Les plantes médicinales constituent une source inexhaustible de composés (des produits naturels - PN) utilisé en médecine pour la prévention et le traitement de diverses maladies. L'introduction de nouvelles technologies et méthodes dans le domaine de la chimie des produits naturels a permis le développement de méthodes ‘high throughput’ pour la détermination de la composition chimique des extraits de plantes, l'évaluation de leurs propriétés et l'exploration de leur potentiel en tant que candidats médicaments. Dernièrement, la métabolomique, une approche intégrée incorporant les avantages des technologies d'analyse moderne et la puissance de la bioinformatique s’est révélé un outil efficace dans la biologie des systèmes. En particulier, l'application de la métabolomique pour la découverte de nouveaux composés bioactifs constitue un domaine émergent dans la chimie des produits naturels. Dans ce contexte, le genre Acronychia de la famille des Rutaceae a été choisi sur la base de son usage en médecine traditionnelle pour ses propriétés antimicrobienne, antipyrétique, antispasmodique et anti-inflammatoire. Nombre de méthodes chromatographiques modernes, spectrométriques et spectroscopiques sont utilisées pour l'exploration de leur contenu en métabolites suivant trois axes principaux constituant les trois chapitres de cette thèse. En bref, le premier chapitre décrit l’étude phytochimique d’Acronychia pedunculata, l’identification des métabolites secondaires contenus dans cette espèce et l'évaluation de leurs propriétés biologiques. Le deuxième chapitre vise au développement de méthodes analytiques pour l'identification des dimères d’acétophénones (marqueurs chimiotaxonomiques du genre) et aux stratégies utilisées pour la déréplication de ces différents extraits et la caractérisation chimique des composés par UHPLC-HRMSn. Le troisième chapitre se concentre sur l'application de méthodologies métabolomique (RMN et LC-MS) pour l'analyse comparative (entre les différentes espèces, origines, organes), pour des études chimiotaxonomiques (entre les espèces) et pour la corrélation des composés contenus avec une activité pharmacologique. / Medicinal plants constitute an unfailing source of compounds (natural products – NPs) utilised in medicine for the prevention and treatment of various deceases. The introduction of new technologies and methods in the field of natural products chemistry enabled the development of high throughput methodologies for the chemical composition determination of plant extracts, evaluation of their properties and the exploration of their potentials as drug candidates. Lately, metabolomics, an integrated approach incorporating the advantages of modern analytical technologies and the power of bioinformatics has been proven an efficient tool in systems biology. In particular, the application of metabolomics for the discovery of new bioactive compounds constitutes an emerging field in natural products chemistry. In this context, Acronychia genus of Rutaceae family was selected based on its well-known traditional use as antimicrobial, antipyretic, antispasmodic and anti-inflammatory therapeutic agent. Modern chromatographic, spectrometric and spectroscopic methods were utilised for the exploration of their metabolite content following three basic axes constituting the three chapters of this thesis. Briefly, the first chapter describes the phytochemical investigation of Acronychia pedunculata, the identification of secondary metabolites contained in this species and evaluation of their biological properties. The second chapter refers to the development of analytical methods for the identification of acetophenones (chemotaxonomic markers of the genus) and to the dereplication strategies for the chemical characterisation of extracts by UHPLC-HRMSn. The third chapter focuses on the application of metabolomic methodologies (LC-MS & NMR) for comparative analysis (between different species, origins, organs), chemotaxonomic studies (between species) and compound-activity correlations.
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