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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
1

SOLUTION AND SOLID STATE INTERACTIONS BETWEEN IONIC π-SYSTEMS

Chen, Jing 01 January 2006 (has links)
Although attractive interactions between π systems (π-π interaction) have been known for many years, understanding of its origin is still incomplete. Quantitative measuring of π-stacking is challenging due to the weak nature of the π-π interaction. This dissertation aims at elucidating a quantitative conformational analysis by NMR ring current anisotropy of an organic compound capable of intramolecular π-stacking in solution and studying charge effects on the stacking of π-systems. This dissertation offers four contributions to the area. (1) A general approach to four-state, conformational analysis based on the magnetic anisotropy of molecules undergoing fast dynamic exchange is described. (2) Study unveiled the importance of charges in the conformation of a dication in the solution. (3) Novel aromatic salt pairs of triangulene derivatives with the delocalized cation-anion interaction were synthesized and studied. (4) Study unveiled ionic π-systems preferred face-to-face stacking due to strong cation-π and anion-cation attractions. A general protocol for the application of magnetic anisotropy to quantitative multi-state conformational analysis of molecules undergoing fast conformational exchange was suggested in the current study. The reliability of this method of conformational analysis was checked by the mass balance. VT-NMR was also conducted to study the enthalpic parameters. This technique can be further used to study canonical interactions such as ion pairing, hydrogen boning, and molecular recognition. In the current study, dependence of the probe conformations on the dispersive interactions at the aromatic edges between solvent and probes was tested by conformational distributions of the fluorinated derivatives (2b and 2c) of the probe molecule (1a). Solution and solid studies of these molecules put the previous conclusion drawn by the Cammers group in question. Current studies show that the dispersive interaction at the aromatic edge could not be the predominant force on the conformational changes in the probe molecule 1a during the fluoroalkanol perturbation. This study indicated that charges might be important in the formation of the folding conformations in the solution and solid state of 1a, 2b, and 2c. A contribution of this thesis was to prepare and study a conformational model that lacked charges. The previous molecules were charged. The solid-state structures of pyridinium-derived aromatic rings from the CSD (Cambridge Structural Database) were studied to investigate the π-π interaction between cationic π-systems in solid state. Novel aromatic salt pairs of triangulene derivatives with the delocalized cation-anion interaction were synthesized to study the π-π interaction between two aromatic rings that carried opposite charges. This study showed that the interaction between ionic π-systems can be enhanced by cation-π and anion-cation attractions. The stackings of these π-systems introduce more overlap, closer packing and stronger atomic contact than that of the solid states of comparable neutral species. Cation-π and anion-cation attractions are synergistic in aromatic salts.
2

Conception, synthèse et études structurales de foldamères aromatiques repliés en feuillet / Design, synthesis and structural studies of ß-sheet-like aromatic amide-based foldamers

Sebaoun, Laure 23 September 2013 (has links)
Ce travail a pour objectif d’augmenter la diversité des foldamères par le développement d’une nouvelle classe d’architectures abiotiques mimant le repliement des feuillets β protéiques. La stratégie employée repose sur des processus de structuration qui diffèrent de ceux observés au sein du vivant. Les deux éléments essentiels des systèmes naturels, à savoir la boucle courte et flexible d’acides aminés et les brins β liés entre eux par des liaisons hydrogènes, sont ici substitués respectivement par un coude rigide formé de noyaux aromatiques et par des oligoarylamides plans interagissant par empilement aromatique.Ces objets ont été conçus pour adopter des structures repliées caractérisables en solution par spectroscopie RMN et à l’état solide par diffraction des rayons X. Dans une première partie, l’optimisation du pseudo-coude β et de la séquence des brins, ainsi que l’exploration des premières architectures en feuillet seront étudiées à travers la conception, la synthèse et les études structurales de ces oligoamides et oligoamines aromatiques. Dans une seconde partie, le concept mis en oeuvre sera étendu à la synthèse de foldamères plus élaborés à brins courbés, ouvrant ainsi des perspectives intéressantes vers l’obtention d’architectures toujours plus complexes. / The purpose of this work is to expand foldamer diversity by developing a novel class of abiotic β-sheet-like architectures. Our strategy uses inter-strand π-π aromatic stacking between sequences of aromatic oligoamides and oligoamines to mimic the natural stabilization of β-strands, which occurs through a network of regularly spaced hydrogen bonds. These oligamide and oligoamine sequences are connected by a rigid U-shaped moiety that creates a turn and initiates strand formation.These molecules have been designed to adopt compact folded structures that can be studied in solution by NMR spectroscopy and in the solid state by X-ray crystallography. In the first part of this dissertation, we report our stepwise approach in the development of β-sheet-like aromatic amide-based foldamers: from the optimization of the design elements and the use of macrocycles, to the synthesis of multi-turn structures. In the second part, the concept will be extented to the synthesis of more elaborate curving strand β-sheet-like foldamers, opening up new perspectives for more complex architectures.
3

Synthèses et analyses structurales d’oligomères d’ATCs : une nouvelle famille de γ-aminoacides hétérocycliques pour la conception de foldamères / Syntheses and structural analyses of ATCs oligomers : a new family of heterocyclic γ-aminoacids for foldamers conception

Mathieu, Loic 15 January 2015 (has links)
Le travail décrit dans ce manuscrit est consacré à la synthèse et à la caractérisation structurale d'une nouvelle famille de γ-amino acides hétérocycliques contraints, les ATCs (acides 4-Amino-(méthyl)-1,3-Thiazole-5-Carboxyliques). Ces monomères sont construits autour d'un noyau thiazole inséré entre les carbones Cα-Cβ permettant de limiter la valeur de l'angle dièdre ζ à 0°. La présence de deux points de substitution, sur le carbone γ asymétrique et en position 2 du noyau aromatique, autorise une large diversification structurale des ATCs. Des séries d'oligomères, i.e. dimères, tétramères et hexamères solubles dans les solvants organiques halogénés, dans les alcools et dans l'eau ont été synthétisées par couplages peptidiques. La conformation adoptée par ces séquences a été déterminée en solution par RMN 1D et 2D associées à des techniques de modélisation sous contraintes RMN. Nous avons montré que les oligomères d'ATCs s'arrangeaient en hélices 39 droites, présentant un pas de 11,8 Å. La conformation hélicoïdale est stabilisée par un réseau de liaisons hydrogène de type CO(i)…NH(i+2) s'établissant tout au long de la séquence, faisant entrer les oligomères d'ATCs dans le monde des foldamères. Des mesures de dichroïsme circulaire ont permis d'apprécier la stabilité conformationnelle des édifices et l'analyse à l'état solide par diffraction des rayons X a confirmé l'arrangement observé par RMN. Dans une seconde partie nous avons étudié le rôle structurant d'un motif ATC placé au sein d'une petite séquence peptidique. Nous montrons au travers d'expériences RMN et de calculs théoriques que la configuration du monomère d'ATC conditionne la conformation de peptides hybrides αγαα en solution. En termes d'application nous décrivons l'utilisation du motif ATC comme mime de coude pour concevoir un analogue fonctionnel de la gramicidine S, un cyclodécapeptide symétrique antibactérien. La dernière partie de ce travail concerne nos efforts pour développer, à partir des connaissances acquises quant à la structure tridimensionnelle des oligomères d'ATCs, des inhibiteurs de l'interaction protéine-protéine STAT6-NCoA-1. / The work described herein is devoted to the synthesis and the structural characterization of a new family of heterocyclic constrained γ-amino acids, named ATCs (4-Amino-(methyl)-1,3-Thiazole-5-Carboxylic acids). These building-blocks are built around a thiazole ring inserted between the Cα-Cβ carbons allowing the limitation of the ζ dihedral angle value to 0°. The presence of two diversification points both on the γ asymmetric carbon and on the position 2 of the aromatic ring, allows a large structural diversification of the ATCs. Series of oligomers consisting in dimers, tetramers and hexamers soluble in halogenated solvents, alcools and water have been synthesized according to peptide chemistry. The conformations of the sequences have been studied by various NMR experiments associated to modelling studies led under NMR constraints. The ATC oligomers adopt a right 39 helical shape, owning a pitch of 11.8 Å which has been confirmed by crystallography. The helix is stabilized by a conserved hydrogen bond pattern between CO(i)…NH(i+2) occurring all along the sequence axis. Circular dichroism measures have been done to check the conformational stability of the architectures. In the second part of the manuscript, we demonstrate by NMR and theoretical computing that when included in a short peptide sequence, ATCs could act as turns. The derived application consists in optimizing the biological behaviour of the ATC moiety as a turn mimetic thanks to the design and the antibacterial evaluation of a gramicidin S analogue. Based on our knowledge about the three-dimensional structure of ATC oligomers, the last part of this work deals with our efforts to develop inhibitors of protein-protein interaction STAT6-NCoA-1.

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