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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

Accès à de nouvelles structures tricycliques di-iodes à base indolique et isoindolique par iodocyclisation / Access to new di-iodinated tricyclic structures based on indoles and isoindoles by iodocyclization

Hammoud, Sokaina 16 December 2015 (has links)
Une nouvelle voie d’accès à des structures tri-cycliques originaux les « oxazino-indole di-iodés» a été mise au point à partir des acides 1H-indole-2-carboxyliques commerciaux ou des acides 1H-indole-2-carboxyliques fonctionnalisés obtenus par la réaction d’Hemetsberger-Knittel. La dernière étape de cette séquence est une réaction d’iodocyclisation qui s’est avérée totalement régio- et stéréosélective selon un processus de type 6-exo-dig. Cette méthodologie a ensuite été étendue en série isoindolique permettant un accès à des motifs « oxazino-isoindolique di-iodés » originaux. Afin d'étendre davantage cette méthodologie, de nouveaux « oxazepino-indole di-iodés » ont été préparés en utilisant la même approche synthétique à partir de l'acide 1H-indole-7-carboxylique. La réactivité des structures tri-cycliques di-iodés a été étudiée via des réactions de Cross-Coupling (Stille, Sonogashira, Suzuki) par l’utilisation de sels de palladium permettant une fonctionnalisation régiosélective de l’iode exocyclique. / A new access pathway to the original tricyclic structures "di-iodinated oxazino-indole" was developed from the commercial 1H-indole-2-carboxylic acids or functionalized 1H-indole-2-carboxylic acid obtained by Hemetsberger-Knittel reaction. The last step in this sequence is an iodocyclisation reaction that is proved to be completely regio- and stereoselective via 6-exo-dig process. This methodology was then extended to isoindolic series allowing access to original "di-iodinated oxazino-isoindole" motifs. To further extend this methodology, new"di-iodinated oxazepino-indoles" were prepared using the same synthetic approach from the 1H-indole-7-carboxylic acid. The reactivity of the di-iodinated tri-cyclic structures has been studied via Cross-Coupling reactions (Stille, Sonogashira and Suzuki) by the use of palladium salts allowing a regioselective functionalization of the exocyclic iodine.
2

bβ-enamino ésteres como precursores de análogos do GABA e de di-hidropiridinas / β-enamine esters as precursors of GABA and dihydropyridines analogues

Gonçalo, Erika Rocha da Silva 01 December 2006 (has links)
Nesta tese foi empregada a iodociclofuncionalização de β-enamino ésteres para obtenção de análogos conformacionalmente restritos do ácido γ-aminobutírico (GABA) e de 4-aril-1,4-di-hidropiridinas (DHP\'s). Foram preparados ciclopentanos trissubstituídos a partir de b-enamino ésteres cíclicos, com o objetivo de investigar o mecanismo desta reação. Utilizando ESI(+)-MS/MS, foi possível identificar e caracterizar os intermediários bicíclicos catiônicos, confirmando que a reação se processa através de uma SN2 intramolecular. A biorredução do grupo acetila existente nos ciclopentanos, utilizando raízes de Daucus carota e células íntegras de Aspergillus terreus CCT 3320 e Rhizopus oryzae CCT 4964, forneceu novos análogos oticamente ativos do GABA, com excelente enantiosseletividade. Também foram preparados iodo-β-enamino ésteres cíclicos de seis membros, contendo um grupo arila na posição 4 do anel tetra-hidropiridínico, cuja desidroiodação forneceu os respectivos derivados 1,4-di-hidropiridínicos. / This thesis presents a study of iodo-cyclization of β-enamino esters in order to obtain conformationally restricted analogues of γ-amino butiric acid (GABA) and of 1,4-dihydropyridines (DHP\'s). Trisubstituted cyclopentanes were obtained from iodo-β-enamino esters and the mechanism of their formation was proposed and corroborated by (+)-ESI-MS/MS through the interception and structural characterization of the key bicyclic iminium ion intermediates. Optically active GABA analogues have been prepared in high enantiomeric excesses (up to >99%) by bioreduction of the keto group in cyclopentane derivatives using whole fungal cells of Aspergillus terreus CCT 3320, Rhizopus oryzae CCT 4964 and Daucus carota root. 4-aryl-1,4,5,6-tetrahydropyridine derivatives were synthesized by iodo-cyclization of a-alkenyl-b-enamino esters and 4-phenyl-1,4-dihydropyridine derivatives were obtained after base-promoted dehydroiodination of the corresponding cyclic iodo-b-enamino esters.
3

bβ-enamino ésteres como precursores de análogos do GABA e de di-hidropiridinas / β-enamine esters as precursors of GABA and dihydropyridines analogues

Erika Rocha da Silva Gonçalo 01 December 2006 (has links)
Nesta tese foi empregada a iodociclofuncionalização de β-enamino ésteres para obtenção de análogos conformacionalmente restritos do ácido γ-aminobutírico (GABA) e de 4-aril-1,4-di-hidropiridinas (DHP\'s). Foram preparados ciclopentanos trissubstituídos a partir de b-enamino ésteres cíclicos, com o objetivo de investigar o mecanismo desta reação. Utilizando ESI(+)-MS/MS, foi possível identificar e caracterizar os intermediários bicíclicos catiônicos, confirmando que a reação se processa através de uma SN2 intramolecular. A biorredução do grupo acetila existente nos ciclopentanos, utilizando raízes de Daucus carota e células íntegras de Aspergillus terreus CCT 3320 e Rhizopus oryzae CCT 4964, forneceu novos análogos oticamente ativos do GABA, com excelente enantiosseletividade. Também foram preparados iodo-β-enamino ésteres cíclicos de seis membros, contendo um grupo arila na posição 4 do anel tetra-hidropiridínico, cuja desidroiodação forneceu os respectivos derivados 1,4-di-hidropiridínicos. / This thesis presents a study of iodo-cyclization of β-enamino esters in order to obtain conformationally restricted analogues of γ-amino butiric acid (GABA) and of 1,4-dihydropyridines (DHP\'s). Trisubstituted cyclopentanes were obtained from iodo-β-enamino esters and the mechanism of their formation was proposed and corroborated by (+)-ESI-MS/MS through the interception and structural characterization of the key bicyclic iminium ion intermediates. Optically active GABA analogues have been prepared in high enantiomeric excesses (up to >99%) by bioreduction of the keto group in cyclopentane derivatives using whole fungal cells of Aspergillus terreus CCT 3320, Rhizopus oryzae CCT 4964 and Daucus carota root. 4-aryl-1,4,5,6-tetrahydropyridine derivatives were synthesized by iodo-cyclization of a-alkenyl-b-enamino esters and 4-phenyl-1,4-dihydropyridine derivatives were obtained after base-promoted dehydroiodination of the corresponding cyclic iodo-b-enamino esters.

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