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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

Studies on Palladium-Catalyzed Arylative Cyclization Reactions / パラジウム触媒による環化を伴うアリール化反応の研究

Fujino, Daishi 24 March 2014 (has links)
京都大学 / 0048 / 新制・課程博士 / 博士(理学) / 甲第18097号 / 理博第3975号 / 新制||理||1573(附属図書館) / 30955 / 京都大学大学院理学研究科化学専攻 / (主査)准教授 依光 英樹, 教授 丸岡 啓二, 教授 大須賀 篤弘 / 学位規則第4条第1項該当 / Doctor of Science / Kyoto University / DGAM
2

Synthesis of 3-Acylbenzo[b]thiophenes via Mercury (II)-Catalyzed Cyclization reaction

Lin, Cheng-Han 20 July 2011 (has links)
Treatment of 1-(methylsulfinyl)-2-(phenylethynyl)benzene with 10 mol % of mercury dichloride and 1 equivalent of 2,3-dichloro-5,6-dicyano-1,4-benzoquinone in refluxing benzene gave benzo[b]thiophene in good yields. This method tolerated various functional groups in phenylethynyl moiety, including electron donating groups and electron withdrawing groups. Useing 1-(benzylsulfinyl)-2-(phenylethynyl)benzene as reaction substrate increased the yields of benzo[b]thiophene derivatives. Isotope effect showed that this cyclization reaction belong to Pummerer type cyclization reaction.
3

Design of Anticancer Agents Based on the Tetrahydroisoquinoline Alkaloids

Sun, Tsung-Hsien 26 November 2007 (has links)
The tetrahydroisoquinoline alkaloids have been studied thoroughly about their biological and chemical significance over the past 30 years. These natural products show great biological activity, especially ET-743 and saframycin A, makes them promising therapeutics, while their structural complexity and particularity provide challenging synthetic targets. These alkaloids or derivatives show interesting biological activity, but the most important drawback as potential market therapeutics is the minute amount of them available from nature, and the synthetic methods published are inconvenient, difficult, and hard to handle. Herein is described our researches about the tetrahydroisoquinoline alkaloids. Chapter 1 describes relevant background related to the biological significance of these alkaloids, and the currently synthetic studies toward these natural products. Chapter 2 describes our design and synthesis of the analogues based on the anticancer mechanism of the tetrahydroisoquinoline alkaloids, and the biological activities of these analogues. Chapter 3 describes a rapid synthetic route for the common structure of the bis-tetrahydroisoquinoline alkaloids via a controlled mono-Pictet-Spengler cyclization.
4

Síntese diastereosseletivas e atividades antinociceptivas de novos derivados tetraidropirânicos substituídos / Diastereoselective synthesis and antinociceptive activities of new substituted tetrahydropyran derivatives

Capim, Saulo Luis 02 August 2013 (has links)
Made available in DSpace on 2015-05-14T13:21:21Z (GMT). No. of bitstreams: 1 ArquivoTotal.pdf: 14314411 bytes, checksum: 28743a0226eb51126ce933c575333208 (MD5) Previous issue date: 2013-08-02 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPES / This work is described the synthesis of ten new tetrahydropyran derivatives (compounds 42-51) designed from (±)-Naproxen structure utilizing the Prins reaction of cyclization as the key step to building shaped diastereoselective 2,4- cis and 2,4,6-cis rings tetrahydropyran, with overall yields between 62 - 65%. These new tetrahydropyran derivatives were in vivo bioevaluated on antinociceptive effect in the acetic acid-induced abdominal writhing test, the tail flick test, the rota-rod performance and open field tests, and all these new compounds showed greater antinociceptive activity compared to compound (±)- 1a, highlighting high activity tetraidropirânico derivative (±)-49, which showed 87.5% of inhibition, whereas compound (±)-1a gave only 14% inhibition in in the acetic acid-induced abdominal writhing test. Moreover, the (tail-flick test) indicated compounds (±)-46 and (±)-49 as the most actives, and all compounds showed antinociceptive activity (except compound (±) -51) without harming the motor impairment and without showing toxicity in mice. In continuation to this work, there was the synthesis of new hybrid molecules based on the structure of six non-steroidal anti-inflammatory drugs with a portion tetrahydropyran using molecular hybridization strategy. These new hybrid tetrahydropyran (74 - 79) were obtained in yields between (70 - 93%). Preliminary studies antinociceptive effect in the acetic acid-induced abdominal writhing test in the compounds (74 - 79) showed that all tetrahydropyran derivatives were more efficacious (lower ED50) and their precursors drugs and no sign of intoxication were observed in the animals. / Neste trabalho, é descrito a síntese de 10 novos derivados tetraidropirânicos compostos (42 51) planejados a partir da estrutura do (±)-Naproxeno, utilizando a reação de ciclização de Prins como etapa chave para a construção em forma diastereosseletiva 2,4-cis e 2,4,6-cis de anéis tetraidropirânicos, com rendimentos globais entre 62 65%. Estes novos derivados tetraidropirânicos foram bioavaliados in vivo em testes de contorções abdominais, retirada de cauda, desempenho no rota-rod e campo aberto, sendo que todos estes compostos apresentaram uma maior atividade antinociceptiva em relação ao composto (±)-1a, com destaque para a alta atividade do derivado tetraidropirânico (±)-49, que apresentou 87,5% de inibição, enquanto que o composto (±)-1a apresentou apenas 14% de inibição no teste de contorções abdominais induzida por ácido acético. Além disso, os testes de retirada de cauda indicaram os compostos (±)-46 e (±)-49 como os mais ativos, sendo que todos os compostos apresentaram atividade antinociceptiva (exceto composto (±)-51) sem prejudicar o comprometimento motor e sem demonstrar toxicidades em camundongos. Em continuação ao nosso trabalho, realizou-se a síntese de moléculas híbridas inéditas baseadas na estrutura de seis fármacos antiinflamatórios não esteroidais com uma porção tetraidropirânica utilizando a estratégia de hibridização molecular. Estes novos derivados tetraidropirânicos híbridos (74 79) foram obtidos em rendimentos entre 70 93%. Estudos preliminares realizados em teste contorções abdominais induzidas por ácido acético realizados nos compostos (74 79) revelaram que todos os derivados tetraidropirânicos foram mais eficazes (DE50 menor) que os seus fármacos percusores e nenhum sintoma de intoxicação foi observado nos animais.
5

Reação de ciclização de prins na síntetica diastereosseletiva de 31 análogos meso-tetraidropirâneos: determinação de estruturas cristalinas, estudos teóricos e avaliação in vitro da atividade antileucêmica. / Prins cyclization reaction of the diastereoselective synthesis of 31 analogues meso-tetrahydropyran: determination of crystal structures, theoretical studies and evaluation in vitro of antileukemic activity

Silva, Fábio Pedrosa Lins 30 August 2013 (has links)
Made available in DSpace on 2015-05-14T13:21:22Z (GMT). No. of bitstreams: 1 ArquivoTotal.pdf: 18195512 bytes, checksum: 6229ab5e9f367190d5f7b4336c07dfec (MD5) Previous issue date: 2013-08-30 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPES / This study was designed based on the concept of achiral / meso compound. The importance of preparing achiral compounds is based on their structural simplification, leading to new molecules which require no further investigations pharmacodynamics and pharmacokinetics of the enantiomers. Therefore, it is proposed to the synthesis of analogues tetrahydropyrans achiral/meso using the Prins cyclization reaction. The homoallylic alcohols synthesized in this work were derived from the Barbier reaction obtained in great yields, wherein these products are used as a synthesis intermediate for the preparation of tetrahydropyrans proposed. The Prins cyclization reaction is an efficient method for the preparation of tetrahydropyrans therefore proved to be a powerful tool for synthesis and versatile for the preparation of substituted tetrahydropyrans to give all the compounds synthesized in satisfactory yields. Through spectroscopic and crystallographic studies were possible to determine in detail the relative configuration of the molecules 40a, 41a, 44a, 45a, 46a, 46b and 48b. Furthermore, a theoretical study was developed using the density functional theory to obtain the molecular geometries optimized in the gas phase, making it possible to compare these preferred conformations with geometries defined by crystals. The tetrahydropyrans bioevaluated were synthesized in the leukemic cell line K562 and two types of normal L929 cells and PBMC. The results were very promising in cancer in vitro assays, highlighting the hydrazones 42a-c and the 43a-c aminoguanidines they were the only compounds that were active against resistant cell line K562, highlighting the tetrahydropyran 42c which showed higher activity series counterpart (present value of IC50 7.59 μM) and the tetrahydropyran 42b with an excellent IC50 (8.97 μM) value and a good selectivity index (2.2 in L929 and 1.6 in PBMC). / Este trabalho foi idealizado baseado no conceito de compostos aquirais/meso. A importância da preparação de compostos aquirais está baseada na sua simplificação estrutural, conduzindo a novas moléculas que não necessitam de posteriores investigações farmacodinâmicas e farmacocinéticas dos enantiômeros. Sendo assim, propomos neste trabalho a síntese de análogos tetraidropirânicos aquirais/meso utilizando a reação de ciclização de Prins. Os álcoois homoalílicos sintetizados foram provenientes da reação de Barbier obtidos em ótimos rendimentos, no qual estes produtos foram utilizados como intermediário de síntese para a preparação dos tetraidropiranos propostos. A reação de ciclização de Prins é um método eficiente na preparação dos tetraidropiranos, pois mostrou-se ser uma ferramenta de síntese poderosa e versátil para a preparação dos tetraidropiranos substituídos, obtendo-se todos os compostos sintetizados em rendimentos satisfatórios. Através de estudos espectroscópicos e cristalográficos foi possível determinar detalhadamente a configuração relativa das moléculas 40a, 41a, 44a, 45a, 46a, 46b e 48b. Além disso, foi desenvolvido um estudo teórico utilizando a teoria do funcional densidade para se obter as geometrias moleculares otimizadas em fase gasosa, tornando possível comparar estas conformações preferenciais com as geometrias definidas pelos cristais. Os tetraidropiranos sintetizados foram bioavaliados na linhagem de células leucêmicas K562 e dois tipos de células normais L929 e PBMC. Os resultados em câncer foram bastante promissores nos ensaios in vitro, dando destaque para as hidrazonas 42a-c e as aminoguanidinas 43a-c que foram os únicos compostos que se mostraram ativos contra a linhagem celular resistente K562, destacando-se o tetraidropirano 42c que apresentou maior atividade da série congênere (apresentando valor de CI50 7.59 μM) e o tetraidropirano 42b que apresentou excelente valor de IC50 (8.97 μM) e um bom índice de seletividade (2.2 em L929 e 1.6 em PBMC).
6

Stratégie radicalaire SRN1/Mn(OAc)3 sur des dérivés naphtoquinoniques à visée pharmacologique / Synthesis of new potentially bioactive naphthoquinonic derivatives by SRN1 or Mn(OAc)3 strategy

Meye Biyogo, Alex 12 December 2016 (has links)
Ce travail est consacré à la recherche et au développement de nouvelles molécules à viséepharmacologique en série naphtoquinonique en utilisant des réactions par transfert monoélectroniquede type SRN1 et des cyclisations radicalaires oxydatives induites par l'acétate de manganèse(III). Lapremière partie décrit l’étude de la réactivité SRN1 de la 2-(chlorométhyl)-3-méthoxynaphtoquinoneavec divers anions nitronates conduisant à la formation de produits de C-alkylation avec de bonsrendements. Ces derniers ont fait l’objet d’une réaction de réduction-cyclisation permettant la synthèsede nouveaux dérivés benzo[g]indol-5(3H)-ones. Dans la seconde partie, une nouvelle réactiond’oxydation initiée par l’acétate de manganèse(III) a été développée sur la 2-hydroxy-3-méthylnaphtoquinone dans des conditions opératoires douces. En effet, la réactivité originale de la 2-hydroxy-3-méthylnaphtoquinone avec divers alcènes aromatiques en présence de Mn(OAc)3 et dedioxygène, a permis pour la première fois en série naphtoquinonique, l’obtention de nouveaux dérivésoriginaux dihydronaphto[2,3-c][1,2]dioxine-5,10(3H,10aH)-diones sous forme d’un mélange dediastéréoisomères à potentialités antipaludiques. Un mécanisme réactionnel original a été proposé pourla formation de ces produits. / This work is focused on the research and development of new pharmacologicalmolecules in naphthoquinonic series, synthesized by single electron transfer reaction SRN1 ormanganese(III) acetate catalyzed oxidative radical cyclization. The first part describes the SRN1reactivity of 2-(chloromethyl)-3-methoxynaphthoquinone with various nitronate anions leading to theC-alkylation products. The reduction-cyclization reaction of the latter derivatives allowed us to obtainnew benzo[g]indol-5(3H)-one derivatives. In the second part, a new reaction initiated by Mn(OAc)3 on2-hydroxy-3-methylnaphthoquinone was developed under mild conditions. Indeed, the original reaction of2-hydroxy-3-methylnaphthoquinone with various aromatic alkenes in presence of dioxygen led to newdihydronaphtho[2,3-c][1,2]dioxine-5,10(3H,10aH)-dione derivatives as a mixture of diastereoisomerswith antimalarial potential. An original mechanism was proposed in order to explain the formation ofthese products.
7

Accès original aux hétérocycles par la catalyse organométallique : développement de nouveaux inhibiteurs de kinases / Original access to heterocycles through organometallic chemistry : development of selective kinases inhibitors

Mariaule, Gaëlle 28 November 2014 (has links)
Cette thèse est composée de deux parties distinctes ayant comme thématique commune, la synthèse d’hétérocycles via la catalyse organométallique.Nous nous sommes intéressés, dans un premier temps, à une voie de synthèse permettant un accès rapide au squelette tétrahydrocyclopenta[c]acridine. Ces composés polyfonctionnalisés sont obtenus très efficacement en seulement trois étapes dans des conditions particulièrement douces. L’étape clé de cette synthèse est une réaction de Pauson-Khand intramoléculaire catalysée au cobalt. Certains composés issus de la famille des tétrahydrocyclopenta[c]acridines présentent une activité d’inhibition sélective envers les kinases dépendantes des cyclines (CDKs), et plus particulièrement la CDK2. Un composé chef de file est identifié, puis grâce aux données de co-Cristallisation avec CDK2 et de modélisation moléculaire, suivi de l’étude des relations structure-Activité, la conception rationnelle d’une deuxième génération de molécules est rendue possible. Le composé le plus avancé présente une CI50 de 300 nM envers CDK2/cyclin A et un excellent profil de stabilité métabolique.Dans un deuxième temps, nous avons étudié et développé une réaction tandem d’addition/cyclisation catalysée par l’argent, avec des nucléophiles carbonés sur des substrats ortho-Alcynylbenzaldéhydes. La stratégie de synthèse conduit à des dérivés 1H-Isochromènes par création de deux nouvelles liaisons (C-C et C-O). Une étude approfondie de la réaction tandem nous a permis d’obtenir une large gamme de dérivés d’isochromènes en mettant en évidence l’influence de différents substituants, portés par le groupement alcyne ou le substrat, ainsi que l’utilisation de différents nucléophiles carbonés (alcynes, aromatiques, hétéroaromatiques). Les limitations de la réaction tandem ont également pu être identifiées. / My thesis proJect is organized around two main topics having in common organometallic chemistry and the synthesis of heterocycles.Firstly, we were interested in a methodology for the synthesis of tetrahydrocyclopenta[c]acridines. These compounds are synthesized in three steps from various quinolines. The key step is a cobalt-Catalyzed intramolecular Pauson-Khand reaction. Some compounds of this family exhibit selective Cyclin Dependent Kinases (CDKs) inhibition, particulary against CDK2, in the submicromolar range. A hit compound has been identified, and then using data from co-Crystallization with CDK2 and molecular modeling, followed by the study of structure-Activity relationships, the rational design of a second generation of molecules has been investigated. The most advanced compound has an IC50 of 300 nM against CDK2/cyclin A with an excellent metabolic profile. In the second axis of research, we have studied and developed a new silver-Catalyzed tandem addition/cyclization reaction with carbon nucleophiles. The systems studied are (hetero)aromatics compounds having an aldehyde group and in ortho-Position an alkynyl group. The synthetic strategy leads to 1H-Isochromene derivatives by creating two new bonds. A thorough study of the tandem reaction allowed us to obtain a wide range of isochromene derivatives, highlighting the influence of different substituents carried by the alkyne group or on the (hetero)aromatic substrates; and also to investigate the use of different carbon nucleophiles (alkynes, aromatics and heteroaromatics). The limitations of the tandem reaction have also been identified.

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