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Síntese total do (-)-criptocariol A / Total synthesis of (-)-criptocariol AKuroishi, Paula Kishi, 1989- 12 March 2014 (has links)
Orientador: Luiz Carlos Dias / Dissertação (mestrado) - Universidade Estadual de Campinas, Instituto de Química / Made available in DSpace on 2018-08-26T10:31:22Z (GMT). No. of bitstreams: 1
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Previous issue date: 2014 / Resumo: Os criptocarióis A-H foram isolados em 2011 por Gustafson e colaboradores. Esses compostos apresentaram uma promissora atividade contra o câncer por serem capazes de estabilizar Pdcd4, uma proteína supressora de tumor. Neste trabalho, foi concluída a síntese total do enantiômero do criptocariol A em 17 etapas e 0,1% de rendimento (rota linear mais longa) a partir do (R)-penten-2-ol. As etapas chave dessa rota foram reações aldólicas mediadas por boro, assim como reduções estereosseletivas que permitiram a instalação de todos os seis estereocentros presentes na molécula. Além disso, realizamos a reação de Horner-Wadsworth-Emmons utilizando o protocolo de Ando para obter a olefina Z presente no anel a-pirona. Nas etapas finais da síntese, foram observados baixos rendimentos. Sendo assim, foram realizados estudos de modo a tentar otimizar essas condições reacionais utilizando substratos modelo. Embora as condições otimizadas tivessem sido apropriadas para os compostos modelos, elas não se mostraram efetivas para o substrato real / Abstract: Cryptocaryols A-H were isolated in 2011 by Gustafson and coworkers. These compounds have notable anticancer activity because of their ability to stabilize tumor suppressor protein Pdcd4. In this work, the total synthesis of the enantiomer of cryptocaryol A was completed in 17 steps and 0.1% yield (longest linear sequence) starting from (R)-penten-2-ol. The key steps are comprised of boron-mediated aldol reactions and stereoselective reductions allowing the installation of all six stereocenters present in the molecule. In addition, we performed a Horner-Wadsworth-Emmons reaction using Ando's protocol to obtain the Z-alkene present in the a-pyrone ring. The final steps of the synthesis were low yielding; thus, we attempted to optimize the reaction conditions with model substrates. Although the optimized conditions worked well for the model compounds, they were ineffective for the actual substrate. / Mestrado / Quimica Organica / Mestra em Química
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Synthèse stéréosélective de 1,3-polyols - synthèse du (+)-cryptocaryol A et du squelette carboné de la filipine III / Stereoselective synthesis of 1,3-polyols - synthesis of (+)-cryptocaryol A and synthesis of the carbon skeleton of filipin IIIBrun, Elodie 09 November 2015 (has links)
Les motifs 1,3-polyols sont fréquemment rencontrés dans de nombreuses molécules naturelles biologiquement actives. Cependant, à ce jour, il n'existe que peu de méthodes générales et efficaces permettant d'accéder à ces motifs de manière stéréocontrôlée. Nous nous sommes particulièrement intéressés à la synthèse de 1,3,5,7-tétraols et une méthode a été mise au point pour former ces composés en utilisant deux cyclisations de Prins successives suivies d'une coupure réductrice du bis-tétrahydropyrane obtenu. Cette méthode permet d'accéder à tous les diastéréoisomères des tétraols efficacement et elle a été appliquée avec succès à la synthèse du (+)-cryptocaryol A, un composé polyhydroxylé stabilisant PdCd4, qui est une protéine inhibant le développement cellulaire. Par ailleurs, nous avons développé une approche synthétique de la filipine III, un macrolide naturel possédant des propriétés antibiotiques et antifongiques, et comportant un fragment 1,3-polyol et un fragment pentaénique. Plusieurs stratégies ont été envisagées afin d'accéder à ces deux fragments, qui ont été synthétisés de manière convergente. Leur assemblage a été réalisé grâce à une réaction d'aldolisation diastéréosélective et nous avons pu accéder au squelette carboné complet de la filipine III. / 1,3-Polyols are present in a large variety of biologically active natural products. However, right now only a few general and efficient methods have been described to access these compounds in a stereocontrolled manner. We were particularly interested in the synthesis of 1,3,5,7-tetraols and a method has been developed to prepare these compounds, using two successive Prins cyclizations followed by a reductive cleavage of the resulting bis-tetrahydropyran. This efficient method allows the access to all the diastereomers of these tetraols and has successfully been applied to the synthesis of (+)-cryptocaryol A, a polyhydroxylated compound which stabilizes PdCd4, a protein inhibiting the cellular growth. We have also developed a synthetic approach toward filipin III, an antibiotic and antifungal macrolide, which possesses a 1,3-polyol part and a pentaenic part. Several strategies have been envisaged to construct these fragments, which have been synthesized in a convergent manner. These fragments were then coupled using a diastereoselective aldolisation and we were able to access the complete carbon skeleton of filipin III.
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