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Sintese do fragmento C29-C39 da sangliferina A / Synthesis of the C29-C39 fragment of sanglifehrin ASalles Junior, Airton Gonçalves, 1977- 22 February 2006 (has links)
Orientador: Luiz Carlos Dias / Dissertação (mestrado) - Universidade Estadual de Campinas, Instituto de Quimica / Made available in DSpace on 2018-08-06T22:02:57Z (GMT). No. of bitstreams: 1
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Previous issue date: 2006 / Resumo: Este trabalho relata a síntese assimétrica do fragmento C29-C39 do potente imunossupressor sangliferina A. O plano sintético utiliza como etapa-chave a reação aldólica com indução 1,5-anti entre a metil cetona 7.3 e o aldeído 31.3(S). A metil cetona 7.3 foi obtida a partir da amida de Weinreb 10.3 utilizando como etapas principais, reação de Horner-Wadsworth-Emmons, epoxidação régio- e diastereosseletiva e abertura de epóxido com cuprato de alta ordem. A amida 10.3 foi obtida a partir da reação aldólica entre N-propioniloxazolidinona 12.3 e a metacroleína mediada por titânio e hidroboração diastereosseletiva. O rendimento total para obtenção do fragmento C29-C39 foi de 18% para 16 etapas. / Abstract: This work describes the stereoselective synthesis of the C29-C39 fragment of the immunosuppressant sanglifehrin A. Our strategy involved a diastereoselective boron-mediated 1,5-anti aldol reaction of methyl ketone 7.3 with chiral aldehyde 31.3(S) as the key step.j Methyl ketone 7.3 is viewed as arising from Weinreb amide 10.3. Key steps in this approach are Horner-Waddsworth-Emmons homologation, selective epoxidation and epoxide ring opening with a higher order cuprate. The Weireb amide 10.3 is available from a titanium mediated aldol reaction of N-propionyloxazolidinone 12.3 with metacrolein followed by a diastereoselective hydroboration. This approach to the C29-C39 fragment of sanglifehrin A requires 16 steps and produced the desired molecule in 18% overall yield. / Mestrado / Quimica Organica / Mestre em Química
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New oxy-dihydrofuran annulation methodologyBarbieri-Arhancet, Graciela I. 16 September 2005 (has links)
This work describes mechanistic studies concerning the addition of the dienolate derived from ethyl 2-bromocrotonate 11 to enones and aldehydes to yield vinylcyc1opropanes 12 and 13, and vinyloxiranes 14 respectively. The conditions that affect the generation of the lithium dienolate 16 from croton ate 11 and the dienolate composition have been investigated. The possibility of asymmetric induction using chiral auxiliaries located either at the ester site or at the r- position of 11 was addressed.
A new oxydihydrofuran annulation methodology was developed following the above investigation. The addition of the lithium dienolate generated from ethyl 2-bromo-4-[(tert-butyldimethylsilyl)oxy]-butenoate 105 to aldehydes provided vinyloxiranes of type 127 as single isomers. Vinyloxirane 127 was thermally rearranged to give dihydrofuran 141 as mixture of stereoisomers. Alternatively, 127 was converted to dihyrofuran via a new low temperature rearrangement. This rearrangement proceeded stereoselectively under mild conditions to give a single isomer of dihydrofuran 141 in good to excellent yields. Thus, the addition of the dienolate derived from 105 to aldehydes and the subsequent low temperature rearrangement of the vinyloxirane intermediate constitute a versatile new [2+3] dihydrofuran annulation. / Ph. D.
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Indução assimétrica remota na adição de enolatos de boro de metilcetonas quirais a adeídos quirais e aquirais / Remote asymmetric indusction in the addition of boron enolates of chiral methyl ketones to chiral and achirals adehydesPinheiro, Savio Moita 16 August 2018 (has links)
Orientador: Luiz Carlos Dias / Tese (doutorado) - Universidade Estadual de Campinas, Instituto de Química / Made available in DSpace on 2018-08-16T16:04:10Z (GMT). No. of bitstreams: 1
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Previous issue date: 2010 / Resumo: As reações aldólicas com enolatos de boro de metilcetonas quirais contendo o protetor p-metóxi- benzilideno cetal (105 e 106) levaram a obtenção do diastereoisômero com indução 1,5-anti em boas seletividades. A avaliação do processo de dupla-diastereosseletividade da metilcetona 105 mostrou que existe uma influência parcial por parte do aldeído no nível de seletividade. Reações aldólicas com metilcetonas acíclicas 1,2-syn-dissubstituídas contendo os grupos protetores PMB (108) e TBS (107) levaram ao isômero 1,5-anti em baixa seletividade. O emprego das metilcetonas contendo a relação 1,2-anti entre os seus estereocentros mostrou baixos níveis de indução 1,5-anti para a metilcetona 109 e 1,5-syn, para a metilcetona 110, eliminando a possibilidade de competição entre as induções 1,4-syn e 1,5-anti. Com o objetivo de compreender os fatores que controlam a reação aldólica, outros estudos estão em andamento no nosso grupo de pesquisas. / Abstract: We report herein that good to excellent levels of 1,5-anti stereoinduction are obtained in boron enolate aldol reactions of 1,2-syn -alkoxy methyl ketones with achiral aldehydes, when the b-alkoxy protecting group is part of a benzylidene ketal. The strong internal stereoinduction of the b-alkoxy stereocenter of the boron enolates dominates the overall stereochemical outcome of the corresponding aldol addition reactions, leading to the 1,5-anti products with good levels of diastereoselectivities. Even with the use of acyclic a-methyl-b-alkoxy methyl ketones, the b-stereocenter plays a dominant role in determining the sense of 1,5-anti asymmetric induction, although lower levels of diastereoselectivities were obtained. Due to the lower energy difference observed between transition states, it looks like a mismatched relationship case as a competition between 1,4-syn induction from the a-methyl stereocenter and 1,5-anti induction from the b-alkoxy stereocenter. The results showed a predominance of 1,5-induction in competition with 1,4-induction. / Doutorado / Quimica Organica / Doutor em Ciências
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Conception rationnelle, synthèse et caractérisation de composés à transition de spin chiraux / Rational design, synthesis and characterization of chiral spin crossover compoundsNaim, Ahmad 26 January 2016 (has links)
D'importants progrès ont été accomplis dans le domaine des matériaux à transition despin depuis leur première observation par Cambi en 1931. La combinaison de lachiralité avec le magnétisme résulte en de nouvelles propriétés très intéressantes quiouvrent la voie pour de potentielles applications technologiques. Ce manuscrit décritles résultats obtenus par diverses stratégies poursuivies vers des matériauxmoléculaires non-centrosymétriques à transition de spin par combinaison decomplexes à transition de spin avec des anions chiraux à symétries D3 et D2. / Many advancements in the field of spin crossover materials have been carried outsince the first observation by Cambi in 1931. The combination of chirality andmagnetism yields fascinating properties that open the way for potential technologicalapplications. Obtaining new non-centrosymmetric magnetic compounds yieldsinteresting subjects for non-linear optical studies or crystallography. This manuscriptdescribes the results obtained by various strategies pursued toward spin crossovernon-centrosymmetric molecular materials by combining spin crossover complexes withchiral anions based on D3 and D2 symmetric anions.
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Stereoselective intramolecular Michael addition reactions of pyrrole and their application to natural product synthesesBeck, Daniel Antony Speedie, beckautomatic@gmail.com January 2006 (has links)
Chapter one; (-)-Rhazinilam and (-)-Rhazinal: Alkaloids with Anti-mitotic Properties Derived from Kopsia teoi, provides the background information behind the motives that initiated this research project. The plant alkaloid (-)-rhazinilam [(-)-1] and its naturally-occurring derivative (-)-rhazinal [(-)-13] both exhibit potent anti-mitotic activities and, as such, are interesting targets for total synthesis. Chapter one is a review of the literature regarding these two compounds and discusses the occurrence, proposed biosynthetic origins, structural elucidation and biological activites of compound (-)-1 and that of its analogues including alkaloid (-)-13. Previous total syntheses of these two compounds are then examined, concluding with the only reported total synthesis of compound (-)-13. Developed within the Banwell research group, this total synthesis produced the racemic modification of alkaloid (-)-13 due to a lack of any stereocontrol in the key intramolecular Michael addition step. This unprecedented key step, involving cyclisation of the C2 of pyrrole onto an N-tethered and ?,?-disubstituted acrylate to produce a quaternary-carbon stereogenic centre, would be of greatly enhanced utility if it could be achieved in a catalytic-enantioselective fashion. The realisation of this goal is the central aim of the research conducted within this thesis.
¶
Chapter two; Investigating Asymmetric Induction in the Intramolecular Michael Addition of pyrrole to N-Tethered Acrylates and Related Species, introduces the model study used to direct research towards achieving the goal of asymmetric induction in the title process. The model is a somewhat simplified version of the original process used in the total synthesis of compound (-)-13 involving cyclisation of the C2 of pyrrole onto an N-tethered and ?-monosubstituted Michael acceptor, to produce a tertiary-carbon stereogenic centre. This simplification allows the rapid synthesis of a broad range of potential substrates for use in the title process, thus enabling the investigation of various different approaches to inducing asymmetry therein. High levels of asymmetric induction are observed with the use of chiral substrates or catalysts, facilitating the synthesis of both 6- and 7-membered rings annulated to pyrrole with construction of the relevant tertiary-carbon stereogenic centre in enantio-enriched form. For the reactions producing a 6-membered ring annulated to pyrrole, unambiguous proof of the absolute sense of asymmetric induction observed in the intramolecular Michael addition event is established using a chemical correlation study involving elaboration of a key indolizine-type cyclisation product, to the plant alkaloid of known absolute stereochemistry, (-)-tashiromine [(-)-75]. For the reaction producing a 7-membered ring annulated to pyrrole, the same information is obtained via X-ray crystallographic analyses of a dibrominated derivative of a key pyrroloazepine-type cyclisation product.
¶
Chapter three An Enantioselective Total Synthesis of the Alkaloid (-)-Rhazinal: An Anti-mitotic Agent Isolated from Kopsia teoi., focuses on the application of methodology developed in the previous chapter, to the original goal of inducing asymmetry in the intramolecular Michael addition reaction, involving cyclisation of the C2 of pyrrole onto an N-tethered and ?,?-disubstituted acrylate to produce a quaternary-carbon stereogenic centre. This is ultimately achieved in a catalytic-enantioselective fashion, resulting in the first such total synthesis of the anti-mitotic alkaloid (-)-rhazinal [(-)-13].
¶
Chapter four Extending the Reaction Manifold to the Syntheses of Related Natural Products: A Formal Total Synthesis of (+)-Aspidospermidine and Syntheses of (-)-Rhazinilam and (-)-Leuconolam from (-)-Rhazinal, describes three extensions to the reaction manifold used in the enantioselective total synthesis of alkaloid (-)-13:
The acquisition in an enantioselective manner, of an intermediate previously obtained in racemic form, en route to the racemic modification of the natural product (±)-aspidospermidine [(±)-134], constitutes a formal and enantioselective total synthesis of (+)-aspidospermidine
[(+)-134].
The direct deformylation of (-)-rhazinal [(-)-13], is carried out, to produce the parent alkaloid
(-)-rhazinilam [(-)-1].
The pyrrole ring present in (-)-rhazinilam [(-)-1] is oxidised, to produce the related natural product (-)-Leuconolam [(-)-12] which has not, hitherto, been prepared by total synthesis.
¶Chapter five contains the experimental procedures and characterisation data associated with compounds described in chapters two to four.
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Stereoselective Nucleophilic Additions to Aldehydes and Synthesis of α-Amino-β- Hydroxy-EstersDanielsson, Jakob January 2012 (has links)
This thesis deals with the development of new reaction methodology as well as stereochemical investigations. The first part concerns the investigation of 1,2- and merged 1,2- and 1,3- asymmetric induction in Mukaiyama aldol additions to α-heteroatom and α,β- heteroatom substituted aldehydes respectively. In particular, the unexpected 1,2-syn selectivity obtained in the addition of sterically hindered nucleophiles to α-chloroaldehydes is examined, and an explanation for the observed stereochemical trends is proposed. The second part describes the development of a novel entry to α-amino-β- hydroxy esters by a 1,3-dipolar cycloaddition reaction of aldehydes and azomethine ylides, generated by thermolysis of aziridines. The third part deals with our efforts to develop a novel entry to vicinal all- carbon quaternary centers, based on an intramolecular domino Heck- carbonylation reaction using tetrasubstituted olefins. / QC 20120611
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