Amino Aacohols : stereoselective synthesis and applications in diversity-oriented synthesis

Torssell, Staffan

January 2005

This thesis is divided into three separate parts with amino alcohols as the common feature. The first part describes the development of a novel three-component approach to the synthesis of α-hydroxy-β-amino esters. Utilizing a highly diastereoselective Rh(II)-catalyzed 1,3-dipolar cycloaddition of carbonyl ylides to various aldimines, syn-α-hydroxy-β-amino esters formed in high yields and excellent diastereoselectivities. This methodology was also applied in a short enantioselective synthesis of the C-13 side-chain of Taxol. The second part of the thesis describes a total synthesis of D-erythro- Sphingosine based on a cross-metathesis approach to assemble the polar head group and the aliphatic chain. The last part deals with the application of amino alcohols as scaffolds in a diversity-oriented protocol for the development of libraries of small polycyclic molecules. The design of the libraries is based on the iterative use of two powerful ring-forming reactions; a ring-closing metathesis and an intramolecular Diels-Alder reaction, to simultaneously introduce structural complexity and diversity. / QC 20101222

Organic chemistry

amino alcohol

carbenoid

carbonyl ylide

cross-metathesis

diastereoselective

1

3-dipolar cycloaddition

sphingosine

Organisk kemi

Organic Chemistry

Organisk kemi

Dipyrazolylphosphanes in Condensation and P–N/P–P Bond Metathesis Reactions

Schoemaker, Robin

13 October 2020

Phosphorus plays a crucial role in modern p-block chemistry.1 One reason for that is the diagonal relationship between phosphorus and carbon.2 Comparable to carbon and its chemistry, phosphorus tends to form homoatomic bonds, which is explainable by the relatively high P–P single bond energy (ca. 200 kJ/mol).3 Thus, a plethora of poly-phosphorus compounds are reported in the last decades comprising of fascinating bonding motifs4 and interesting applications in coordination5-7 and synthetic8-11 chemistry, as well as in ligand design.12,13 A crucial point in the chemistry of polyphosphanes is of course the formation of P–P bonds. Numerous synthetic procedures are established and reviewed including salt metathesis,4a,14 dehalosilylation15 and dehalostannylation16 reactions, base promoted dehydrohalogenation reactions17 and dehydrogenative coupling reactions mediated by main group compounds18 or catalysis by transition metals.5,19 Moreover, dialkylamino-substituted phosphanes are used in condensation reactions to form P–P bonds since the early 1960’s. Yet these reactions need elevated temperatures, somewhat limiting the formation of polyphosphorus compounds as stated by the few examples reported.17d,20 The application of pyrazolyl-substituted phosphanes in P–P bond formation reactions is a relatively young field of research.21 Their synthesis and general chemical behavior as well as advantages in comparison to dialkylamino-substituted phosphanes is discussed in the following chapter.

info:eu-repo/classification/ddc/540

ddc:540

Controlled Synthesis and Characterization of Branched, Functionalized, and Cyclic Polymers

Chavan, Vijay S.

10 August 2011

No description available.

Polymers

Anionic Polymerization

Cationic Polymerization

Ring Opening Metathesis Polymerization

ATRP

Hydrosilation

Functionalization

Electrospinning

Star Polymers

Branched Polymers

Deuterated Polymers

Cyclic Polymers

AFM

GPC

DSC

TGA

MALDI-TOF

Oligopeptide-functionalized Graft Copolymers: Synthesis and Applications in Nucleic Acid Delivery

Breitenkamp, Rebecca Boudreaux

01 February 2009

Utilizing the diverse functionality of amino acids, a new class of amphiphilic graft copolymers has been synthesized, characterized, and explored for applications in biomaterials and nucleic acid delivery. This thesis research focused on the syntheses of oligopeptide-functionalized polyesters and polyolefins. Polyester functionalization was geared towards applications in biomaterials, tissue engineering, and drug delivery by incorporating sequences that promote cell-adhesion. These polyester- graft -oligopeptide materials were prepared by a 1,3-Huisgen cycloaddition reaction, "click" chemistry, of an azide-terminated oligopeptide (prepared by Fmoc-based solid phase peptide synthesis (SPPS)) and alkyne-containing polyester (synthesized by ring-opening polymerization). Following the syntheses of these materials, they were analyzed by nuclear magnetic resonance (NMR) and organic gel permeation chromatography (GPC). The oligopeptide-functionalized polyolefins were designed for nucleic acid complexation, and therefore the oligopeptide sequences were intended to incorporate positively-charged moieties ( e.g. , oligolysine) for DNA and short interfering RNA (siRNA) complexation. These graft copolymers, prepared by SPPS followed by ring-opening metathesis polymerization, have highly tunable structures that enable control over charge density and polymer backbone rigidity. Moreover, non-ionic hydrophilic grafts such as polyethylene glycol were integrated into these polyelectrolytes such that the charges along the polymer backbone are spaced accordingly while maintaining the hydrophilicity of the polymer. While numerous applications for such charged, "bio-tailored" materials can be envisioned, this work is geared towards positively-charged polyelectrolytes for their potential application in nucleic acid therapy, specifically the delivery of plasmid DNA and siRNA. These graft copolymers were characterized ( 1 H, 13 C NMR, organic and aqueous GPC), studied for their solution properties (static and dynamic light scattering), and investigated as polyplexes with plasmid DNA.

Amphiphilic graft copolymers

Functionalized polyesters

Gene delivery

Nucleic acid delivery

Oligopeptides

Ring-opening metathesis polymerization

Materials Science and Engineering

Polymer and Organic Materials

Studien zur Synthese von Jatrophan-Diterpenen / Enantioselektive Synthese von (-)-15-Acetyl-3-propionyl-17-norcharaciol / Towards the synthesis of Jatrophane-diterpenes / Synthesis of the Norjatrophane Diterpene (-)-15-Acetyl-3-propionyl-17-norcharaciol

Helmboldt, Hannes

02 May 2006

Es wird die enantioselektive Synthese eines substituierten Cyclopentanfragmentes beschrieben, welches zur Synthese einer Vielzahl von Diterpenen aus Euphorbiaceae genutzt werden kann. Schlüsselschritt hierbei ist eine intramolekulare Carbonyl-En-Reaktion. In zwei verschiedenen Syntheseansätzen wurde versucht, dieses zu einem Jatrophan-Diterpen umzusetzen. Versuche hinsichtlich einer Nozaki-Hiyama-Kishi-Kupplung werden beschrieben. Im zweiten Ansatz, wurde über eine Ringschlussmetathese bzw. eine Relay-Ringschlussmetathese versucht entsprechende Jatrophane herzustellen. Dies gelang bei einem Substrat, welches eine zweifach substituierte Doppelbindung beinhaltet. Somit konnte ein nichtnatürliches 17-Norjatrophan enantioselektiv synthetisiert werden. / The enantioselective synthesis of a highly substituted cyclopentan, useful for the synthesis of diterpenes from Euphorbiaceae is described. Key step is a intramolecular carbonyl-en reaction. Two different approaches towards Jatrophanes were examined. The first one envisioning a Nozaki-Hiyama-Kishi coupling didn´t work. The second one employed a ring-closing-metathesis which was successful in the case of a disubstituted double bond formed. The use of an relay-ring-closing-metathesis was also examined. The enantioselective synthesis of a nonnatural 17-Norjatrophane is described in all details.

Carbonyl-En

Characiol

Cyclopentan

Euphorbia

Jatrophane

Nozaki-Hiyama-Kishi

RCM

RRCM

Relay-Ringschlussmetathese

Ringschlussmetathese

Totalsynthese

enantioselektiv

Characiol

Jatrophanes

Nozaki-Hiyama-Kishi

RCM

RRCM

carbonyle en

cyclopentanes

euphorbia

relay-ring-closing-metathesis

ring-closing-metathesis

total synthesis

ddc:540

rvk:VK 8507

Asymmetrische Synthese

Cyclopentan

Diterpene

Kupplungsreaktion

Ringschlussmetathese

Wolfsmilch

Studien zur Synthese von Jatrophan-Diterpenen: Enantioselektive Synthese von (-)-15-Acetyl-3-propionyl-17-norcharaciol

Helmboldt, Hannes

30 May 2006

Es wird die enantioselektive Synthese eines substituierten Cyclopentanfragmentes beschrieben, welches zur Synthese einer Vielzahl von Diterpenen aus Euphorbiaceae genutzt werden kann. Schlüsselschritt hierbei ist eine intramolekulare Carbonyl-En-Reaktion. In zwei verschiedenen Syntheseansätzen wurde versucht, dieses zu einem Jatrophan-Diterpen umzusetzen. Versuche hinsichtlich einer Nozaki-Hiyama-Kishi-Kupplung werden beschrieben. Im zweiten Ansatz, wurde über eine Ringschlussmetathese bzw. eine Relay-Ringschlussmetathese versucht entsprechende Jatrophane herzustellen. Dies gelang bei einem Substrat, welches eine zweifach substituierte Doppelbindung beinhaltet. Somit konnte ein nichtnatürliches 17-Norjatrophan enantioselektiv synthetisiert werden. / The enantioselective synthesis of a highly substituted cyclopentan, useful for the synthesis of diterpenes from Euphorbiaceae is described. Key step is a intramolecular carbonyl-en reaction. Two different approaches towards Jatrophanes were examined. The first one envisioning a Nozaki-Hiyama-Kishi coupling didn´t work. The second one employed a ring-closing-metathesis which was successful in the case of a disubstituted double bond formed. The use of an relay-ring-closing-metathesis was also examined. The enantioselective synthesis of a nonnatural 17-Norjatrophane is described in all details.

info:eu-repo/classification/ddc/540

ddc:540

Investigations of the type ii intramolecular Diels-Alder reaction directed toward natural product synthesis

Muscroft-Taylor, Andrew Clive

January 2006

This thesis describes synthetic studies directed towards the total synthesis of the nakafuran and florlide marine natural products. Chapter One provides an overview of the importance of natural products to current medicinal chemistry and describes how the "supply issue" associated with these biologically derived compounds can be resolved through the process of total synthesis. Two families of marine natural products, the nakafurans and the florlides, are introduced as synthetic targets and strategies utilising a type II intramolecular Diels-Alder (IMDA) reaction to achieve their total synthesis are delineated. The efficient preparation of regio- and stereodefined vinyl coupling fragments via hydrostannylation and hydrohalogenation methodology is described in Chapter Two. The palladium-catalysed cross-coupling of these fragments, via Stille or Negishi coupling methodology, yielded dienes which were successfully advanced to IMDA triene precursors. Chapter Three describes investigation of the type II IMDA reaction to give bicyclo[4.3.1]decene carbocyclic skeletons. A facile acid-catalysed 6,7-alkene to 7,8-alkene olefinic isomerisation, via a proposed oxonium intermediate, and the inability to appropriately functionalise the desired adducts impeded progress along the synthetic route. Molecular modelling was conducted to investigate the causes of this unexpected reactivity. Investigations in Chapter Four describe the successful synthesis and cyclisation of homomethyl triene analogues prepared via application of enyne metathesis chemistry. The use of an exo-cyclopropylcarbinyl fragmentation was found to be unsuccessful as a means of installing the desired 6-methyl-bicyclo[4.3.1]decan-2-one core with a competing endo-ring expansion giving rise to a bicyclo[4.4.1]undecane ring system. Chapter 5 summarises the above results and gives a brief discussion of the future potential of this research to provide for a total synthesis of the nakafuran and florlide natural products.

IMDA

T2IMDA

Stille

Negishi

Hydrostannylation

Enyne metathesis

Radical Fragmentation

Natural product synthesis

Nakafuran

Xenolide

Florlide

Bicyclo[4.3.1]decane

Bicyclo[4.3.1]decanone

Bicyclo[5.3.1]undecanone

Design, synthesis and testing of β-strand mimics as protease inhibitors

Aitken, Steven Geoffrey

January 2006

Chapter 1 gives background information on proteases and discusses the concept of protease inhibition as a therapeutic strategy for humans. It introduces the key concept that conformation defines biological activity. It also outlines how proteases almost universally bind their substrate/inhibitors in an extended β-strand conformation. The use of calpain as a prototype protease for the testing of β-strand mimics synthesised later in the thesis is also discussed. Chapter 2 describes how molecular modeling was used to rationalise the structure based activity relationships (SAR) of known calpain inhibitors. Molecular modeling was then used to successfully design a number of acyclic β-strand mimics. The synthesis and testing of eight such inhibitors is described. The most potent β-strand mimic prepared was 2.13. This was determined to have an IC₅₀ of 30 nM against calpain II. Chapter 3 outlines the history and application of ring closing metathesis (RCM) to the synthesis of cyclic compounds. The attempted synthesis of an eight membered cyclic nitrogen to nitrogen conformationally constrained dipeptide is described. The synthesis of a conformationally constrained β-amino acid calpain inhibitor (3.73) is also described. A novel calpain inhibitor motif was designed in Chapter 4. On the basis of this an in-silico combinatorial library of two hundred and eighty eight possible β-strand templates was prepared. Conformational analysis of this library was performed and from this a number of excellent β-strand templates were identified and selected for synthesis. The preparation of ten β-strand templates is described. New microwave irradiation methodology was developed to achieve this. vii The formation of a six-membered catalyst deactivating chelate is also proposed to explain why some dienes fail to undergo RCM. Two methods to circumvent the formation of such a chelate are outlined. The addition of Lewis acid chloro-dicyclohexyl borane to the RCM reaction mixture and chain length alteration are investigated. Chapter 5 describes the design of macrocyclic β-strand mimics using induced fit molecular modelling. The physicochemical properties of these were calculated in-silico. From this analysis a number of Tyr-XX-Gly based and Tyr-XX-Cys based macrocyclic calpain inhibitors were selected for synthesis. The preparation and testing of these are described. In the Tyr-XX-Gly macrocyclic system a number of variables were investigated and numerous SAR implications concluded. Aldehyde 5.14 was identified as the best electrophilic warhead macrocyclic calpain inhibitor with an IC₅₀ against calpain II of 27 nM. The best non-electrophilic warhead macrocycle (5.13) had an IC₅₀ against calpain II of 704 nM. Chapter 6 describes synthetic optimisation for the preparation of calpain inhibitors 2.13, 5.14 and 5.17. Multi-gram quantities of each were prepared. Aldehydes 2.13 and 5.14 were evaluated as anti-cataract agents using in-vivo cataract sheep model. Both of these β-strand mimics were demonstrated to retard cataract development. Macrocycle 5.14 was found to be the most effective, decreasing the rate of cataract development between forty four and forty nine per cent relative to control. Chapter 7 outlines the attempted development of RCM methodology for the chiral synthesis of α-α disubstituted amino acid lactams. In addition, methodology for the stereoselective incorporation of a C-N constrained β-amino acid carbocycle into a peptide or peptidomimetic is described.

Beta-strand

Peptidomimetics

drug design

calpain inhibitors

protease inhibitors

computational chemistry

molecular modeling

ADME

Cataract

anti-cataract drugs

Beta-strand mimic

SAR

structure activity relationships

RCM

ring closing metathesis

Étude de réactivité et de sélectivité de nouveaux catalyseurs à base de ruthénium

Stenne, Brice

08 1900

Ce projet de recherche consiste en l’étude de la réactivité et de la sélectivité de nouveaux catalyseurs de métathèse d’oléfines à base de ruthénium lors de réaction de fermeture de cycle par métathèse d’oléfines (RCM). L’emphase de cette étude repose sur l’évaluation de nouveaux catalyseurs possédant un ligand NHC (carbène N-hétérocyclique) C1-symétrique développés par le laboratoire Collins pour des réactions de désymétrisations asymétriques de méso-triènes par ARCM. Le projet a été séparé en deux sections distinctes. La première section concerne la formation d’oléfines trisubstituées par ARCM de méso-triènes. La seconde section consiste en la formation d’oléfines tétrasubstituées par le biais de la RCM de diènes et de la ARCM de méso-triènes. Il est à noter qu’il n’y a aucun précédent dans la littérature concernant la formation d’oléfines tétrasubstituées suite à une désymétrisation par ARCM. Lors de l’étude concernant la formation d’oléfines trisubstituées, une étude de cinétique a été entreprise dans le but de mieux comprendre la réactivité des différents catalyseurs. Il a été possible d’observer que le groupement N-alkyle a une grande influence sur la réactivité du catalyseur. Une étude de sélectivité a ensuite été entreprise pour déterminer si le groupement N-alkyle génère aussi un effet sur la sélectivité des catalyseurs. Cette étude a été effectuée par l’entremise de réactions de désymétrisation d’une variété de méso-triènes. En ce qui a trait à la formation d’oléfines tétrasubstituées, une étude de la réactivité des différents catalyseurs a été effectuée par l’intermédiaire de malonates de diéthyldiméthallyle. Il a encore une fois a été possible d’observer que le groupement N-alkyle possède un effet important sur la réactivité du catalyseur. Une étude de sélectivité a ensuite été entreprise pour déterminer si le groupement iv N-alkyle génère aussi un effet sur la sélectivité des catalyseurs. Cette étude a été effectuée par l’entremise de réactions de désymétrisation de différents mésotriènes. / This research consists in the study of the reactivity and selectivity of new chiral Ru-based olefin metathesis catalysts in ring-closing metathesis (RCM) reactions. The study focused on evaluating new catalysts possessing C1- symmetric NHC (N-heterocyclic carbene) ligands developed in our laboratories for asymmetric desymmetrization reactions of meso-trienes. The research was divided into two distinct sections, the first concerns the asymmetric ring closing metathesis (ARCM) processes that form trisubstituted olefins from meso-trienes. The second concerns the RCM and ARCM processes that form tetrasubstituted olefins from meso-trienes. It can be observed that there is no precedent in the literature concerning the formation of tetrasubstituted olefins via ARCM. During the investigation concerning the formation of trisubstituted olefins, a kinetic study was done to have better understanding of the catalyst selectivity. With this study in hand, it was possible to observe the effect induced by the N-alkyl group on the catalysts’ reactivity. A selectivity study was done to observe if the Nalkyl group could affects the catalysts’ selectivity. These investigations were done using a variety of meso-trienes in desymmetrization reactions to afford trisubstituted olefins. Concerning the formation of tetrasubstituted olefins, the catalysts’ reactivity was investigated in RCM processes involving diethyldimethallyl malonates. Once again, an effect induced by the N-alkyl group was observed concerning the reactivity of the catalysts. A selectivity study was performed. As for ARCM processes forming trisubstituted olefins, the N-alkyl group also had an impact on the selectivity of the catalysts. This investigation was done with ARCM desymmetrization of meso-trienes.

métathèse d'oléfines

RCM

ARCM

désymétrisation

oléfines tétrasubstituées

C1-symmetric N-heterocyclic carbenes

olefin metathesis

RCM

ARCM

desymmetrization

tetrasubstituted olefins

Synthèse énantiosélective du [7]hélicène à l’aide de la réaction de fermeture de cycle par métathèse d’oléfine asymétrique et synthèse de binaphtols via une réaction de couplage oxydatif

Grandbois, Alain

08 1900

L’intérêt pour les hélicènes s’est accru au fur et à mesure que de nouvelles applications pour ce genre de molécules ont été découvertes. Par contre, la recherche dans ce domaine a été limitée par le petit nombre de voies de synthèse de ces molécules, la plupart nécessitant une étape de résolution ou de séparation des énantiomères par HPLC à la fin de la synthèse. Le présent projet de recherche propose d’utiliser la réaction de fermeture de cycle asymétrique par métathèse d’oléfines (asymmetric ring closing metathesis, ARCM) pour effectuer une synthèse d’hélicène à la fois catalytique et énantiosélective. La synthèse énantiosélective du [7]hélicène a été effectuée à l’aide d’une résolution cinétique du précurseur racémique. Au cours de cette synthèse, nous avons été en mesure de démontrer l’efficacité de différents catalyseurs de métathèse chiraux en plus de démontrer l’effet de l’ajout de simples oléfines comme additifs à la réaction. De plus, nous avons formulé une hypothèse expliquant cet effet à l’aide du mécanisme de la réaction. Finalement, nous avons aussi montré l’effet du changement de solvant sur la sélectivité de la réaction. Au cours de ces travaux, nous avons également développé une nouvelle méthode de synthèse de binaphtols à l’aide d’une réaction de couplage oxydatif impliquant un catalyseur de cuivre. À l’aide d’études de réactivité, nous avons été en mesure de démontrer que le métal portait deux ligands N-hétérocycliques (NHC). Nous avons aussi observé que le catalyseur favorisait la formation de binaphtol non symétrique avec un groupement naphtol avec une densité électronique élevée et un autre groupement naphtol avec une faible densité électronique. / The interest in helicenes has increased as new potential applications have been proposed for these twisted conjugated aromatics. However, further research is limited by the lack of methods for the enantioselective synthesis of helicenes. The current traditional syntheses often conclude with a resolution, most often via separation on a chiral stationary phase. This thesis describes the development of new catalytic method for the synthesis of helicenes using ring closing metathesis (RCM) employing highly reactive Ru-based catalysts or commercially available catalysts and microwave heating. Furthermore, an enantioselective variant of the asymmetric ring closing metathesis (ARCM) reactions was developed for the synthesis of enantioenriched [7]helicene via a kinetic resolution protocol. The development of the kinetic resolution involved the preparation and screening of a number of novel chiral Ru-based olefin metathesis catalysts. During these studies, the beneficial effect of simple olefins additives on the selectivity of the reaction was observed and a hypothesis to explain these effects has been proposed. In addition, intriguing solvent effects were also observed. Lastly, this thesis describes the investigation of a new method for the preparation of binaphthol via an oxidative coupling with a novel copper catalyst bearing two N-heterocyclic carbene (NHC) ligands. It was demonstrated that the cationic catalyst allowed for the formation of mixed oxidative couplings between electron rich and electron poor 2-naphthols to form C1-symmetric binaphthol derivatives.

Hélicène

Résolution cinétique

Catalyseur

Métathèse d'oléfines

ARCM

Couplage oxydatif

Cuivre

Binaphtol

NHC

Helicene

Kinetic resolution

Olefin metathesis

RCM

ARCM

Oxidative coupling

Copper

Binaphthols

NHC