Syntéza a studium vlastností derivátů tetrathiofulvalenu / The tetrathiofulvalene derivatives: Their synthesis and properties

Nejedlý, Jindřich

January 2012

The goal of the diploma thesis was to prepare a spectrum of electron-rich macrocyclic derivatives of tetrathiafulvalene (TTF), which should serve as electron donors in interactions with electron-deficient acceptor molecules. A two-step synthesis was used for their preparation. First, a non-cyclic three-segment precursor was prepared by a reaction of a thiolate TTF construction block with a bis(bromomethyl)aromate. Then, a reaction of this precursor with another molecule of bis(bromomethyl)derivative closed the macrocycle. The latter reaction produced mainly [2+2] macrocycles containing two TTF and two aromatic units. In most cases, larger [4+4] macrocycles were also isolated from the reaction mixture. Besides thiolate TTF unit two other thiolate units, one with extended TTF core and other with smaller trithiafulvene ring, were used analogically in synthesis. By a combination of three thiolate blocks and five bis(bromomethyl)aromates 11 three-segment components were prepared and these were converted to 11 structural types of macrocycles with [2+2] and 7 macrocycles with [4+4] stoichiometry. The resulting macrocycles were characterized by 1 H a 13 C NMR spectroscopy and analyzed by a gel permeation chromatography. Their structures were also confirmed by high-resolution mass spectroscopy. Interaction...

Etudes sur la catalyse de la réaction de Huisgen et nouvelles applications synthétiques

Elamari, Hichem

25 May 2011

Au cours de ce travail, nous avons effectué une étude méthodologique pour la préparation de banques de triazoles, en utilisant la réaction de la chimie " clic ". Ces études ont démontré que la réaction entre un alcyne vrai activé et un azoture est possible dans les conditions sans solvant et sans catalyseur pour conduire un mélange d'isomères 1,4 et 1,5 avec un rendement moyen de 76%. Nous avons remarqué que l'addition des métaux (SiO2, MgCl2, Al2O3, FeCl3 et CuCl2) permettait d'améliorer les rendements des réactions, et on a observé que la silice est la meilleur catalyseur, alors que la catalyse au cuivre (I) donne une sélectivité complète pour l'isomère 1,4. Ce résultat est bien confirmé par l'étude de la régiosélectivité qui montre que les molécules contenant deux types d'alcynes (activé et non activé) peuvent êtres fonctionnalisés séquentiellement et sélectivement. Nous avons aussi préparé les bis-triazoles en deux étapes : la première sur l'alcyne activé sans catalyseur et la deuxième étape se fait sur l'alcyne non activé par catalyse au cuivre (I), ce qui permet de dire que les alcynes terminaux portant un groupement carbonyle en  de la triple liaison sont beaucoup plus réactifs.Nous avons également pu étendre l'application de la catalyse supportée dans la réaction de Huisgen dans les domaines de la synthèse de dérivés de produits naturels et d'éthers couronne. En utilisant la synthèse classique et en flux continu, nous avons pu préparer des structures originales dérivées de l'acide quinique porteuse de cycles triazoliques. Ces composés seront testés pour leur activité biologique. Nous avons également entrepris la synthèse de dérivés nouveaux d'éthers couronnes azotes afin d'incorporer à ces structures des bras contenant un ou deux noyaux triazoles. L'obtention de ces substances permettra d'ouvrir l'étude de leur propriétés complexantes dans l'avenir

Catalyseurs supportés

Chimie click

Triazoles

Synthèse chimiosélective

Chimie en flux continu

Macrocycles triazoliques

Synthesis, Characterization, and Self-Assembly of Gold Nanorods and Nanoprisms

Tran, Kristina L.

29 June 2010

The unique properties of gold nanoparticles make them excellent candidates for applications in electronics, sensing, imaging, and photothermal therapy. Though abundant literature exists for isotropic gold nanoparticles, work on nanoparticles of different shapes has been gaining interest recently. Anisotropic gold nanoparticles, such as nanorods and nanoprisms, have tunable optical properties in the visible and near-infrared regions. Through synthesis and surface modification, the production of various shapes of these gold nanoparticles can be controlled to meet different applications. Two different types of gold nanorods were used in this thesis. The first type was stabilized with cetyltrimethylammonium bromide (CTAB) and had aspect ratios of 3-4 (defined as the nanorod length divided by the diameter). The second type was synthesized using CTAB and benzyldimethylhexadecylammonium chloride (BDAC) in a binary surfactant system which produced aspect ratios greater than 4. The nanorods were characterized with UV-Vis spectroscopy and transmission electron microscopy (TEM). Two types of bowl-shaped macrocyclic compounds called resorcinarenes were used to direct self-assembly of the nanorods. The first type of resorcinarene (R2S) consisted of thiol(SH)-terminated alkyl chains on both rims. The second type (R1S) contained thiol-terminated alkyl chains on only one rim. The monolayer formation of these resorcinarenes on planar gold surfaces was studied and characterized by FTIR spectroscopy. Resorcinarene-mediated assembly of gold nanorods was monitored with UV-Vis spectroscopy, dynamic light scattering (DLS), and TEM. In addition to gold nanorods, gold nanoprisms were synthesized through a kinetically-controlled reduction route in the presence of CTAB. The linking of nanoprisms using resorcinarenes was also explored.

resorcinarenes

macrocycles

anisotropic gold nanoparticles

metal nanoparticles

binary surfactant synthesis

American Studies

Arts and Humanities

Chemical Engineering

The Design, Synthesis and Biological Assay of Cysteine Protease Specific Inhibitors

Mehrtens (nee Nikkel), Janna Marie

January 2007

This thesis investigates the design, synthesis and biological assay of cysteine protease inhibitors within the papain superfamily of cysteine proteases. This is achieved by examining the effect of inhibitor design, especially warheads, on IC₅₀ values and structureactivity relationships between cysteine protease inhibitors of the papain superfamily. The representative proteases used are m-calpain, μ-calpain, cathepsin B and papain. Chapter One is an introductory chapter; Chapters Two-Four describe the design and synthesis of cysteine protease inhibitors; Chapter Five discusses assay protocol; and Chapter Six contains the assay results and structure-activity relationships of the synthesised inhibitors. Chapter One introduces cysteine proteases of the papain family and examines the structure, physiology and role in disease of papain, cathepsin B, m-calpain and μ-calpain. The close structural homology that exists between these members of the papain superfamily is identified, as well characteristics unique to each protease. Covalent reversible, covalent irreversible and non-covalent warheads are defined. The generic inhibitor scaffold of address region, recognition and warhead, upon which the inhibitors synthesised in this thesis are based, is also introduced. Chapter Two introduces reversible cysteine protease inhibitors found in the literature and that little is known about the effect of inhibitor warhead on selectivity within the papain superfamily. Oxidation of the dipeptidyl alcohols 2.6, 2.26, 2.29, 2.30, 2.35 and 2.36 utilising the sulfur trioxide-pyridine complex gave the aldehydes 2.3, 2.27, 2.19, 2.2, 2.21 and 2.22. Semicarbazones 2.37-2.40 were synthesised by a condensation reaction between the alcohol 2.3 and four available semicarbazides. The amidoximes 2.48 and 2.49 separately underwent thermal intramolecular cyclodehydration to give the 3-methyl-1,2,4- oxadiazoles 2.41 and 2.50. The aldehydes 2.3 and 2.27 were reacted with potassium cyanide to give the cyanohydrins 2.51 and 2.52. The cyanohydrins 2.51 and 2.52 were separately reacted to give 1) the α-ketotetrazoles 2.43 and 2.55; 2) the α-ketooxazolines 2.42 and 2.58; 3) the esterified cyanohydrins 2.60 and 2.61. A two step SN2 displacement reaction of the alcohol 2.6 to give the azide 2.62, an example of a non-covalent cysteine protease inhibitor. Chapter Three introduces inhibitors with irreversible warheads. The well-known examples of epoxysuccinic acids 3.1 and 3.5 are discussed in detail, highlighting the lack of irreversible cysteine protease specific inhibitors. The aldehydes 2.3 and 2.27 were reacted under Wittig conditions to give the α,β-unsaturated carbonyls 3.14-3.18. Horner- Emmons-Wadsworth methodology was utilised for the synthesis of the vinyl sulfones 3.20- 3.23. The dipeptidyl acids 2.24 and 2.28 were separately reacted with diazomethane to give the diazoketones 3.25 and 3.26. The diazoketones 3.25 and 3.26 were separately reacted with hydrogen bromide in acetic acid (33%) to give the α-bromomethyl ketones 3.27 and 3.28, which were subsequently reduced to give the α-bromomethyl alcohols 3.29-3.32. Under basic conditions the α-bromomethyl alcohols 3.29-3.32 ring-closed to form the peptidyl epoxides 3.33-3.36. Chapter Four introduces the disadvantages of peptide-based inhibitors. A discussion is given on the benefits of constraining inhibitors into the extended bioactive conformation known as a β-strand. Ring closing metathesis is utilised in the synthesis of the macrocyclic aldehyde 4.4, macrocyclic semicarbazone 4.15, the macrocyclic cyanohydrin 4.16, the macrocyclic α-ketotetrazole 4.18 and the macrocyclic azide 4.19. Chapter Five introduces enzyme inhibition studies. The BODIPY-casein fluorogenic assay used for establishing inhibitor potency against m-calpain and μ-calpain is validated. Assay protocols are also established and validated for cathepsin B, papain, pepsin and α- chymotrypsin. A discussion of the effect of solvent on enzyme activity is also included as part of this study. Chapter Six presents the assay results for all the inhibitors synthesised throughout this thesis and an extensive structure-activity relationship study between inhibitors is included. The alcohols 2.26 and 2.30 are unprecedented examples of non-covalent, potent, cathepsin B inhibitors (IC₅₀ = 0.075 μM selectivity 80-fold and 1.1 μM, selectivity 18-fold). The macrocyclic semicarbazone 4.15 is an unprecedented example of a potent macrocyclic cysteine protease inhibitor (m-calpain: IC₅₀ = 0.16 μM, selectivity 8-fold). The cyanohydrin 2.51 contains an unprecedented cysteine protease warhead and is a potent and selective inhibitor of papain (IC₅₀ = 0.030 μM, selectivity 3-fold). The O-protected cyanohydrin 2.61 is a potent and selective inhibitor of pepsin (IC₅₀ = 1.6 μM, selectivity 1.5-fold). The top ten warheads for potent, selective cathepsin B inhibition are: carboxylic acid, methyl ester, diazoketone, esterified cyanohydrin, α-bromomethyl ketone, α,β- unsaturated aldehyde, vinyl sulfones, α-bromomethyl-C₃-S,R-alcohol, alcohol and α,β- unsaturated ethyl ester. The selectivity of these warheads was between 5- and 130-fold for cathepsin B. The best inhibitors for cathepsin B were the α-bromomethyl ketone 3.26 (IC₅₀ = 0.075 μM, selectivity 16-fold), the α,β-unsaturated aldehyde 3.18 (IC₅₀ = 0.13 μM, selectivity 13-fold) and the esterified cyanohydrin 3.59 (IC₅₀ = 0.35 μM, selectivity 22- fold). Chapter Seven outlines the experimental details and synthesis of the compounds prepared in this thesis.

cysteine proteases

cysteine protease inhibitors

cathepsin B

papain

calpains

IC50. reversible inhibitors

irreversible inhibitors

non-covalent inhibitors

macrocycles

assays

The Design, Synthesis and Biological Assay of Cysteine Protease Specific Inhibitors

Mehrtens (nee Nikkel), Janna Marie

January 2007

This thesis investigates the design, synthesis and biological assay of cysteine protease inhibitors within the papain superfamily of cysteine proteases. This is achieved by examining the effect of inhibitor design, especially warheads, on IC₅₀ values and structureactivity relationships between cysteine protease inhibitors of the papain superfamily. The representative proteases used are m-calpain, μ-calpain, cathepsin B and papain. Chapter One is an introductory chapter; Chapters Two-Four describe the design and synthesis of cysteine protease inhibitors; Chapter Five discusses assay protocol; and Chapter Six contains the assay results and structure-activity relationships of the synthesised inhibitors. Chapter One introduces cysteine proteases of the papain family and examines the structure, physiology and role in disease of papain, cathepsin B, m-calpain and μ-calpain. The close structural homology that exists between these members of the papain superfamily is identified, as well characteristics unique to each protease. Covalent reversible, covalent irreversible and non-covalent warheads are defined. The generic inhibitor scaffold of address region, recognition and warhead, upon which the inhibitors synthesised in this thesis are based, is also introduced. Chapter Two introduces reversible cysteine protease inhibitors found in the literature and that little is known about the effect of inhibitor warhead on selectivity within the papain superfamily. Oxidation of the dipeptidyl alcohols 2.6, 2.26, 2.29, 2.30, 2.35 and 2.36 utilising the sulfur trioxide-pyridine complex gave the aldehydes 2.3, 2.27, 2.19, 2.2, 2.21 and 2.22. Semicarbazones 2.37-2.40 were synthesised by a condensation reaction between the alcohol 2.3 and four available semicarbazides. The amidoximes 2.48 and 2.49 separately underwent thermal intramolecular cyclodehydration to give the 3-methyl-1,2,4- oxadiazoles 2.41 and 2.50. The aldehydes 2.3 and 2.27 were reacted with potassium cyanide to give the cyanohydrins 2.51 and 2.52. The cyanohydrins 2.51 and 2.52 were separately reacted to give 1) the α-ketotetrazoles 2.43 and 2.55; 2) the α-ketooxazolines 2.42 and 2.58; 3) the esterified cyanohydrins 2.60 and 2.61. A two step SN2 displacement reaction of the alcohol 2.6 to give the azide 2.62, an example of a non-covalent cysteine protease inhibitor. Chapter Three introduces inhibitors with irreversible warheads. The well-known examples of epoxysuccinic acids 3.1 and 3.5 are discussed in detail, highlighting the lack of irreversible cysteine protease specific inhibitors. The aldehydes 2.3 and 2.27 were reacted under Wittig conditions to give the α,β-unsaturated carbonyls 3.14-3.18. Horner- Emmons-Wadsworth methodology was utilised for the synthesis of the vinyl sulfones 3.20- 3.23. The dipeptidyl acids 2.24 and 2.28 were separately reacted with diazomethane to give the diazoketones 3.25 and 3.26. The diazoketones 3.25 and 3.26 were separately reacted with hydrogen bromide in acetic acid (33%) to give the α-bromomethyl ketones 3.27 and 3.28, which were subsequently reduced to give the α-bromomethyl alcohols 3.29-3.32. Under basic conditions the α-bromomethyl alcohols 3.29-3.32 ring-closed to form the peptidyl epoxides 3.33-3.36. Chapter Four introduces the disadvantages of peptide-based inhibitors. A discussion is given on the benefits of constraining inhibitors into the extended bioactive conformation known as a β-strand. Ring closing metathesis is utilised in the synthesis of the macrocyclic aldehyde 4.4, macrocyclic semicarbazone 4.15, the macrocyclic cyanohydrin 4.16, the macrocyclic α-ketotetrazole 4.18 and the macrocyclic azide 4.19. Chapter Five introduces enzyme inhibition studies. The BODIPY-casein fluorogenic assay used for establishing inhibitor potency against m-calpain and μ-calpain is validated. Assay protocols are also established and validated for cathepsin B, papain, pepsin and α- chymotrypsin. A discussion of the effect of solvent on enzyme activity is also included as part of this study. Chapter Six presents the assay results for all the inhibitors synthesised throughout this thesis and an extensive structure-activity relationship study between inhibitors is included. The alcohols 2.26 and 2.30 are unprecedented examples of non-covalent, potent, cathepsin B inhibitors (IC₅₀ = 0.075 μM selectivity 80-fold and 1.1 μM, selectivity 18-fold). The macrocyclic semicarbazone 4.15 is an unprecedented example of a potent macrocyclic cysteine protease inhibitor (m-calpain: IC₅₀ = 0.16 μM, selectivity 8-fold). The cyanohydrin 2.51 contains an unprecedented cysteine protease warhead and is a potent and selective inhibitor of papain (IC₅₀ = 0.030 μM, selectivity 3-fold). The O-protected cyanohydrin 2.61 is a potent and selective inhibitor of pepsin (IC₅₀ = 1.6 μM, selectivity 1.5-fold). The top ten warheads for potent, selective cathepsin B inhibition are: carboxylic acid, methyl ester, diazoketone, esterified cyanohydrin, α-bromomethyl ketone, α,β- unsaturated aldehyde, vinyl sulfones, α-bromomethyl-C₃-S,R-alcohol, alcohol and α,β- unsaturated ethyl ester. The selectivity of these warheads was between 5- and 130-fold for cathepsin B. The best inhibitors for cathepsin B were the α-bromomethyl ketone 3.26 (IC₅₀ = 0.075 μM, selectivity 16-fold), the α,β-unsaturated aldehyde 3.18 (IC₅₀ = 0.13 μM, selectivity 13-fold) and the esterified cyanohydrin 3.59 (IC₅₀ = 0.35 μM, selectivity 22- fold). Chapter Seven outlines the experimental details and synthesis of the compounds prepared in this thesis.

cysteine proteases

cysteine protease inhibitors

cathepsin B

papain

calpains

IC50. reversible inhibitors

irreversible inhibitors

non-covalent inhibitors

macrocycles

assays

Dynamika paramagnetických komplexů a její studium pomocí jaderné magnetické rezonance / Dynamics of paramagnetic complexes observed by Nuclear Magnetic Resonance

Blahut, Jan

January 2018

In this Thesis, structure and dynamics of paramagnetic complexes for medical application are studied by Nuclear Magnetic Resonance (NMR). It focuses mainly on development of contrast agents (CA) for Magnetic Resonance Imaging (MRI) which is one of the most effective radiodiagnostic method nowadays. Most of the MRI CAs contains paramagnetic complexes of d- and f-metal ions. The presence of unpaired electron in proximity of NMR active nuclei has two main effects: paramagnetically induced shift and paramagnetically induced relaxa- tion. Both processes can dramatically change the NMR spectrum and often make it unobservable at all. Nevertheless, in many cases, acquisition of such spectra is possible and sometimes even less time-consuming than observation of diamag- netic molecules. Enhanced T1 relaxation allows faster pulse sequence repetition and increased chemical shift dispersion may lead to resolution of originally over- lapped signals. Moreover, the analysis of paramagnetic effects can provide useful information about the structure and dynamics of the studied system. Theoretical background of these effects is described in the Introduction of the Thesis. In the first part of Discussion in the Thesis, a new class of contrast agents for 19F-MRI based on nickel(II) and cobalt(II/III) ions is introduced...

Synthese und Charakterisierung beta-substituierter Thiaporphyrine und ihrer Übergangsmetallkomplexe

Götzke, Linda

13 May 2013

In den letzten Jahren haben sich die Anwendungsoptionen natürlicher und synthetischer Porphyrinsysteme stark erweitert, was sich auch in der permanent steigenden Anzahl von Publikationen in der Fachliteratur widerspiegelt. Die Inhalte der Veröffentlichungen reichen dabei von grundlegenden Fragestellungen zur Synthese und Charakterisierung über die Untersuchung typischer Eigenschaften bis hin zur Testung der Systeme in der Photovoltaik, als optische Speicher-medien, molekulare Schalter und Drähte oder in der Medizin. Eine interessante Eigenschaft von Porphyrinen besteht darin, nach Lichtanregung Energie an die Umgebung zu übertragen. Diese Beobachtung ist bereits seit etwa 100 Jahren bekannt und hat zur Entwicklung der photodynamischen Therapie (PDT) und Diagnostik (PDD) geführt, die vorteilhaft zur Erkennung und Bekämpfung von Krebs eingesetzt werden kann. Um die Beziehungen zwischen Struktur und Wirkung aufzuklären, ist es notwendig, Porphyrine innerhalb des Grundgerüsts zu modifizieren sowie das Substitutionsmuster gezielt zu variieren. Die logischen Schlüsse, die aus den Untersuchungen der synthetisierten Substanzreihen gezogen werden, können beim Aufbau einer idealen Wirkstruktur helfen, wodurch dessen Wirksamkeit optimiert und die auftretenden Nebenwirkungen minimiert werden können. Im Rahmen dieser Arbeit sollen als potentielle PDT-Agenzien neue meso- und beta-substituierte Thiaporphyrine synthetisiert und charakterisiert werden. Neben dem Einsatz spektroskopischer Methoden in Lösung, wie UV/Vis-, NMR- und Fluoreszenzspektroskopie, sollen vor allem Kristalle für die Röntgeneinkristallstrukturanalyse gezüchtet werden, um charakteristische Bindungsmotive und strukturelle Besonderheiten zu identifizieren. Desweiteren soll durch die Einführung kationischer, funktioneller Gruppen die Löslichkeit der Thiaporphyrine in polaren Lösungsmitteln erhöht werden.

info:eu-repo/classification/ddc/540

ddc:540

Neuartige photoschaltbare Makrocyclen und Pseudorotaxane auf Acridanbasis

Orda-Zgadzaj, Marzena Maria

03 November 2005

In der vorliegender Arbeit wurde die photochemische Bildung der Acridiniumionen in einem Pseudorotaxan und die daraus resultierende Transformation der Lichtenergie in die Translationsenergie, was als erster Schritt in Richtung der molekularen Maschinen angesehen wird, untersucht. 9-Phenyl-9-hydroxyacridan unterscheidet sich in ihrer Lichtabsorption, Molekülgeometrie und Elektronen- Donatorstärke gravierend von den korrespondierenden Acridiniumionen. Die Änderung der elektronischen Eigenschaften bei der Umwandlung der Acridane- in die Acridinium ist daher potentiell nutzbar, um nichtkovalente Bindungskräfte in supramolekularen Einheiten zu beeinflussen. Ziel der vorliegenden Arbeit war die Erschließung eines neuen Zugangs zu linearen und makrocyclischen Systemen, die als Strukturelement eine Acridaneinheit besitzen. Die Makrocyclen mit elektronenreichen 9-Phenylacridanbausteinen wurden unter high-dilution-Bedingungen erhalten. Bei der Photoanregung wurden unter Abspaltung von Methoxidionen die elektronenarmen korrespondierenden Acridiniummakrocyclen gebildet. Die Photoheterolyse findet in alkoholischen Lösungsmitteln, Acetonitril und in Toluol statt. Die Lebensdauer des Acridiniummethoxids kann durch Mischen des Alkohols mit dem Acetonitril gesteuert werden. Auch nach zehn Schaltcyclen ist keine Ermüdung des Systems festzustellen. Als molekulare Fäden kommen für die neuen Makrocyclen entweder Moleküle mit elektronenarmen Erkennungstationen für die Acridanverbindungen oder elektronenreiche Erkennungsstationen für die Acridiniumringe in Frage. Es wurden zahlreiche Untersuchungen zur Komplexierung der neuen Makrocyclen mit Hilfe der spektroskopischen Titrationen durchgeführt. Dabei wurde das photoschaltbare Pseudorotaxan gefunden. Im Rahmen dieser Arbeit wurde ein neuer langlebiger Photoschalter optimiert und mit Hilfe der 1H-NMR-Spektroskopie wurde die durch Licht injizierte molekulare Bewegung beobachtet. / For this work we have examined the photolytic formation of acridinium ion within pseudorotaxanes and the resulting transformation of light energy into translational movement. This can be regarded as the first step towards (creating a) molecular machine. 9-phenyl-9-methoxyacridane distinguishes itself from its corresponding acridinium ions in terms of light absorption, shape, and electronic donor strength. The acridane can be regarded as candidates for photoswitching supramolecular units, because they can be transformed into positively charged acridinium ions. These ions generate an electron acceptor from an electron donor. The object of the following thesis is the development of a new synthetic approach to linear or makrocyclic systems, which contain acridane as a structural element. Macrocycles with electron-rich 9-phenyl-9-methoxyacridan units were prepared under high dilution conditions. The acridinium macrocycles are generated by photoheterolysis of this methoxy derivative, which has a thermal response to acridane macro cycles, thus closing the switching cycle. Heterolytic photodissociation occurs in alcohols, acetonitrile and toluene. Mixing alcohol with acentonitril can control the lifespan of the acridinium methoxide. Even after 10 switching cycles the system seemed unaffected. The molecular thread and macrocycles must be complementary in that they can interact by attracting forces, through generating an electron acceptor from an electron donor. The complex formation of acridan macrocycles with electron acceptor molecular thread was studied using spectrophotometric titration. As a result, photoswitchable pseudorotaxane was formed between acridan crown ethers and (2,2-bipyridine) molecular thread. In the context of this research, we have found that such a transformation is possible. A new, durable photoswitch has been developed, and using the 1H-NMR-spectroscope, we observed the molecular movement, which was made visible through the application of light.

Acridane

Acridiniumionen

Makrocyclen

Pseudorotaxane

molekulare Photoschalter

supramolekulare Chemie

acridane

acridinium ions

macrocycles

pseudorotaxane

540 Chemie

30 Chemie

ddc:540

Synthèse et étude de nouveaux agents chélatants optimisés ciblant le récepteur de chimiokine CXCR4

Désogère, Pauline

22 November 2012

L'objectif de ce travail de thèse était de développer des outils pour détecter et traiter le cancer àun stade précoce. Nous avons donc entrepris la synthèse de nouveaux radiopharmaceutiques ciblantspécifiquement le récepteur CXCR4, en utilisant le savoir-faire et l'expertise de notre groupe dans lasynthèse et la fonctionnalisation des polyazacycloalcanes. Nous avons travaillé simultanément surdeux aspects : l'agent chélatant et la molécule vectrice.Dans un premier temps, les travaux ont concerné la conception, la synthèse et la caractérisationde nouveaux macrocycles à fort potentiel pour la chélation du cuivre et du gallium. Nous avons toutd'abord développé une nouvelle voie de synthèse permettant d'accéder à des dérivés homocyclènesC-functionnalisés. Nous nous sommes ensuite intéressés aux dérivés du 1,4,7-triazacyclononane(TACN). En optimisant une voie de synthèse déjà développée au laboratoire, nous avons facilitél'accès à des dérivés TACN N- et C-fonctionnalisés. Nous avons ainsi préparé une série denouveaux agents chélatants bifonctionnels adaptés pour la complexation du cuivre ou du gallium, envariant la nature de la fonction de greffage et des bras coordinants. Nous avons également réalisé lasynthèse de nouveaux cryptands en série cyclène et nous avons étudié leur propriété decomplexation vis à vis du cuivre.Dans un second temps, nous avons développé une nouvelle famille d'agents imageants duCXCR4 en modifiant la structure des AMD3100 et AMD3465. Ce travail a tout d'abord nécessité lamise au point de nouvelles méthodes de fonctionnalisation de ces structures. Nous avons ainsi pupréparer de nouveaux synthons porteur d'une fonction de greffage dans les deux séries. Nous avonsensuite introduit différentes sondes imageantes, telles que des chélates adaptés pour la complexationdu cuivre, gallium et indium ainsi que des sondes fluorescentes de type bodipy.

[CHIM:OTHE] Chemical Sciences/Other

CXCR4

AMD3100/AMD3465

Complexation Cuivre/Gallium

Macrocycles

Cryptand

Homocyclène

1

4

7-triazacyclononane

C-functionalisation

Agents bifonctionnels chélatants

Développement de nouveaux outils de contrôle conformationnel utilisant des interactions non-covalentes pour effectuer des macrocyclisations

Bolduc, Philippe

11 1900

Les macrocycles ont longtemps attiré l'attention des chimistes. Malgré cet intérêt, peu de méthodes générales et efficaces pour la construction de macrocycles ont été développés. Récemment, notre groupe a développé un programme de recherche visant à développer de nouvelles voies vers la synthèse de paracyclophanes et ce mémoire présente l pluspart des efforts les plus récents dans ce domaine. Traditionnellement, la synthèse de paracyclophanes rigides est facilitée par l'installation d'un groupe fonctionnel capable de contrôler la structure de la molécule en solution (ex un élément de contrôle de conformation (ECC)). Cependant, cette approche utilisant des auxiliaires exige que le ECC soit facilement installé avant macrocyclisation et facilement enlevé après la cyclisation. Le présent mémoire décrit une méthode alternative pour guider la macrocyclisations difficile à travers l'utilisation d'additifs comme ECC. Les additifs sont des hétérocycles aromatiques N-alkylé qui sont bon marché, faciles à préparer et peuvent être facilement ajoutés à un mélange de réaction et enlevés suite à la macrocyclisation par simple précipitation et de filtration. En outre, les ECCs sont recyclables. L'utilisation du nouveau ECC est démontré dans la synthèse des para-et métacyclophanes en utilisant soit la métathèse de fermeture de cycle (RCM) ou couplage de Glaser-Hay. / Macrocycles have long attracted the attention of chemists. Despite that interest, few general and efficient methods for the construction of macrocycles have been developed. Recently our group has developed a research program aimed at developing novel routes towards the synthesis of paracyclophanes and the present thesis details the most recent efforts in this area. Traditionally, the synthesis of rigid paracyclophanes is aided by the installation of functional groups capable of controlling the solution state structure of the molecules (ie. a conformational control element (CCE)). However, this auxiliary-like approach requires that the CCE be readily installed prior to macrocyclization and easily removed following the cyclization. In the present thesis describes an alternative method to guiding difficult macrocyclizations through the use of additives as CCEs is described. The additives are N-alkylated aromatic heterocycles that are cheap, easily prepared and can be easily added to a reaction mixture and removed following the macrocyclization through simple precipitation and filtration. In addition, the CCEs are recyclable. The use of the new CCEs is demonstrated in the synthesis of para- and metacyclophanes using either ring closing metathesis (RCM) or Glaser-Hay couplings.

Paracyclophanes

Metacyclophane

Glaser-Hay

Éléments directeurs chiraux

ring closing olefin metathesis

conformational control element

macrocycles