Synthesis of new heterocycles by SNAr reactions of perfluoroarenes

Riaz, Shahzad

January 2016

The reactivity of perfluoroarenes and hetarenes towards SNAr reactions was studied as part of a synthetic programme to form an assembly of novel heterocyclic aromatic compounds for material and pharmaceutical applications. In chapter 1 the chemistry of perfluoroarenes is reviewed together with the use of conjugated compounds in organo-electronic applications. In chapter 2 the successful replacement of the remaining fluorine atoms in 6,12-difluorobenzo[1,2-b:4,5-b']bis[b]benzothiophene through SNAr reaction with long chain alkoxy and alkylthio nucleophiles is reported. An X-ray crystallographic investigation into their solid state packing was undertaken which would provide useful information for organoelectronic applications. Reactions with nitrogen and carbon based nucleophiles were also studied but met with little success. In chapter 3, alternative methods for the reductive cyclization of aryl and 2-bromoaryl perfluoroethers and sulfides to replace the currently used lithium-bromine exchange were explored, namely the use of radical cyclizations, palladium, magnesium, copper and Rieke metals. Some success was found using magnesium as a reagent although yields were low. Attempts to effect cyclisation reactions by ortho-lithiation and Ullmann coupling reaction with fluoroarenes is also reported. In chapter 4 attempts to generate alternative ring fusion in annulation reactions to form fused benzothiophenes by a dianion strategy are described. Development of methods to synthesise helicene or curved polycyclic structures from dibenzothiophene precursors is reported. In chapter 5 the synthesis of nitrogen containing fluorinated compounds with potential bioactivity is described. A series of novel amino substituted fluoroaromatics were successfully synthesised by adding different nitrogen based nucleophiles to pentafluoropyridine. Smiles rearrangement of a tetrafluoropyridyl sulphonamide was found to occur. A number of fluoropyridyl aniline derivatives were successfully synthesised some of which were submitted for biological screening. Substitution reactions of bis-nucleophiles bearing two heteroatom groups to form fused six membered rings were also studied. A Smiles rearrangement was identified in the reaction with an aminobenzenethiolate and confirmed by X-ray crystallography. Experimental procedures are given in chapter 6 as well as characterisation and crystallographic data of molecules synthesised during the research.

546

Regioselective, Nucleophilic Activation of C-F Bonds in o-Fluoroanilines

Hough, Sarita Elizabeth

25 June 2019

Reactions of fluorinated anilines with stoichiometric Ti(NMe2)4 in mesitylene (typically for 23 h at 120 °C) afforded moderate to high yields of the corresponding N,N-dimethyl-o-phenylenediamine derivatives resulting from defluoroamination of a fluorine atom ortho to the NH2 of the starting aniline. Reactivity increased with additional ring fluorination in general accordance with established regiochemical (activating and deactivating) trends. Based on results, we propose a metal-mediated, SNAr-based mechanism. We report the scope and limitations of this reaction and discuss trends in reactivity according to a putative mechanistic scheme. / Master of Science / This thesis describes reactions of fluorinated anilines with titanium amides to make fluorinated 1,2-phenylenediamines. The reaction gives high to moderate yields, and is highly selective for ortho substitution. The scope of the reaction, trends in reactivity among substrates, product characterization, and reaction mechanism are discussed. This reaction is of interest because fluorinated aniline derivatives are a privileged structural motif in pharmaceuticals and agricultural chemicals. The first chapter presents an overview of C-F bond activation and key background information. Chapter 2 is a description of the experiments and an in-depth analysis of their results. Chapter 3 presents detailed characterization data for substances generated in this research. Chapter 4 comprises some concluding remarks and plans for possible future extensions of the research.

titanium amide

SNAr

defluorination

anilines

organometallic

nucleophiles

Approche théorique de la réactivité des isonitriles en chimie organique

Chéron, Nicolas

18 November 2011

Les isonitriles sont des espèces connues depuis longtemps, mais étudiées depuis peu. Une approche théorique a permis de s'intéresser en détails aux réactions de Nef et de Ugi. Nous nous sommes tout d'abord focalisés sur la première. Après en avoir élucidé le mécanisme, nous avons étudié l'effet du solvant et nous avons proposé de nouvelles conditions expérimentales. Nous avons ensuite étudié l'influence des groupements de l'acyl, de l'isonitrile et du groupe partant. L'ensemble des variations considérées a pu être rationalisé en reliant l'énergie d'activation au pKa du groupe partant. En parallèle, nous avons étudié la réaction de Ugi. Le mécanisme proposé par Ugi pour cette réaction complexe n'avait toujours pas été vérifié 50 ans après sa découverte. Une étude quasi-exhaustive des différents mécanismes possibles a été menée, en utilisant une approche originale mêlant théorie et expériences. Le mécanisme de cette réaction a ainsi été démontré, tant dans le méthanol que dans le toluène. Les étapes cinétiquement déterminantes et les forces motrices ont été mises en lumière et diffèrent de celles proposées par Ugi. Une variation de la réaction de Ugi est le couplage Ugi-Smiles pour lequel de nombreux résultats expérimentaux n'ont toujours pas trouvé d'explications. Nous nous sommes donc intéressés au réarrangement de Smiles. Nous avons montré l'importance d'une liaison hydrogène intramoléculaire sur la faisabilité de la réaction, et nous avons étendu cette observation aux réactions intermoléculaires. Nous avons également étudié l'influence des substituants des quatre réactifs sur les barrières afin de construire un modèle prédictif.

[CHIM:OTHE] Chemical Sciences/Other

Réaction de Nef

Etats de transition

SnAr

DFT

Synthesis of fluorinated heterocyclic compounds and study of their interaction with DNA

Zeinali, Fatemeh

January 2017

Over fifty structurally diverse, novel fluorinated heteroarenes, have been successfully synthesised by SNAr reaction of a range of fluorinated arenes including pentafluoropyridine, hexafluorobenzene, and methyl pentafluorobenzoate by introduction of a range of groups such as imidazole, triazole, benzimidazole, benzotriazole, and carbazole. Different water solubilising side chains were introduced to some of the successfully synthesised fluorinated heteroarenes to improve water solubility and potential biological activity. X-ray crystal structures of over 10 compounds were obtained including those of two macrocyclic compounds containing 21- and 24-membered rings. The synthesised compounds have been characterized by elemental analysis, IR, 1H and 19F spectroscopy and high resolution mass spectrometry. These compounds have been screened for their biological activities and possible interaction with DNA by methods including UV-visible spectroscopy, fluorescence spectroscopy, co-crystallization for X-ray diffraction analysis, and antimicrobial activity. A number of the fluoroaryl benzimidazole derivatives have been tested against K-562 and MCF-7 cell lines and G361 and HOS cell lines. From the all tested compounds three tethered fluoroaryl benzimidazole derivatives demonstrated micromolar inhibition against K-562 and MCF-7 cell lines. These compounds, in addition to 1-tetrafluoropyrid-4-yl-2-tetrafluoropyrid-4-ylsulfanyl-1H-benzimidazole, also demonstrated micromolar inhibition against G361 and HOS cell lines. Two of the compounds were found to activate caspases leading to apoptosis.

547

Zwitterionic Poly(arylene ether sulfone) Copolymers: Membrane Applications and Fundamentals

January 2019

abstract: Zwitterionic polymers, due to their supurior capability of electrostatically induced hydration, have been considered as effective functionalities to alleviate bio-fouling of reverse osmosis (RO) membranes. Bulk modification of polysulfone-based matrices to improve hydrophilicity, on the other hand, is favored due to the high membrane performance, processibility, and intrinsic chlorine resistance. Here a novel synthetic method was demonstrated to prepare zwitterionic poly(arylene ether sulfone) (PAES) copolymers, which was blended with native polysulfone (PSf) to fabricate free-standing asymmetric membranes via non-solvent induced phase separation process. Both the porosity of the support layer and surface hydrophilicity increased drastically due to the incorporation of zwitterion functionalities in the rigid polysulfone matrix. The water permeance and antifouling ability of the blend membranes were both remarkably improved to 2.5 Lm−2 h−1 bar−1 and 94% of flux recovery ratio, respectively, while salt rejection remained at a high level (98%) even under the high exposure to chlorine (8,000 ppm•h). Besides the preliminary blended membrane design, for the future membrane property enhancement, this dissertation also focused on polymer structure optimizations via elucidating the fundamentals from two perspectives: 1). Synthetic reaction kinetics and mechanisms on polycondensation of PAES. Interestingly, in combination of experiments and the computational calculations by density functional theory (DFT) methods in this work, only the aryl chlorides (ArCl) monomer follows the classical second-order reaction kinetics of aromatic nucleophilic substitution (SNAr) mechanism, while the kinetics of the aryl fluorides (ArF) reaction fit a third-order rate law. The third order reaction behavior of the ArF monomer is attributed to the activation of the carbon-fluorine bond by two potassium cations (at least one bounded to phenolate), which associate as a strong three-body complex. This complex acts as the predominant reactant during the attack by the nucleophile. 2). Optimized copolymer structures were developed for controlled high molecular weight (Mw ~ 65 kDa) and zwitterionic charge content (0~100 mol%), via off-set stoichiometry during polycondensations, following with thiol-ene click reaction and ring-opening of sultone to introduce the sulfobetaine functional groups. The structure-property-morphology relationships were elucidated for better understanding atomic-level features in the charged polymers for future high-performance desalination applications. / Dissertation/Thesis / Doctoral Dissertation Chemical Engineering 2019

Chemical engineering

Desalination

Membranes

Polymer synthesis

SNAr mechanisms

STUDIES TOWARDS THE TOTAL SYNTHESIS OF VANCOMYCIN AGLYCON

Basu, Shubhamita

03 July 2007

No description available.

Chemistry, Organic

vancomycin

glycopeptide antibiotics

ruthenium-mediated SNAr

Approche théorique de la réactivité des isonitriles en chimie organique / Theoretical aspects of the reactivity of isocyanides in organic chemistry

Chéron, Nicolas

18 November 2011

Les isonitriles sont des espèces connues depuis longtemps, mais étudiées depuis peu. Une approche théorique a permis de s'intéresser en détails aux réactions de Nef et de Ugi. Nous nous sommes tout d'abord focalisés sur la première. Après en avoir élucidé le mécanisme, nous avons étudié l'effet du solvant et nous avons proposé de nouvelles conditions expérimentales. Nous avons ensuite étudié l'influence des groupements de l'acyl, de l'isonitrile et du groupe partant. L'ensemble des variations considérées a pu être rationalisé en reliant l'énergie d'activation au pKa du groupe partant. En parallèle, nous avons étudié la réaction de Ugi. Le mécanisme proposé par Ugi pour cette réaction complexe n'avait toujours pas été vérifié 50 ans après sa découverte. Une étude quasi-exhaustive des différents mécanismes possibles a été menée, en utilisant une approche originale mêlant théorie et expériences. Le mécanisme de cette réaction a ainsi été démontré, tant dans le méthanol que dans le toluène. Les étapes cinétiquement déterminantes et les forces motrices ont été mises en lumière et diffèrent de celles proposées par Ugi. Une variation de la réaction de Ugi est le couplage Ugi-Smiles pour lequel de nombreux résultats expérimentaux n'ont toujours pas trouvé d'explications. Nous nous sommes donc intéressés au réarrangement de Smiles. Nous avons montré l'importance d'une liaison hydrogène intramoléculaire sur la faisabilité de la réaction, et nous avons étendu cette observation aux réactions intermoléculaires. Nous avons également étudié l'influence des substituants des quatre réactifs sur les barrières afin de construire un modèle prédictif. / Isocyanides are known for a long time, but have been studied only recently. A theoretical approach allowed us to investigate in details the Nef and the Ugi reactions. We first focused on the former. After elucidating its mechanism, we studied solvent effects and proposed new experimental conditions. We then studied the acyl moiety and isocyanide influences, such as the leaving group one. All the variations were rationalized by linking the activation energy to the leaving group pKa. Simultaneously, we studied the Ugi reaction. The mechanism proposed by Ugi for this complex reaction was still unverified 50 years after its discovery. A thorough and quasi-complete study of all the possible mechanisms were lead, using a mixed theoretical and experimental approach. The mechanism of this reaction was demonstrated, in both methanol and toluene. Rate determining steps and driving forces were highlighted and differ from those proposed by Ugi. A variation of the Ugi reaction is the Ugi-Smiles coupling, for which numerous experimental results are still unexplained. We thus studied the Smiles rearrangement. We showed the key-role of an intramolecular hydrogen bond on the reaction feasibility, and extended this observation to intermolecular reactions. We also studied the four substituent influence on the barrier, aiming to build a predictive model.

Réaction de Nef

Etats de transition

SnAr

DFT

Nef reaction

Transition states

Hydrogen bond

Ugi reaction

Mechanisms

SnAr

DFT

Méthodologies de synthèses d'hétérocycles bicycliques (6-5) et (5-5). Application à la conception d'inhibiteurs de kinases impliquées en oncologie et dans les maladies du système nerveux central. / Synthetic methodologies of [6-5] and [5-5] fused ring bicycles; Application toward conception of kinases inhibitors involved in oncology and in nervous central system disorders

Place, Matthieu

21 December 2017

Depuis le début des années 2000, la connaissance précise du kinome a entraîné l’émergence de nouvelles stratégies thérapeutiques ciblant des protéines kinases impliquées dans de nombreuses pathologies en oncologie et dans les maladies du système nerveux central. Afin de cibler les kinases d’intérêts identifiées au sein de ces travaux, nous avons effectué, dans une démarche orientée vers la diversité moléculaire, la synthèse de nouveaux hétérocycliques a fort potentiel de valorisation. Nous nous sommes appuyé sur la création et la fonctionnalisation de bicycles à 5 ou 6chaînons de type [6-5] ou [5-5], ces espèces chimiques représentant la voie d’accès à des inhibiteurs compétitifs du substrat naturel des kinases, l’ATP. Nous avons dans un premier temps travaillé autour des imidazo[1,2-b]pyridazines puis des[1,2,4] triazolo[4,3-b]pyridazines, scaffold plus original, pour concevoir des inhibiteurs plus actifs et spécifiques de la kinase HASPIN, nouvelle cible prometteuse en oncologie.Nous avons ensuite poursuivi les études précédentes du laboratoire sur les imidazo[2,1-b][1,3,4]thiadiazoles. Nous basant sur une méthodologie de synthèse bien développée, nous avons créé une librairie de composés dirigés contre les kinases DYRK1A et CLK1 impliquées dans les processus de neuro dégénération, notamment dans la maladie d’Alzheimer. Ainsi, au travers d’analogues des imidazothiadiazoles originaux, nous avons proposé des méthodologies de synthèses de ces nouveaux hétérocycles permettant des pharmaco modulations aisées.Ces divers projets de chimie médicinale ont pu être entrepris de façon à améliorer les connaissances des relations structure-activité, et concevoir de nouveaux inhibiteurs puissants des kinases HASPIN, DYRK1A etCLK1. / Since the early 2000s, precise knowledge of kinome has induced the emergence of novel therapies targeting kinases involved in several kinds of pathologies in oncology and nervous central systems disorders.In order to target original kinases of interest identified in this work, we have developed diversity-oriented synthesis to create new high-valuable heterocycles. We have focused our efforts on the design and functionalization of [6-5] or [5-5] fused ring bicycles. Those chemical species representing a great pathway tocreate competitive inhibitors of ATP; the natural substrate of kinases.First-of-all, we have worked on imidazo[1,2-b]pyridazines and then on [1,2,4]triazolo[4,3-b]pyridazinesscaffolds, to create more active and selective HASPIN kinase inhibitors, a new hot-target in oncology.Then, we have pursued previous laboratory studies on imidazo[2,1-b][1,3,4]thiadiazoles. Based on a well-built methodology, we have synthesized severals DYRK1A and CLK1 kinases inhibitors involved in neurodegenerative disorders, as Alzheimer’s disease. Thus, through original imidazothiadiazoles analogues,we have proposed synthetic methodologies to design these novel heterocycles allowding esay pharmacomodulations.These medicinal chemistry projects have been undertaken to improved knowledge of structure-activityrelashionship, and providing novel strong inhibitors of HASPIN, DYRK1A or CLK1 kinases.

Kinase

HASPIN

DYRK1A

CLK1

Inhibiteur

Cancer

Maladies neurodégénératives

Imidazopyridazine

Imidazothiadiazole

Réactions pallado-catalysées

SNAr

Kinase

HASPIN

DYRK1A

CLK1

Inhibitor

Cancer

Neurodegenerative diseases

Imidazopyridazine

Imidazothiadiazole

Pallado-catalyzed reactions

SNAr

Conception et caractérisation de nouveaux fluorophores organiques de la famille des triazapentalènes : outils pour l'imagerie cellulaire / Design and characterization of new organic fluorophores analogs of triazapentalenes as tools for cellular imaging

Sirbu, Doina

20 December 2016

Au cours du 21ème siècle, les techniques de fluorescence ont montré une expansion considérable dans l’étude du mécanisme du vivant. Un progrès majeur dans le développement, la conception et les applications de divers types de chromophores organiques ont été achevés. Bien que largement utilisés, les sondes fluorescentes les plus utilisées souffrent encore de quelques limitations qui diminuent leur étendue d'action. Les plus problématiques sont : un nombre restreint de familles de chromophores, une faible résistance au photoblanchiment, une faible solubilité aqueuse, une durée de vie de fluorescence relativement courte, etc…. A ce titre, le développement de nouveaux motifs organiques inédits, compacts et possédants des propriétés de fluorescence alternatives et/ou complémentaires aux fluorophores usuels organiques reste plus que jamais d’actualité. Dans ce contexte, les noyaux 1,3a, 6a-triazapentalènes nous sont apparus particulièrement prometteuses et encore très peu exploitées. Dans ce manuscrit, il est décrit la synthèse de noyaux tricycliques et tétracycliques comportant ce motif, obtenus par substitution nucléophiles aromatiques, suivi d’une thermolyse. La modulation de ces noyaux a ensuite été effectuée par couplage métallo-catalysé. L’évaluation photophysique de ces composés révèle des propriétés spectroscopiques remarquables comme des rendements quantiques supérieurs à 50%, des déplacements de Stokes d’environ 100 nm et des longueurs d’ondes d’émission allant de 450 à 650 nm. Le dernier volet de cette thèse a porté sur l’imagerie cellulaire, qui nous a permis d’évaluer les meilleurs fluorophores sur cellules vivantes. / Over the last two decades, fluorescence technologies have shown a spectacular spreading in biological research. Major progress in the development, design, and purposeful application of various types of organic chromophores was achieved. Although widely used, the most commonly fluorescent probes still suffer from some limitations which decrease their use in the field of life sciences. The most problematic ones are: low scaffold diversity, high sensitivity to photobleaching, low water solubility and modest Stokes Shift… In this context, the main idea of our work focuses on the development of novel organic motifs responding to the conventional fluorophores issues. The 1,3a, 6a-triazapentalene moiety represents a real interest in this field with its promising optical properties. In this manuscript, the syntheses of tricyclic and tetracyclic derivatives containing this scaffold were obtained by aromatic nucleophilic substitution followed by the thermolysis cyclization. The modulation of these cores was then allowed by various organometallic cross of these compounds provides remarkable spectroscopic properties, as quantum yields above 50%, Stokes shift around 100 nm, and emission wavelengths between 450 and 650 nm. The last part of this thesis was focused on cellular imaging, that allowed us to evaluate the best fluorophores in living cells.

Fluorescence

Triazapentalène

Photoblanchiment

Amphiphile

Propriétés photophysiques

Imagerie cellulaire

Couplages organo-métalliques

Thermolyse

SNAr

Fluorescence

Triazapentalène

Photobleaching

Amphiphile

Photophysics properties

Organometallic coupling

Thermolysis

SNAr

547

Síntese e caracterização de amino ácidos e ésteres n-(aminoalquil)-lactâmicos derivados do paba com potencial atividade biológica

Gonçalves, Renato Sonchini [UNESP]

27 July 2010

Made available in DSpace on 2014-06-11T19:30:18Z (GMT). No. of bitstreams: 0 Previous issue date: 2010-07-27Bitstream added on 2014-06-13T18:06:41Z : No. of bitstreams: 1 goncalves_rs_me_bauru.pdf: 4669388 bytes, checksum: b30004cd2539c06798b6a06a2acbec15 (MD5) / Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq) / Amino ésteres lactâmicos derivados do PABA e que podem ser potencialmente bioativos, por exemplo, como anestésicos locais, foram sintetizados com bons rendimentos por uma reação seletiva de SnAr de ácidos benzóicos com n-(3-aminopropil)-lactamas seguida por esterificação com aminoálcoois terciários. Produtos da N-arilação do N, N-dimetilformamida foram também obtidos através da esterificação direta do ácido 4-cloro-3-nitrobenzóico / Lactamic amino esters PABA-related, and can potentially bioactive, for exemple, as local anesthetics were synthesized in good yields by a selective 'S IND. n'Ar reactions of benzoic acids with N-(3-aminopropyl)lactams followed by esteterification with tertiary aminoalcohols. Products of the N-arylation with N,N-dimethylformamide are also obtained through of direct esterification of 4-chloro3-nitrobenzoic acid

Esterificação (Quimica)

Arilação

Compostos bioativos

Reação química

SnAr reaction

Esterification reaction

N-arylation

Potentially bioactive