Réactions de transfert de nitrènes catalysées par des complexes de fer : de la compréhension des mécanismes au développement de réactions multi-séquentielles / Iron-catalyzed nitrene transfer reactions : from mechanistic understanding to multi-sequential reactions

Coin, Guillaume

29 October 2018

Les amines sont des composés essentiels en biologie, pharmacie et agriculture. La synthèse directe de tels composés constitue un enjeu majeur dans le domaine de la chimie. Le travail présenté dans ce manuscrit porte sur l’étude et le développement de synthèses intégrant le transfert de nitrène par des catalyseurs de fer pour l’obtention de composés aminés. Dans une première partie, nous avons étudié la réaction d’aziridination par plusieurs catalyseurs à base de fer sur différentes oléfines. Nous rapportons ici, comment des études mécanistiques couplées à des investigations des structures électroniques et des profils réactionnels, par des méthodes quantiques de type DFT, peuvent conduire à une complète compréhension du mécanisme, ainsi qu’au développement rationnel de nouveaux catalyseurs de fer pour la réaction d’aziridination. Nous avons pu établir que l’affinité électronique joue un rôle majeur dans ce type de transformation. Dans une seconde partie, nous avons étudié la possibilité d’intégrer la catalyse de transfert de nitrène de fer dans des processus multi-séquentiels. Nous avons pu obtenir des amidines et imidazolidines dans des réactions multicomposants via la réaction entre un substrat, un donneur de nitrène et un nitrile, le tout catalysé par le fer. Les calculs DFT ont pu confirmer le mécanisme proposer expérimentalement. Une seconde étude a pu mettre en lumière les réactions monotopes à travers la synthèse de 2-iminothiazolidines via l’ouverture de cycle d’une aziridine suivie de l’insertion d’un isothiocyanate avec de bons rendements. Ces deux types de réactions ont démontré le fort potentiel du transfert de nitrène dans des réactions multi-séquentielles et ouvrent la porte au développement de nouvelles voies de synthèses efficaces dans une chimie durable. / Amines are essential compounds in biology, pharmacy and agriculture. Therefore, their direct synthesis is a major issue in chemistry. The work presented in this manuscript focuses on the study and development of syntheses integrating nitrene transfer by iron catalysts in order to obtain amines. In a first part, we studied the aziridination reaction with several iron catalysts on different olefins. We report here, how mechanistic studies coupled with investigations of electronic structures and reactivity profiles, by quantum methods of DFT type, can lead to a complete understanding of the mechanism, as well as to the rational development of new iron catalysts for the aziridination reaction. We have been able to establish that electron affinity plays a major role in this type of transformation. In a second part, we studied the possibility to integrate iron-catalyzed nitrene transfer in multi-sequential processes. We have been able to obtain amidines and imidazolidines in multicomponent reactions via the reaction between a substrate, a nitrene donor, a nitrile and an iron catalyst. The DFT calculations were able to confirm the mechanism proposed experimentally. A second study was to highlight telescoping reactions through the synthesis of 2-iminothiazolidines via the ring opening of an aziridine followed by the insertion of an isothiocyanate with good yields. These two types of reactions have shown the strong potential of nitrene transfer in multi-sequential reactions and open the way to the development of new efficient synthesis routes in the context of green chemistry.

Catalyse

Complexes de fer

Transfert de nitrène

Etudes mécanistiques

Réactions multi-Séquentielles

Synthèses d'amines

Catalysis

Iron complexes

Nitrene transfer

Mechanistic studies

Multi-Sequential reactions

Amines synthesis

540

Design, Synthesis and Applications of Novel Thiosugars & Amino Acid Derivatives

Gunasundari, T

January 2012

Glycosidases are carbohydrate processing essential enzymes necessary for the growth and development of all organisms such as intestinal digestion, post-translational processing of glycoproteins and the lysosomal catabolism of glycoconjugates. The function of these glycosidases is limited and studies are still in progress to understand their function at cellular level. In recent years, biological role of carbohydrates has resulted in various carbohydrate-based therapeutics2. These carbohydrates serve as a tool to study the function of glycosidases by inhibiting their active site. The concept of inhibition is yet another approach for the discovery of drugs. Glycosidase inhibitors studied are often sugar analogs and a wide range of such inhibitors are reported in the literature.3, 4 Thiosugars, in particular, have gained new perspectives owing to their electronic, geometric, conformational and flexibility differences, as sulfide moiety being less electronegative and more polarizable than the oxygen counter-part.5 These differences make the thiosugars distinct from their oxygen analogs and hence can mimic the active site of the enzyme. Many molecules are reported to be promising glycosidase inhibitors but are not easily accessible due to difficulties in their synthesis. Hence, the chemical synthesis of thio-analogs of carbohydrates, by synthetic routes, remains a major challenge. To address the complexity of synthesis and to make available new strategies, we envisioned the use of benzyltriethylammonium tetrathiomolybdate [BnEt3N]2MoS4, a versatile and efficient sulfur transfer reagent. Objectives of the study: a. Design novel thiosugars as glycosidase inhibitors. b. Devise strategy for the synthesis of novel thiosugars through a simple, practical approach. c. Evaluate the synthesized molecules as glycosidase and HIV-1 protease inhibitors, in silico. d. Study miscellaneous applications of the novel thiosugar-derived thialactones. The thesis is divided into five sections: Section A entitled “Synthesis of deoxythiosugars and thiosugar-based lactones” is divided into two parts, Part A and Part B. Part A – “An introduction and background on thiosugars and sulfur transfer reagents” has been provided. A brief discussion of sulfur transfer reagents in carbohydrate synthesis and earlier work related to the use of benzyltriethylammonium tetrathiomolybdate, [BnEt3N]2MoS4, as an efficient sulfur transfer reagent have been provided. Part B –“Design of inhibitors of glycosidases and HIV-1 protease” deals with the design of inhibitors of glycosidase and HIV-1 protease. The designed thiosugar molecules exhibit the characteristics of sugars and will act as planar molecules to mimic the active site conformation of a good inhibitor. Synthetic methodologies devised and adopted for the synthesis of constrained sugar-derived thialactones include: (a) Double displacement, (b) Displacement-cum-intramolecular thia-Michael addition, (c) Epoxide ring-opening-cum-intramolecular thia-Michael addition, and (d) Displacement-cum-epoxide ring opening in an intramolecular fashion. In all the above mentioned strategies, sulfur transfer step is the crucial step which was achieved by the use of benzyltriethylammonium tetrathiomolybdate [BnEt3N]2MoS46 as the key reagent. (a) Various constrained thialactones synthesized by double displacement strategy using tetrathiomolybdate as the sulfur transfer reagent are shown in Scheme – 1. (b) A number of constrained thialactones were synthesized following nucleophilic displacement-cum-intramolecular thia-Michael addition strategy as shown in Scheme – 2. (c) Synthesis of bicyclic thiolactones was achieved using the strategy of epoxide ring-opening-cum-intramolecular thia-Michael addition. (Scheme – 3) (d) A few bicyclic thialactones were synthesized through displacement-epoxide ring opening-cyclization as shown in Scheme – 4. The methodology was also utilized for the synthesis of thiosugar derivatives and azido-thialactones. (Fig. 1) Figure 1 Synthesis of deoxythiosugars: The bicyclic thialactones (designed as inhibitors) on reduction with borohydride exchange resin (BER) easily furnished the deoxythiosugars (Fig. 2). It is worth mentioning that the synthesis of these thiosugars as reported in the literature involved lengthy procedures whereas the present methodology turns out to be short and concise. Figure 2 Section B entitled “Synthesis of amines, β-amino acids and novel thiosugar-based dehydroamino acids” comprises a brief introduction on the importance of amines, β-amino acids and dehyroamino acids. In this section the effective utilization of benzyltriethylammonium tetrathiomolybdate as a key reagent for reductive transformations and its application in the synthesis of amines, β-amino acids and dehyroamino acids have been presented. A one pot reduction of azides to amines followed by intermolecular aza-Michael addition employing tetrathiomolybdate was achieved to furnish a number of different β-amino esters as shown in Scheme -4: Scheme 4 The study was further extended to the reduction of a few anomeric azides to afford the corresponding anomeric amines and derivatives. (Fig. 3) Figure 3 A one-pot thia-Michael addition-vinyl azide reduction in a tandem fashion employing benzyltriethylammonium tetrathiomolybdate was studied and was shown to be effective for the synthesis of thiosugar derived dehydroamino acid derivatives. (Scheme – 5) Scheme 5 Section C entitled “Molecular docking studies of deoxythiosugar probes” gives an overview of different glycosidases, HIV-1 protease and their inhibitors. This section also deals with a brief introduction on active site conformations of potent inhibitors. In this connection we have studied the crystal conformations of the synthesized molecules whose conformations were the same as that of the existing inhibitors in the active site. (Fig. 4) With this background in silico study of the synthesized deoxythiosugar probes was conducted on human glycosidases: α-mannosidase, α-galactosidase, β-glucosidase and HIV-1 protease, respectively. Figure 4 Molecular docking was carried out using Autodock suite, molecular modeling simulation. Separate docking procedures were employed for the four different receptors. The PDBs representing the four enzyme targets were 2V3D, 3H53, 1X9D and 3I8W for β–glucosidase, α–galactosidase, α–mannosidase and HIV–1 protease respectively. The control compounds used for α–mannosidase were mannostatin and kifunensine. NMB, THK, and BED were the positive controls for HIV–1 protease. Similarly, NBV and cyclophellitol were the controls used for β–glucosidase and NOJ, N–methyl calystegine B2 for α–galactosidase. (Fig. 5) Ligands TGSB68 and TGSB482 had the energy value of –6.49 kcal/mol comparable to that of the average reference value of the positive control, and thus, the potent candidate as identified by molecular docking to HIV-1 protease. (Fig. 6a) The control compounds used for α–mannosidase were mannostatin and kifunensine, which bind with mean binding energy of -9.11 and -5.56. In the case of α–mannosidase, the same compounds TGSB68 and TGSB482 were selected due to comparable energy and a good cluster size with that of positive control. (Fig. 6b) For β– glucosidase, ligands TGSC108 and TGSC236, which had comparable values to that of positive control was identified as the Figure 5 Figure 6 potent candidate. (Fig. 6c) In the case of α–galactosidase, again the ligands TGSB68 and TGSB482 were selected based on binding energies. (Fig. 6d) In conclusion, the concept analogy (deoxy nature, planarity, thiosugar framework, lactone moiety) for the design of inhibitors indeed worked positively. The results are really encouraging. An in vivo study of the synthesized novel thiosugar probes will certainly provide a potent inhibitor. Section D entitled “Research methodology” provides experimental procedures adopted with details of synthesis. Section E entitled “Bibliography” provides the references cited in this work.

Glycosidase Inhibitors

Thiosugars

Amino Acids - Synthesis

Sulfur Transfer Reagents

HIV-Protease Inhibitors

Thialactone

Amines - Synthesis

Thiosugar Dehyroamino Acids - Synthesis

Deoxythiosugars

Azidothialactones

Dehyroamino acid

Glycosidase Inhibitors

Thiosugar Lactones - Synthesis

Deoxythiosugar Probes

Deoxythiosugars

HIV-1 Protease Inhibitors

Deoxythialactones

Deoxythiosugar-based Lactones

Organic Chemistry