Amino sugars and their glycosides

Hindle, Neil

January 1995

This thesis describes approaches to the transformation of simple carbohydrates into a polyhydroxylated pyrrolidine and the formation of its glucosides. Chapter one describes the synthesis of the naturally occurring pyrrolidine 2,5-dideoxy-2,5-imino-D-mannitol. Synthesised from di-O-isopropylidene-D-glucose, the key steps are the introduction of nitrogen at C-5 with retention of configuration. Then cyclisation of the nitrogen onto the C-2 position with inversion to form the pyrrolidine ring. Reduction of the aldehyde furnished the polyhydroxylated heterocycle in 3.4% yield over 16 steps. The synthetic compound matched the naturally occurring compound in all respects. Chapter two contains a review of commonly used glycosylation methods. It also describes the glycosylation of di-O-isopropylidene-α-D-glucose as a model system comparing the Koenig-Knorr method to the trichloroacetimidate method using several reaction conditions. Glycosylation of 2,5-dideoxy-2,5-imino-D-mannitol was carried out using the trichloroacetimidate method to synthese all four glucosides. Boron trifluoride etherate and trimethylsilyl trifluoromethanesulphonate were used as catalysts in dichloromethane, diethyl ether and acetonitrile under strictly anhydrous conditions. All four glucosides were prepared 1-O-(αβ-D-glucopyranosyl)-2,5-dideoxy-2,5-imino-D-mannitol and 3-O-(αβ-D-glucopyranosyl)-2,5-dideoxy-2,5-imino-D-mannitol. Biological screening carried out against a wide range of glycosidases and glycosyl transferases indicated that the glucosides showed little inhibition in comparison to 2,5-dideoxy-2,5-imino-D-mannitol. Chapter three describes the isolation and identification of 1-O-(β-D-glucopyranosyl)- 2,5-dideoxy-2,5-imino-D-mannitol from Nephthytis poisonii N.E.Br. a member of the Araceae family found in tropical Africa. Identification was made by comparison with the previously synthesised glucosides of 2,5-dideoxy-2,5-imino-Dmannitol. Investigations of Hyacinthoides non-scriptus (L.) chouard ex Rothm are also discussed. Chapter four describes the synthesis of a diazidolactone that could be used to form a 1,5 disubstituted tetrazole. This would have a second nitrogen functionality in the molecule allowing the possibility of the inclusion of the tetrazole into a peptide sequence. The synthesis was carried out from L-gulono-1,4-lactone. An azido group was introduced selectively at C-2, this unexpectedly occurred with retention of configuration. A second azide was then introduced at C-5, this occurring with the more commonly observed inversion of configuration to afford the 2,5-diazido-2,5-dideoxy-D-manno-1,4-lactone.

547

Synthesis And Characterization Of Zsm-35

Coskun, Zuhal

01 January 2003

No description available.

The synthesis of substituted pyrrolidines, piperidines and hexah[y]droazepines

Hill, Ralph Madison.

January 1937

Thesis (Ph. D.)--University of Wisconsin--Madison, 1937. / Typescript. Includes abstract and vita. eContent provider-neutral record in process. Description based on print version record. Includes bibliographical references: leaf [52].

Die sintese van alkaloiedagtige glikosidase-inhibeerders vanuit monosakkariede

Greyling, Hendrik Frederik

02 June 2014

M.Sc. (Chemistry) / The aim of this study was to investigate alternative routes for the stereocontrolled synthesis of hydroxylated indolizidine, piperidine and pyrrolidine alkaloids, starting from monosaccharides as chiral building blocks. This study was not aimed at improving consisting routes - it was rather aimed at developing new routes towards the synthesis of these alkaloids. Mixed results were obtained in the investigation into alternative routes for the synthesis of the bicyclic poly hydroxylated indolizidine alkaloids, but a new and efficient stereospecific synthesis of polyhydroxylated piperidine- and pyrrolidine alkaloids were developed. The aims and results can be summarised in more detail as follows: a. Stereospecific synthesis of castanospermine. The synthesis of this medium sized nitrogen-containing bicyclic molecule was approached in a unique way. The utilization of bifunctional Wittig- and Wittig-Horner reagents containing nitrogen functionalities was considered promising for the aims of this study. By the usage of known reactions, e.g. Wittig, Wittig-Horner, Schiff-base and Aza-Wittig reactions, it was foreseen that these bifunctional reagents could be coupled in two concurrent steps to dicarbonyl compounds to form a nitrogen containing rings. Several nitrogen containing Wittig reagents were prepared. At the one end of these reagents a phosphonate or phosphine group furnished the phosphorus moiety while the other end of these reagents comprised the nitrogen moiety by reduction of a nitrile group or azide displacement of a leaving group. No coupling was obtained between these bifunctional reagents and a dicarbonyl compound derived from D-glucose and the influence of two functional groups in such close proximity in the Wittig reagent is being further investigated. Coupling was, however, achieved by the utilization of an alternative bifunctional reagent in which a Wittig-Horner reaction was used. The successful implementation of this unique methodology in the synthesis of medium size nitrogen containing ring is being further investigated.

Alkaloids - Synthesis

Indole alkaloids

Pyrrolidine

Piperidine

Synthèse d'oxazolidines et de pyrrolidines trifluorométhylées chirales : applications en synthèse asymétrique / Synthesis of chiral trifluoromethylated oxazolidines and pyrrolidines : applications in asymmetric synthesis.

Lubin, Hodney

19 November 2010

L'oxazolidine trifluorométhylée (trans-Fox) dérivée du (R)-phénylglycinol a été préparée sous forme diastéréoisomériquement pure par résolution dynamique induite par la cristallisation d'un mélange d'oxazolidines cis et trans.La trans-Fox a été utilisée avec succès comme auxiliaire chiral pour des réactions d'hydroxylation par l'oxygène moléculaire et de fluoration électrophile d'énolates d'amide ainsi qu'en réarrangement sigmatropique [2,3] d'amines allyliques. Après clivage, des composés énantiomériquement purs d'une grande importance synthétique sont obtenus.Une voie d'accès à des pyrrolydines trifluorométhylées chirales a été mise au point à partir de la trans-Fox. La trans 2-phenyl-5-trifluoromethylpyrrolidine a été utilisée comme auxiliaire chiral pour des réactions d'alkylation asymétriques. / The trifluoromethylated oxazolidine (trans-Fox) derived from (R)-phenylglycinol was prepared as a single diastereoisomer by a cristallisation induced dynamic resolution of a mixture of cis and trans oxazolidines.The trans-Fox was used with success as a chiral auxiliary for hydroxylation by oxygen and electrophilic fluorination of amide enolates reactions and [2,3] sigmatropic rearrangements of allylic amines. After deprotection, very synthetically useful enantiomerically pure compounds were obtained.An acces to chiral trifluoromethylated pyrrolidines was developped starting from trans-Fox. The trans 2-phenyl-5-trifluoromethylpyrrolidine was used as a chiral auxiliary for asymmetric alkylation reactions.

Fluor

Auxiliaire chiral

Oxazolidine

Pyrrolidine

Hydroxylation

Fluoration

Fluorine

Chiral auxiliary

Oxazolidine

Pyrrolidine

Hydroxylation

Fluorination

Synthesis of Amphibian Alkaloids and Synthesis and Affinity of Novel Cannabinoid Receptor Ligands

Noble, April R.

20 December 2009

Amphibian alkaloids are attractive targets for synthesis due to their biological activity. An important class of amphibian alkaloids is the 2,5-disubstituted pyrrolidine-based family of compounds. There are many synthetic approaches for the preparation of the trans-2,5- disubstituted pyrrolidines, but methods for the construction of the cis-2,5-pyrrolidines are limited. Therefore, it was desired to develop an enantioselective approach for the preparation of cis-2,5-disubsituted pyrrolidines. (+)-Tropin-2-one derived from cocaine was used as starting material to exploit the inherent stereochemistry for construction of the cis-pyrrolidine ring. This permitted the unequivocal assignment of the absolute configuration of the target pyrrolidine. The structurally simple pyrrolidine alkaloid, 225H, was selected as a target to develop a general synthetic approach. The enantioselective synthesis of 225H was achieved in nine steps and good overall yield. The search for potent cannabinoid receptor partial agonist ligands as potential marijuana addiction therapeutic agents has led to an investigation of the synthesis of diaryl ether hybrid analogues of BAY 59-3074. A series of 2-(3-alkyl-5-hydroxyphenoxy)-6- (trifluoromethyl)benzonitriles, 3-(2-cyano-3-(trifluoromethyl)phenoxy)phenylalkanoates, and (3- (benzyloxy)phenoxy)-6-(trifluoromethyl)benzonitriles were synthesized and evaluated in vitro for CB1 affinity. The olivetol diaryl ether analogue was the most potent ligand of the alkyl series, but the diaryl ester analogues exhibited modest affinity for CB1 receptors. The most potent compound of the series was the 2-(3-(benzyloxy)phenoxy)-6- (trifluoromethyl)benzonitrile.

amphibian alkaloids

enantioselective synthesis

pyrrolidine

cannabinoid receptor

marijuana

Transition metal-catalyzed carbon-carbon bond formation utilizing transfer hydrogenation

Montgomery, Timothy Patrick

03 September 2015

A central tenant of organic synthesis is the construction of carbon-carbon bonds. One of the traditional methods for carrying out such transformations is that of carbonyl addition. Unfortunately, traditional carbonyl addition chemistry suffers various drawbacks: preactivation, moisture sensitivity, and the generation of stoichiometric organometallic waste. The research presented in this dissertation focuses on the development of methods that make use of nucleophile-electrophile pairs generated in situ via transfer hydrogenation, which allow the formation of carbonyl or imine addition products from the alcohol or amine oxidation level; streamlining the construction of complex molecules from simple, readily available starting materials. Additionally, studies toward the total synthesis of the fibrinogen receptor inhibitor tetrafibricin, utilizing the methods developed in catalytic carbon-carbon bond formation through the addition, transfer or removal of hydrogen, are presented. / text

Transfer hydrogenation

Iridium

Ruthenium

Carbonyl addition

Pyrrolidine

Imine

The Stereochemistry of Pyrrolidine Ring Biosynthesis in Tobacco

Wigle, Ian D.

11 1900

<p> In four separate experiments, DL-[5-3H]/DL-[5-14C]ornithine, L-[5-3H]/DL- [5- 14C]ornithine, D-[5-3H]/DL- [5- 14C]ornithine and L-[2-3H]/L-[5- 14c]ornithine were administered to intact tobacco plants (Nicotiana tabacum). Nicotine, ornithine and proline were isolated in each of these experiments. In another experiment, R-[1-2H][l ,4-14C] putrescine was administered to intact tobacco plants and nicotine was isolated. The results of these experiments are consistent with the accepted mode of biosynthesis of nicotine from ornithine via putrescine (1,4-diaminobutane), N-methylputrescine, N-methyl-4-aminobutanal and N- methyl-1-pyrrolinium ion. The 3H:14c ratios of nicotine, the distribution of tritium within nicotine as established by chemical degradation and the distribution of deuterium within nicotine as established by 2H NMR are interpreted as showing that L-ornithine is the preferred enantiomer for nicotine biosynthesis, that the decarboxylation of L-ornithine to yield putrescine proceeds with retention of configuration at the reaction site, and that the oxidation of N-methylputrescine to N-methyl-4-aminobutanal proceeds with loss of the 4(S)hydrogen. </p> <p> Contrary to earlier reports, ornithine isolated in the 3H, 14C experiments had a changed 3:14c ratio from the ornithine which was fed. These results are interpreted as showing that L-ornithine is metabolised more rapidly than is D-ornithine in the tobacco plant. </p> <p> In all 3H, 14c experiments, proline was found to contain at least a small amount of tritium. In particular, when L-[2- 3H]/L-[5-14C] ornithine served as substrate, proline was found to contain 40 + 1% of the tritium, relative to 14C, that had been present in the feeding material. This result is interpreted as showing that, contrary to earlier reports, L-ornithine can be converted into proline via either a-keto-s-aminovaleric acid or glutamic semialdehyde. Together with the 3H: 14C ratios of proline in the other experiments, the results of this work are interpreted as showing that, when DL-ornithine serves as the substrate for proline biosynthesis in tobacco, 88 + 1% of the proline arises from D-ornithine via a-oxidation, 7 + 1% of the proline comes from L-ornithine via a-oxidation and 5 + 1% of the proline is produced from L-ornithine via s-oxidation. </p> / Thesis / Master of Science (MS)

pyrrolidine ring biosynthesis

Tobacco

stereochemistry

proline biosynthesis

ornithine

Syntheses via modifications of the Knorr-Paal procedure :|bA. Derivatives of 2,6-dioxa-10-azatricyclo[5.2.1.0[superscript 4,10]]decane ; B. Highly sterically crowded 1,2,5-trialkylpyrroles and pyrrolidines

Burnham, Weldron Severin

01 June 1969

Earlier work in these laboratories on the heterotricyclic system 2,6-dioxa-10-azatricyclo[5.2.1.04,10]-decane, formed from 1,4-diketones and 2-amino-1,3-propanediols by a product-water-azeotroping procedure, was extended with the synthesis of analogous compounds, e.g., the 1,4,7-triethyl-, 1,7-dimethyl-4-isopropyl-1,7-diethyl-4-isopropyl-, 1,7-dimethyl-3- and 4-phenyl- compounds. The 1,7-dimethyl heterotricycle, the kinetically-controlled product, was accompanied by the thermodynamically-controlled product, 2-(2,5-dimethyl-1-pyrryl)-1,3-propanediol. The 1,7-diethyl heterotricycle was also accompanied by the isomeric pyrrole as were the 1,7-dimethyl-3- and 4-phenyl compounds. A scheme postulating a common intermediate is presented. The interesting analogous compounds, 1,7-dimethyl-2-oxa-6-thia-10-azatricyclo[5.2.1.04,10]decane, 1,4,7-trimethyl-2,6-dioxa-11-azatricyclo[5.3.1.04,11]undecane and 11-hydroxymethyl- and 11-methyl-9,13-dioxa-14- azatetracyclo[6.5.1.02,7 011,14]tetradeca-2,4,6-triene were also prepared. The syntheses in good yields of a considerable number of moderately to severely sterically crowded 1,2,5-trisubstituted pyrroles by means of modifications of the Knorr-Paal condensation are described in this work. The classical procedure succeeded in moderately sterically-crowded cases, e.g., R2=R5=Me, R1=i-Pr; R2=R5=Et, R1=i-Pr. A product-water azeotroping procedure succeeded in more severely sterically-crowded cases, e.g., R2=R5=Et, R1=i-Pr; R2=R5=Me, R1=Me3-CCH2; R2=R5=i-Pr, R1=PhCH2. Highly sterically-crowded pyrroles, e.g., R2=R5=Me, R1=t-Bu, PhSO2, adamantyl, PhCH2CMe2; R2=R5=Et, R1=t-Bu; R1=R2=R5=i-Pr; R2=R5=t-Bu, R1=Me, Et, PhCH2, were obtained using titanium tetrachloride as a Lewis acid catalyst and as a water scavenger. Infrared spectra of the reacting mixtures provided evidence pertinent to the mechanism of the reaction, which is discussed. All of the pyrroles described above were easily catalytically hydrogenated over platinum oxide or rhodium-on-alumina under low hydrogen pressure to the corresponding pyrrolidines. A study into the stereochemistry of the hydrogenation, using 1-benzyl-, 1-ethoxycarbonylmethyl-, and 1-(2,2,2-trifluoroethyl)-2,5-dialkylpyrroles, showed that when R2=R5=Me, Et, R1=PhCH2; R2=R5=Me, R1=CF3CH2 a mixture of cis- and trans-2,5-dialkylpyrrolidines was obtained. Only the cis-isomer was obtained when R2=R5=Me, Et, R1=CH2CO2Et; R2=R5=i-Pr, R1=PhCH2. Several of these heterotricyclics, pyrroles, and pyrrolidines were submitted for pharmacological testing. Results for these compounds as hypotensive agents are presented.

Pyrrolidine

Hydrogenation

Hypertension

Chemistry

Organic

Research

Chemistry

Physical Sciences and Mathematics

Isolation of Flavonoids from Prunus Avium and Synthesis of Polyhydroxylated Pyrrolidines and Anilines as Potential Antibacterial Agents

Bollareddy, Endreddy

01 1900

<p> This thesis describes the isolation and structural determination of flavonoids from the heart wood of Prunus avium as well as synthesis of polyhydroxy pyrrolidine derivatives and aniline core structures as potential antibacterial agents. Nitrogen-synthons containing saturated heterocyclic systems and aniline core structures are important synthons in organic chemistry because of their presence in many biologically-active natural products. Mycobacterial viability is dependent upon the ability of the organism to produce an intact cell wall. Therefore, compounds that interfere with the biosynthesis of the cell wall complex glycons have the potential to become new drugs for the treatment of mycobacterial infections. The oligosaccharide galactan is one of the major structural components of the outer wall of the micro-organism. Galactofuranose is essential for cell growth and survival and therefore, its biosynthesis constitutes a new drug target. The biosynthetic process involves several enzymes having Uridine-diphosphogalacto furanose (UDP-Galf) as the substrate; uridine 5^1 -diphosphogalacto pyranose mutase which catalyzes the interconversion of UDP galacatopyranose to UDP-galactofuranose as well as Galf-transferase. We are seeking and designing molecules that could be mechanistic probes and/or inhibitors of efflux pumps to potentially combat multidrug resistance.</p> <p> The isolation and structure-determination of six naturally occurring Flavan-type Natural products was performed. Such derivatives are known to reverse multiple-drug-resistance (MDR) in persistent microbial infections. The synthesis of pyrrolidine-based antibacterial agents was attempted using two different approaches from tartaric acid. These derivatives were designed as potential transition-state mimics of a carbohydrate processing enzyme specific to TB. A synthetic approach to the aromatic core structure of the antibacterial agent Platensimycin was also investigated. The synergistic use of cytotoxic agents in conjunction with efflux-pump modulators is an emerging area of research in the MDR field; our efforts to make available materials for high-throughput screening in this area will be described.</p> / Thesis / Master of Science (MSc)