Synthesis,characterization, and solution properties of 5-ethyl-substituted poly(L-prolines). Synthesis of cis- and trans-5-ethyl-L-proline and optically active poly(cis-5-ethyl-D-proline)

This article reports a continuation of our work on the substituent effects on the preferred helical conformations and the mutarotation of substituted poly(L -prolines). The size of the substituent has been increased from a methyl group to an ethyl group in the 5 position. The purpose is twofold: (i) according to our theoretical conformational energy calculations, an ethyl group in the 5 position can exert a greater steric effect than can a methyl group; and (ii) the rotation-isomerization of the ethyl group introduces a new intriguing fact to the problem. The cis isomer of 5-ethylproline was synthesized by catalytic hydrogenation of Δ′-2-ethylpyrroline-5-carboxylic acid, whereas for trans-5-ethylproline, a chemical separation method involving p-toluenesulfonyl chloride was used. The resolution of cis-5-ethylproline and the assignment of absolute configurations have been carried out by fractional crystallization and circular dichroism spectroscopic techniques, respectively. Poly(cis-5-ethyl-D -proline) was obtained from its corresponding N-carboxyanhydrides via a ring opening polymerization.     

Separation of new antidiabetic agent,N-(trans-4-isopropylcyclohexylcarbonyl)-d-phenylalanine and three related compounds by RP-HPLC

Summary A high-performance liquid chromatographic method is proposed for the simultaneous separation of two pairs of isomers:N-(trans-4-isopropylcyclohexylcarbonyl)-d-phenylalanine, (Nateglinide) andN-(cis-4-isopropylcyclohexylcarbonyl)-d-phenylalanine,trans-4-isopropylcyclohexane-carboxylic acid andcis-4-isopropyl-cyclohexanecarboxylic acid using a C₁₈ column. The mobile phase is a ternary mixture of acetonitrile-methanol-0.1 M ammonium dihydrogen phosphate buffer, pH 3.0 (5:2:4 v/v/v) and UV detection at 210 nm. Precision, linearity, limit of detection and recovery were also evaluated for each compound. Satisfactory results were obtained.     

Synthesis of perfluorochemicals for use as blood substitutes,Part I. Electrochemical fluorination of N-methyldecahydroquinoline and N-methyldecahydroisoquinoline

Electrochemical fluorination of N-methyldecahydroquinoline afforded mainly a mixture of $\text{cis}$ and $\text{trans}$ N-(F-methyl)-F-decahydroquinoline, their rearranged isomers and F-propyl-F-cyclohexane arising from the cleavage at carbon-nitrogen bonds, in a ratio of approximately 2:4:6:3. N-Methyldecahydroisoquinoline was also fluorinated electrochemically to give a mixture of $\text{cis}$ and $\text{trans}$ N-(F-methyl)-F-decahydroisoquinoline, their rearranged isomers and 1-(F-ethyl)-2-(F-methyl)-F-cyclohexane in a ratio of approximately 4:4:6:1. No correlation was found between the $\text{cis}$ and $\text{trans}$ ratio of starting materials and that of the corresponding perfluorinated amines. Fluorination of N-methyl-1,2,3,4-tetrahydroquinoline gave much lower yields.     

Synthesis of 6,7,8,9-tetrahydro-N,N-di-n-propyl-1H-benz[g] indol-7-amine,a potential dopamine receptor agonist

In this work, the synthesis of 6,7,8,9-tetrahydro-N,N-di -n-propyl-1H-benz[g]indol-7-amine (1) is described. This compound was designed as an indole bioisostere to the known dopamine receptor agonist 5-OH-aminotetraline 2 . The key step of the synthesis was a Mukaiyama type aldol condensation between the dimethyl acetal of 1-(p-toluenesulfonyl)pyrrole-3-acetaldehyde ( 4 ) and 4-di-n-propylamino-1-trimethylsilyloxycyclohexene ( 8 ) followed by cycloaromatization to afford 1-p-toluenesulfonyl-6,7,8,9-tetrahydro-N,N-di-n- propyl-1H-benz[g]indol-7-amine ( 10 ). Scission of the sulfonamide bond in 10 gave the target compound 1 . A byproduct which was isolated was assigned to the structure of 1-(p-toluenesul-fonyl)-6-[3-[1-(p-toluenesulfonyl)]pyrrolyl]indole ( 11 ). This compound was also synthesized in good yield by an acid catalyzed dimerization of the dimethyl acetal of 1-(p-toluenesulfonyl)pyrrole-3-acetaldehyde ( 4 ). Preliminary screening of 1 indicated that it possesses central dopamine receptor agonist properties.     

Stereochemical studies. Part 67. Saturated heterocycles. Part 52. The mass spectra of some condensed skeleton 1,3-oxazin-4-one derivatives

The mass spectrometric behaviour of twenty saturated heterocyclic compounds with a 1,3-oxazin-4-one moiety fused with cis or trans anellation to a cycloalkane ring (C₅-C₈) was studied. The roles of the C-2 and N-3 substituent(s) were found to be characteristic, while the size of the cycloalkane ring seemed to be unimportant. Some fragmentation processes involving breakdown of the oxazinone ring of the cis or trans isomers displayed significant stereoselectivity. A striking new decomposition process involving significant chlorine elimination from the molecular ion of some 2-p-chlorophenyl derivatives was observed and was studied in some detail.     

The stereochemistry of the dichlorocobalt(III) complexes with (2S,5S,9S)- and (2S,5R,9S)-trimethyltriethylenetetraamines

Dichlorocobalt(III) complexes of (2S,5S,9S)-trimethyltriethylenetetraamine (L₁) and (2S,5R,9S)-trimethyltriethylenetetraamine (L₂) have been prepared. Both L₁ and L₂ coordinate to the cobalt(III) ion to give three isomers: Λ-cis-α, Δ-cis-β, trans isomers for L₁ and Δ-cis-α, Δ-cis-β, trans isomers for L₂. Each of the trans-dichloro complexes of the two ligands have been isomerized stereospecifically to the cis-α-dichloro complex in methanol, and each of the cis-α-dichloro complexes stereospecifically to the trans-diaqua complex in water. Both the geometrical and optical inversions took place at the same time in the observed stereospecific isomerizations.     

Design,synthesis, resolution,and stereochemical assignment of a conformationally rigid chiral ligand derived from anthracene and a dienophile containing a pyridine moiety

The conformationally rigid chiral ligand, trans-12-(pyridin-2-yl)-9,10-dihydro-9,10-ethanoanthracene-11-carboxylic acid ethyl ester, 1, was designed and synthesized in racemic form. Both isomers were successfully obtained in enantiomerically pure form through classical resolution using l-(+)-tartaric acid in acetonitrile. The nature of the diastereomeric complex formed in this resolution was elucidated using single crystal X-ray crystallographic studies. The absolute configuration of (+)-1 was unambiguously assigned as (11S,12S) by single crystal structural analysis of salt 5 formed from (+)-1 and l-(+)-tartaric acid.     

The mass spectral rearrangements of aryl propenyl sulfones. An electron impact induced smiles type rearrangement

The mass spectral behavior of trans-1-arylsulfonyl-2-arylsulfenyl-propenes, trans-1-arylsulfonyl-2-arylsulfinyl-propenes and trans-1, 2-(arylsulfonyl)-propenes was examined. A Smiles type rearrangement was present in the sulfonyl-sulfides, but was completely absent in the trans-1-arylsulfonyl-2-arylsulfinyl-propenes and trans-1, 2-(arylsulfonyl)-propenes. Vinyl migration to the sulfone oxygen predominates over aryl migration in all of the compounds studied. The mass spectra of the cis and trans isomers of 1-p-tolylsulfenyl-2-p′-tolysulfonyl-propene and 1, 2-(p-tolylsulfonyl)-propene are also described.     

Cis/trans ISOMERIZATION OF CAROTENOIDS BY THE TRIPLET CARBONYL SOURCE 3-HYDROXYMETHYL-3,4,4-TRIMETHYL-1,2-DIOXETANE*

Abstract— The interaction of biological carotenoids with 3-hydroxymethyl-3,4,4-trimethyl-1,2-dioxetane (HTMD), a thermodissociable source of electronically excited ketones, was investigated using reversed-phase high-performance liquid chromatography. Incubation of the all-trans isomers of β-carotene, lycopene and canthaxanthin with HTMD led to significant trans-to-cis isomerization, with cis isomers accounting for 20–50% of products formed (the balance assigned as oxidation products). The isomers forming from all-trans-β-carotene were identified as 9-cis-, 13-cis- and 15-cis-β-carotene by cochromatography of cis isomer standards and by on-line diode array absorbance spectroscopy. An HTMD-dependent cis-to-trans isomerization was observed in incubations started with 15-cis-β-carotene, and it occurred more rapidly and to a greater extent than the isomerization of all-trans-β-carotene. The isomer patterns generated from lycopene and β-carotene are generally similar to those reported recently for various human tissues (Stahl et al, 1992, Arch. Biochem. Biophys. 294 , 173–177).     

Polymerization and conformational studies of poly(trans-3-ethyl-D and L-proline)

Poly(L -trans-3-ethylproline), L -PT3EP, and poly(D -trans-3-ethylproline), D -PT3EP, were prepared by ring opening polymerization of the corresponding N-carboxyanhydrides (NCA) using triethylamine as an initiator. Using circular dichroism spectroscopy, it was shown that the incorporation of an ethyl group at the 3 position of the pyrrolidine ring caused a noticeable change in the conformational behavior of the polymer in solution. The ethyl group limited to some extent rotation of the polymer chain around the C_? ? CO bond and prevented the mutarotation between the two forms found in poly-L -proline polymers.     

Temperature and Concentration Dependent Circular Dichroism of Mono- and Di-cis Isomers of (3S,3′S)-Astaxanthin Diacetate

The circular dichroism (CD.) spectra of all-trans-(3S, 3′S) astaxanthin diacetate and its 9-cis, 13-cis, 9,9′-di-cis, 9,13′-di-cis, and 9,13-di-cis isomers conform to the rules previously formulated for optically active carotenoids with a 4-oxo-β-end ring containing an asymmetric C-atom [1]. Thus the CD. bands of the all-trans and the di-cis isomers show the same signs whereas those of the mono-cis isomers have opposite signs. The CD. spectra of all the astaxanthin diacetate isomers invert sign upon cooling to ?180°. The CD. spectra of the 9-mono-cis and 9,9′-di-cis isomers and to a lesser extent also those of the 9, 13′-di-cis and 9, 13-di-cis isomers are concentration dependent at ?180°, with the longest wavelength band giving at the higher concentration a bisignate CD. curve under the main absorption characteristic of aggregation. This phenomenon has been observed only in isomers with a 9-cis linkage. It is suggested that steric hindrance prevents such aggregation taking place in the other isomers.     

Studies on quinones. XII. Cycloketalization of michael adducts from hydroxyquinones

The reaction of 2-hydroxy-3-(1-phenyl-3-oxobutyl)-1,4-naphthoquinone ( 1 ) with either acidic methanol or a mixture of trimethyl orthoformate, methanol and ammonium chloride resulted in the formation of the p-quinonic cycloketals: trans- and cis-4-phenyl-2-methyl-2-methoxy-3,4-dihydro-2H-naphtho[2,3-b]pyran-5,10-dione ( 2a,2b ). Cyclization of the Michael adducts 6, 10 and 11 , which are structurally related to 1 , with trimethyl orthoformate-methanol-ammonium chloride gave the corresponding p-quinonic cycloketals 7, 12 and 13 . The structures of the regioisomers 2a and 2b are proposed based on the spectral properties of compound 7 and by analysis of its proton nmr spectra.     

Herstellung von Dihydro-, Tetrahydro- und Hexahydrochelidamsäure-Derivaten

Preparation of dihydro-, tetrahydro- and hexahydro-chelidamic-acid derivatives. Three methods for the preparation of 4-oxo-2,6-piperidine-dicarboxylic acid ( 3 ) and derivatives, required as a synthon for betalaine pigments, were explored. The best method was found to be the catalytic hydrogenation of chclidamic acid ( 1 ) with 5% Rh/Alox in water under 2.7 atm. H₂ for 33 h at 70° and subsequent esterification with methanol which gave 42% of cis, cis-4-hydroxy-2,6-piperidine- ( 7 ) and 10% of 2,6-cis-piperidine-dicarboxylic acid dimethyl ester ( 8 ), readily separable by chromatography. Oxidation of 7 with dimethylsulfoxide and a carbodiimide attached to a polymer afforded 90% of 4-oxo-2,6-cis-piperidine-dicarboxylic acid dimethyl ester ( 19 ). Other methods of oxydizing 7 to 19 were less successful. The electrochemical reduction of 1 followed by esterification with methanol led in a low yield to a mixture of 4-oxo-0-2,6-trans-piperidine-dicarboxylic acid dimethylester ( 24 ), its dimethyl acetal 25 and presumably trans-4-hydroxy-r-2, cis-6-piperidine-dicarboxylic acid dimethyl ester ( 26 ). Reaction of 4-oxo-hepta-2E, 5E-dienoic acid ( 35 ) with aqueous ammonia gave a 98% yield of a 3 : 2 mixture of cis- and trans-ammonium-4-oxo-2, 6-piperidine-dicarboxylate ( 39 and 40 ). The above mentioned catalytic hydrogenation method was also applied to N-ethyl-chelidamic acid ( 16 ) to give a 4:6 mixture of the N-ethyl derivatives 17 and 18 . Furthermore, a number of functional derivatives of 5 , of 19 , of 39 and of 40 were prepared. Oxidation of the hydroxy-diester 7 with dimethylsulfoxide and a carbodiimidc derivative in the presence of trifluoroacetic acid afforded 4-oxo-1,2,3,4-tetrahydro-2, 6-pyridine-dicarboxylic acid dimethyl ester ( 50 ). This ester was also obtained under the same conditions from thc keto-diester 19 .     

Cyclopentyl derivatives of 8-azahypoxanthine and 8-azaadenine. Carbocyclic analogs of 8-azainosine and 8-azaadenosine

Four types of carboeyclic analogs of 8-azahypoxanthine and 8-azaadenine nucleosides have been prepared. This group of analogs is comprised of derivatives having the (±)-as-3-(hydroxy-methyl)cyclopentyl,(±)-trans-3-hydroxy-cis-4-(hydroxymethyl)cyclopentyl), (±)-trans-2-hydroxy-cis-4-(hydroxymethyl)cyclopentyl, and (±)-trans-2, trans-3-dihydroxy-cis-4-(hydroxymethyl)-cyelopentyl groups at position 3 of 3,6-dihydro-7H-v-triazolo[4,5-d]pyrimidm-7-one and of 7-amino-3H-v-triazolo[4,5-d]pyrimidine. Diazotization of (5-amino-6-chloropyrimidin-4-yl-amino)eyclopentane derivatives and acidic hydrolysis, without isolation of the resulting 7-chloro-3H-v-triazolo[4,5-d]pyrimidines yielded the 8-azahypoxanthine derivatives (III). Treatment of unpurified 7-chloro-3H-v-triazolo[4,5-d]pyrimidines with anhydrous ammonia gave the 8-azaadenine derivatives (IV). The cyclopentane analogs of 8-azaadenylic acid and of 8-aza-adenosine 3′,5′ -cyclic monophosphate were prepared from the 8-azaadenosine analog.     

Saturated heterocycles, 248. Synthesis of 2,4-dioxo and 4-oxo-2-thioxo derivatives of octahydrocyclopenta[d]pyrimidines

Unsubstituted and 1-benzyl-substituted cis-cyclopenta[d]pyrirnidine-2,4-diones and cis-2-thioxo-cyclopenta[d]pyrimidin-4-ones 9a,b and 10a,b were prepared from the corresponding cis-2-amino-1-cyclopentanecarboxylates 3 and 5 with potassium cyanate and thiocyanate. It was found that the cis derivatives 7a-h readily underwent ring closure, resulting in 3-substituted cis-2,4-cyclopenta[d]pyrimidinediones and cis-2-thioxocyclopenta[d]pyrimidin-4-ones 11a-d and 12a-d , whereas the trans counterparts 8a-d failed to cyclize, but gave hydrolysed amino acid derivatives 13a,b and 14 . This difference in the reactivities of the cis and trans isomers is a further example of the difficulty of preparing cyclopentane trans-fused six-membered 1,3-heterocycles by ring closure.     

Synthesis of (-)-delta6,1-3,4-trans-tetrahydrocannabinol, as well as (+)-delta 6,1-3,4-trans-tetrahydrocannabinol

Acids, such as p-toluenesulfonic acid, mediate the direct formation of optically active (?)-Δ6,1-3,4-trans-tetrahydrocannabinol from (+)-cis-or (+)-trans-p-menthadiene-(2,8)-ol-(1) and olivetol.     

The cis-trans Isomerisation of Homologous 2-Hydroxycycloalkanecarboxylic Acids under Basic Conditions

The cis→trans isomerisation of homologous 2-hydroxycycloalkanecarboxylic acids in strongly basic aqueous solution was studied starting from the cis isomers. It was found that the cyclopentane, cyclohexane and cycloheptane homologues afforded synthetically useful amounts of the trans acids and the procedure resulted in relatively small quantities of the corresponding olefinic acids. In contrast, the isomerisation of the cis-2-hydroxycyclooctanecarboxylic acid produced roughly equal amounts of the cis and trans isomers and the 1-cyclooctenecarboxylic acid at equilibrium. Molecular modelling with the PM3 semiempirical method of the reactants, products and the intermediates applying explicit water molecules as reaction medium gave a fair estimate for the rate sequence of the idealised （dehydration-free） isomerisation reactions in aqueous base solution.     

Synthesis,stereochemistry and pharmacological activity of rac.-cis-tetrahydro-6-hydroxy-7-(4-methoxyphenyl)-1,4-thiazepin-5(2H)-ones

Reaction of 2-aminoethanethiol ( 3 ) with trans-3-(p-methoxyplienyl)glycidate ( 4 ) gave the rac.-cis-1,4-thiazepinone 5 and a by-product 6 . The structure of 5 was proven by X-ray crystallography. The X-ray data revealed that this compound adopts the chair conformation in the solid state and the heterocyclic ring is sevenmembered. The structure of the by-product 6 was elucidated on the basis of spectral data. Compounds 9 and 10 were inactive as calcium channel blocking agents.     

Polyimidines: A new class of polymers. III. A comparison of isomers of polypyromellitimidines

The cis (3,3,5,5-), trans (3,3,7,7-), oxo, and thio analogs of tetraphenylpyromellitide were polymerized with 1, 6-hexane diamine, p-phenylene diamine, and p,p'-diaminodiphenyl ether under various conditions. A comparison was then made of reactivity of the isomers and of the properties of the polymers. In general the thio monomers were more soluble and reactive than the oxo. They also gave more thermally stable polymers. The cis isomers of the monomers were more soluble than the trans, but the trans were more reactive. The least stable of the 12 polymers prepared was that from the cis–oxo monomer and 1,6-hexane diamine. It gave a 10% weight loss at 300°C in air and 340°C in nitrogen by TGA. The most stable polymer was from the reaction of the cis–thio pyromellitide with p,p'-diaminodiphenyl ether, which showed 10% weight losses by TGA at 560 and 650°C in air and nitrogen, respectively. The polymers were stable in hot dilute hydrochloric acid and sodium hydroxide. They were all soluble in chloroform, dimethylformamide, and sulfuric acid. Polymers that contained sulfur were also soluble in carbon tetrachloride, benzene, xylene, and toluene. Brittle films could be cast from solution or melt-pressed.     

One step synthesis of aziridines by the Michael type addition of free sulfimides: Preparation and absolute configuration of optically active acylaziridines

The Michael type additions of diphenyl N-unsubstituted sulfimide (free sulfimide) to various electrophilic olefins were carried out. The reaction with cis- and trans-dibenzoylethylene, dimethyl-fumarate, dimethylmaleate, benzalacetophenone and benzalacetone gave mainly the corresponding trans-2-acylaziridines and trans-enaminoketones. However, phenyl vinyl sulfone or acrylonitrile afforded not the corresponding aziridine but diphenyl-N-2-cyano or N-2-phenylsulfonylethylsulfimide, a simple Michael adduct When optically active (+)-(R)-o-methoxyphenyiphenyl free sulfimide was treated with such an α,β-unsaturated carbonyl compound as benzalacetopbenone, an optically active 2-acylazindine, i.e., (-)-trans-2-benzoyl-3-phenylaziridine was obtained in ca 30% optical purity and its absolute configuration was assigned as (2R,3S) upon chemical transformation to the configuration-ally known 2-phenyl-2-benzoylamino-1-ethanol or by comparing its CD spectrum with that of (1R,2R)-1-phenyl-2-benzoyl-cyclopropane. Meanwhile, (-)-(S)-o-methoxyphenylphenyl free sulfimide was found to react with benzalacetophenone to afford (+)-trans-2-benzoyl-3-phenylaziridine of 25% optical purity. Effects of solvent and temperature on both die distribution of the products ratio and the optical yield were examined.