Intercalation of ferrocene and dimethylaminomethylferrocene into α-Sn(HPO4)2 · H2O and α-VOPO4 · 2H2O

The intercalation of ferrocene and dimethylaminomethylferrocene into -tin(IV) hydrogen phosphate (SnP) and -vanadyl phosphate has been investigated. Successful intercalation of 0.81 mol of dimethylamino-methylferrocene into -SnP by an acid-base reaction in aqueous medium to form a bilayer of protonated amines was achieved. However, ferrocene was not intercalated under the same conditions. Intercalation of -vanadyl phosphate by 0.11 mol of ferrocene in acetonic medium at room temperature was effected by a redox topotactic reaction. The voluminous dimethylaminomethylferrocene was not intercalated into -vanadyl phosphate.     

Synthesis of 4′4″(5″)-dibenzo-18-crown-6-disulfonic acid disalsolidinide,disalsolinide, and dianabasinide

New disulfamides of dibenzo-18-crown-6 with salsolidine, salsoline, and anabasine were prepared by condensation of the corresponding alkaloids with 4,4(5)-dibenzo-18-crown-6-disulfonyl chlorides.Presented at the 5th International Symposium on the Chemistry of Natural Compounds (Tashkent, Uzbekistan, May 20–23, 2003).Translated from Khimiya Prirodnykh Soedinenii, No. 5, pp. 413–415, September–October, 2004.     

Synthesis of γ-zirconium phosphate by the fluoro-complex method and the intercalation behavior of some α-diimines

The ammonium form of -zirconium phosphate has been synthesized by the direct precipitation method from fluorozirconate solution in the presence of ammonium dihydrogen phosphate. The hydrogen form Zr(HPO₄)₂ · 2H₂O, was obtained by acid treatment of the ammonium form -Zirconium phosphate , Zr(HPO₄)₂ · H₂O, with a relatively large particle size resulted from fluorozirconate solution in the presence of concentrated orthophosphoric acid. The intercalation behavior of such -diimines as 2,2-bipyridine (bpy) and 1,10-phenanthroline (phen) toward -zirconium phosphate was investigated, and it was found that about 0.2 mol of bpy and 0.5 mol of phen have been incorporated respectively per one mol of the host, with the expansion of interlayer distances. Further incorporation of Cu(H) ions into the interlayer space of these intercalates was possible. The bpy intercalate took up more Cu(II) ions than -zirconium phosphate, indicating that effective pillars are constructed between layers and the ion exchange of Cu(II) ions is facilitated thereby.     

Hexafluoroacetone as Protecting and Activating Reagent. Glycosylated Malic, Citramalic, and Thiomalic Acid Derivatives, New Glycosylated Building Blocks for Drug Design [1]

Summary. Glycosylated -hydroxy and -mercapto acids have been synthesized starting from malic/citramalic/thiomalic acid and Ac₄--D-Glc-NH₂/Bzl₄--D-Glc-NH₂ using hexafluoroacetone as protecting and activating reagent.Dedicated to Prof. Dr. Horst Wilde on the occasion of his 65^th birthday     

New route for the synthesis of 2-thiouracil analogues of 3′-azido-2′,3′-dideoxy nucleosides

Summary Reaction of 3-azido-5-O-tert-butyldiphenylsilyl-2,3-dideoxy-D-erythro-pentofuranoside (5) with silylated 2-thiouracil and 5-alkoxy-2-thiouracils in the presence of trimethylsilyl trifluoromethanesulfonate afforded an anomeric mixture of the corresponding 3-azido-2,3-dideoxy-2-thiouridine derivatives with the -anomer as the main product. Deprotected nucleosides were obtained by treatment with tetrabutylammonium fluoride.

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Ein neuer Weg zur Synthese von 2-Thiouracil-Analogen von 3-Azido-2,3-dideoxy-Nucleosiden

Zusammenfassung Die Reaktion von 3-Azido-5-O-tert-butyldiphenylsilyl-2,3-dideoxy-D-erythro-pentofuranosid (5) mit silyliertem 2-Thiouracil und 5-Alkoxy-2-thiouracil in Gegenwart von Trimethylsilyltrifluormethansulfonat ergab eine anomere Mischung der entsprechenden 3-Azido-2,3-dideoxy-2-thiouridin-Derivate, wobei das -Anomer das Hauptprodukt darstellte. Die ungeschützten Nucleoside wurden mittels Behandlung mit Tetrabutylammoniumfluorid erhalten.

     

Enhanced dissolution and oral bioavailability of α-tocopheryl esters by dimethyl-β-cyclodextrin complexation

Inclusion complexation of heptakis (2,6-di-O-methyl)--cyclodextrin (DM--CyD) with -tocopheryl acetate and -tocopheryl nicotinate in aqueous solution was studied by the solubility method. The aqueous solubilities of the esters were about 10⁵ times increased by DM--CyD complexation. The phase-solubility diagram of the tocopheryl ester-DM--CyD systems showed a typicalA _p type, and the stability constants (K) of high-order complexes were estimated by analyzing the upward curvature of the diagrams. The solid complex of -tocopheryl nicotinate with DM--CyD in a molar ratio of 12 was prepared by the kneading method. The dissolution rate of the solid complex was much greater than that of the drug itself, and the rapidly dissolving form of -tocopheryl nicotinate, as an example, showed a markedly increased bioavailability (about 70-fold) after oral administration to fasted dogs.     

The structure of 16, 17β-epoxy-17α-pregn-5-en-3β-ol-20-one monohydrate

The structure of the title compound (1) has been studied by means of X-ray diffraction. The region of cycleD in epoxide1 was compared with that of the 16,17-epoxy derivatives of progesterone and pregnenolone (studied previously) as well as with that of the respective 16,17- and 16,17-cyclopropano analogs. In contrast to the 16,17-epoxy-20-oxo derivatives, in compound1 the electron conjugation of the epoxide ring with the CH₃CO group at C(17) is partly disrupted. Moreover, the steric congestion at C(17) is significantly less pronounced in 16,17-epoxide1 than in its 16,17-counterpart. Both of these factors, especially steric decongestion, are favorable for nucleophilic attack at C(17) in the molecule of1. The X-ray diffraction data do not contradict the previously advanced mechanism of epoxide ring opening in 16,17- and 16,17-epoxy-20-oxo steroids by nucleophilic reagents.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 2, pp. 401–405, February, 1993.     

Zur Kenntnis der gemeinsamen Einwirkung von elementarem Selen und gasförmigem Ammoniak bzw. Ethylenimin auf Ketone

Elemental sulfur reacts with ketones and gaseous ammonia at room temperature yielding thiazoline-3 in excellent yields. Under the same conditions elemental selenium does not react at all. Attempts using the known techniques which have been applied in improving the reactivity of slowly reacting ketones in thiazoline-3-synthesis have been unsuccessful (Exp. No. 1–17). The reaction of -halogenketones with sodiumhydrogenselenide to synthesize -hydroselenoketones gives only the original ketones and selenium in almost quantitative yields (No. 18–23). The same is observed with -haloketones and sodium ore magnesium-diselenides (No. 24–45). The explanation of these unexpected results is the strong reducing power of the hydrogenselenide (No. 46–52). Even -bromoketones with activated bromine (i.g. by phenyl groups) were reduced by sodiumhydrogensulfide giving red undefinite oils. However, -chloroketones give -mercaptoketones in excellent yields (No. 53–61). Hydrogenselenide reduces -mercaptoketones to sulfur and ketones in the presence of triethylamine (No. 62–67). Also the transformation of -selenocyanketones to ,-diketodisenides by alkali or the oxidative hydrolysis of selenium-BUNTE salts does not work and gives elementary selenium only. Studies about the concomitant reaction of elementary selenium and ethylenimine on ketones were continued (No. 68–82).

     

The μ-and δ-opioid pharmacophore conformations of cyclic β-casomorphin analogues indicate docking of the Phe3 residue to different domains of the opioid receptors

Summary Cyclic -casomorphin analogues with a d-configured amino acid residue in position 2, such as Tyr-c[-Xaa-Phe-Pro-Gly-] and Tyr-c[-Xaa-Phe-d-Pro-Gly-] (Xaa=d-A₂bu, d-Orn, d-Lys) were found to bind to the -opioid receptor as well as to the -opioid receptor, whereas the corresponding l-Xaa² derivatives are nearly inactive at both. Low-energy conformers of both active and nearly inactive derivatives have been determined in a systematic conformational search or by molecular dynamics simulations using the TRIPOS force field. The obatained conformations were compared with regard to a model for -selective opiates developed by Brandt et al. [Drug Des. Discov., 10 (1993) 257]. Superpositions as well as electrostatic, lipophilic and hydrogen bonding similarities with the -opioid receptor pharmacophore conformation of t-Hpp-JOM-13 proposed by Mosberg et al. [J. Med. Chem., 37 (1994) 4371, 4384] were used to establish the probable -pharmacophoric cyclic -casomorphin conformations. These conformations were also compared with a -opioid agonist (SNC 80) and the highly potent antagonist naltrindole. These investigations led to a prediction of the -and -pharmacophore structures for the cyclic -casomorphins. Interestingly, for the inactive compounds such conformations could not be detected. The comparison between the -and -pharmacophore conformations of the cyclic -casomorphins demonstrates not only differences in spatial orientation of both aromatic groups, but also in the backbone conformations of the ring part. In particular, the differences in ² and ² (70°,-80°; 165°,55°) cause a completely different spatial arrangement of the cyclized peptide rings when all compounds are matched with regard to maximal spatial overlap of the tyrosine residue. Assuming that both the -and -pharmacophore conformations bind with the tyrosine residue in a similar orientation at the same transmembrane domain X of their receptors, the side chain of Phe³ as a second binding site has to dock with different domains.This paper is based on a presentation given at the 14th Molecular Graphics and Modelling Society Conference, held in Cairns, Australia, August 27–September 1, 1995.     

Synthesis and sorption properties of new hybrid chelating sorbents with β-alanine functional groups

A series of -aminopropylsilylated sorbents was obtained from different oxide supports (silica gels, silica fillers, macroporous glasses, alumina) and by the direct synthesis (hydrolytic polycondensation of tetraalkoxysilanes with -aminopropyltriethoxysilane). The highest degree of immobilization was achieved for silicas, while the most convenient solvent was methanol. Sorbents with -alanine functional groups were obtained by the subsequent reaction with acrylic acid. The degree of -carboxyethylation was 1.3–1.9, and the highest content of functional groups (v_COOH = 3.23 mmol g^–1) was achieved for carboxyethylated xero gel synthesized by the copolycondensation of tetraethoxysilane with -aminopropyltriethoxysilane. The sorbents containing -alanine possess a higher selectivity of Cu²⁺ ion sorption than the initial -aminopropylsilylated sorbents.__________Published in Russian in Izvestiya Akademii Nauk. Seriya Khimicheskaya, No. 12, pp. 2620–2625, December, 2004.     

Conformational Heterogeneity of a Tripeptide in the Solid State and in Solution: Characterization of a γ-Turn Containing Incipient Hairpin in Solution

A terminally blocked tripeptide Boc--Ala-Aib--Ala-OMe 1 with noncoded amino acids forms a novel type of hairpin structure containing a -turn instead of a conventional -turn in the central loop region in solution. This new type structural motif was characterized by NMR and restraint molecular dynamics simulation study. In the solid state peptide 1 adopts an extended backbone conformation and self-assembles to form supramolecular -sheet.     

Molecular orbital calculations on the optical rotatory properties of chiral allene systems

The chiroptical properties associated with the ^* transitions in dissymmetric allene systems are calculated and relationships between the chiroptical observables and the stereochemical and electronic structural features of these systems are examined. The calculations are based on the INDO and CNDO/S semiempirical molecular orbital models for the electronic structure of the molecular systems and excited states are constructed in the virtual orbital-configuration interaction approximation. The dipole strengths, rotatory strengths, and dissymmetry factors for the three lowest energy ^* transitions are computed and reported for eleven chiral allene structures. Relationships between absolute configuration and the signs of the ^* rotatory strengths are examined and discussed.     

Diastereomeric Oxathia[n](1,1′)ferrocenophanes

Zusammenfassung Neue Oxathiaferrocenophane wurden durch Umsetzung von 1,1-Bis(hydroxymethyl)ferrocen mit Dithiolen dargestellt, welche Sauerstoff in den Alkylketten enthalten. Die Reaktion von 1,1-Bis(-hydroxyethyl)ferrocenen mit Dithiolen führte zu Mischungen von Diastereomeren, aus welchen reine Stereoisomere isoliert und charakterisiert wurden. Einige Aspekte des stereochemischen Verlaufes dieser Reaktionen werden diskutiert.

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Diastereomere oxathia[n](1,1)ferrocenophane

Novel oxathiaferrocenophanes have been synthesized by the reaction of 1,1-bis(hydroxymethyl)ferrocene with dithiols bearing oxygen in chains. The reactions of 1,1-bis(-hydroxyethyl)ferrocenes with dithiols afforded mixtures of diastereomeric products from which pure stereoisomers were isolated and characterized. Some aspects concerning a stereochemical course of the reactions described are discussed.

     

Substituierte 3-Amino-thiophene und 3-Amino-selenophene aus β-Chlor-α-cyan-zimtsäurenitril

Summary -Chloro--cyano-cinnamonitrile (1) reacts in one step with -oxo-thioles3 or successively with sodium sulphide and -chlorocarbonyl compounds4 to form the 5-substituted 4-amino-2-phenyl-thiophene-3-carbonitriles5. Analogously, the successive reactions of -chloro cinnamonitrile1 with sodium selenide — produced in situ from selene and sodium boronhydride — and -chlorocarbonyl compounds4 yields the 5-substituted 4-amino-2-phenyl-selenophene-3-carbonitriles6.

     

Ring opening of fluoroalkyl-containing α,β-epoxyketones by aromatic amines

Aromatic amines cause ,-epoxyketones containing a -fluoroalkyl group to undergo ring opening at the -position to give -amino--hydroxyketones.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 5, pp. 882–883, May, 1994.     

Silver ion spray reagent for the discrimination of β- and ε-end groups in carotenoids on thin-layer chromatograms

Summary Thin-layer chromatograms of pure carotenoids and natural carotenoid mixtures were dried and sprayed with saturated methanolic silver nitrate solution. Those carotenoids containing -end groups showed a marked bathchromic colour change for each such end group. Thus, -carotene, -cryptoxanthin and zeaxanthin gave a clear red colour while -carotene, -cryptoxanthin and lutein gave deep organge spots after such treatment. Taraxanthin and antheraxanthin could be similarly distinguished. The method was not applicable to paper chromatography.     

Electrochemical oxidation of tetramethyl esters of α,α,ω,ω-alcaneteracarboxylic acids

Cyclization of esters of butane-1,1,4,4- and pentane-1,1,5,5-tetracarboxylic acids during electrolysis in methanol in the presence of Nal produces, with a yield of 95%, the esters of cyclobutane-1,1,2,2- and cyclopentane-1,1,2,2-tetracarboxylic acids. Under similar conditions, esters of the highest ,,,-alkanetetracarboxylic acids undergo iodation and hydroxymethylation due to electrical oxidation of methanol to formaldehyde. During electrolysis in methanol in the presence of NaOAc, the esters of ,,,-alkanetetracarboxylic acids undergo effective hydroxymethylation, followed by cyclization into substituted five- and six-member lactones, or tetrahydrofurans when structurally possible.N. D. Zelinskii Institute of Organic Chemistry, Russian Academy of Sciences, 117913 Moscow. Translated from Izvestiya Akademii Nauk, Seriya Khimicheskaya, No. 10, pp. 2332–2339, October, 1992.     

Membrane transport of dicarboxylic and α-hydroxy carboxylic acids induced by α-amino phosphonates

New -amino phosphonates containing different alkyl and aryl substituents at the -carbon atom were synthesized in high yields by the Kabachnik—Fields and Pudovik reactions. These compounds were studied as carriers of several -hydroxy carboxylic and dicarboxylic acids through liquid impregnated membranes. These -amino phosphonates studied are capable of molecular recognition of oxalic acid among structurally similar -hydroxy carboxylic and dicarboxylic acids. The efficiency and selectivity of mass transfer of oxalic acid increase with an increase in the lipophilicity of the -amino phosphonate.     

Triterpene Glycosides of Astragalus and Their Genins. LXI. Occurrence of Cycloartane 6-O-Monodesmosides

Cyclosiversigenin 6-O--L-rhamnopyranoside and 6-O--D-glucopyranoside were isolated fromAstragalus coluteocarpusBoiss. (Leguminosae) andAstragalus dissectusB. Fedtsch. et N. Ivanova, respectively. Cyclosiversigenin 5-O--L-rhamnopyranoside was shown to be an artifact forAstragalus coluteocarpus.Thus, the cyclosiversigenin 6-O--D-glucopyranoside that was isolated from certainAstragalusspecies is hypothesized also to be an artifact. Glycosylation of the 6 -hydroxyl group of cycloartanes by D-glucose and D-xylose, in contrast with other substituents, does not change the low-field position of the PMR signal of the 4-CH ₃ group (1.65 2.01 ppm) that is caused by the influence of deuteropyridine directly on the 6 -hydroxyl. Obviously one of the hydroxyls of the -D-glucopyranoside or -D-xylopyranoside residues has the same effect in this instance.     

Condensation of ethyl α-ethoxymethyleneacylacetates withp-bromobenzoyl- and benzylidenehydrazines

Ethyl -ethoxymethyleneacetoacetate and -ethoxymethylenebenzoylacetate react with benzylidenehydrazine andp-bromobenzoylhydrazine to give hydrazones of the corresponding ethyl -formylacylacetates. It was established by¹H NMR and IR spectroscopy that hydrazones, which were obtained from benzylidenehydrazine, andp-bromobenzoylhydrazone of ethyl -formylacetoacetate exist in the ketoenamine (ketoenhydrazine) form, whereasp-bromobenzoylhydrazone of ethyl -formylbenzoylacetate exists in the enolimine (enolhydrazone) form.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 9, pp. 2293–2296, September, 1996.