Synthesen von N-substituterten o-Methylthioanilinderivaten

Zusammenfassung Methylierung von o-Aminothiophenol lieferte o-Methylmercapto-anilin, dessen Tosylat zur Herstellung des Tosylates der N-(o-Methylmercaptophenyl)--aminopropionsäure verwendet wurde. Cyclisierung von -(2-Methylmercaptodiphenyl)-aminopropionsäure ergab 1-(2-Methylmercaptophenyl)-4-oxo-1,2,3,4-tetrahydrochinolin, dessen Oxim zu 1-(2-Methylmercaptophenyl)-4-amino-1,2,3,4-tetrahydrochinolin reduziert wurde. N-[-(4-Methylpiperazinyl-1)-propyl]-2-methylthiodiphenylamin wurde durch Direktsubstitution van 2-Methylthio-diphenylamin erhalten.

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Methylation of o-aminothiophenol gave o-methyl-mercaptoaniline, the tosylate of which was used for the preparation of N-(o-methylmercaptophenyl)--aminopropionic acid tosylate. Cyclization of -(2-methylmercapto-diphenyl)-aminopropionic acid yielded 1-(2-methylmercaptophenyl)-4-oxo-1,2,3,4-tetrahydroquinoline, the oxime of which was reduced to 1-(2-methylmercaptophenyl)-4-amino-1,2,3,4-tetrahydroquinoline. N-[-(4-Methylpiperazino-1)-propyl]-2-methylmercapto-diphenylamine was prepared by direct su stitution of 2-methylmercapto-diphenylamine.

     

7-Azaindole derivatives

A study is made of new synthetic routes, based on accessible 3-formyl-7-azaindoles, to 3-substituted 7-azaindole. 2-Phenyl-4-(1-phenyl-4-methyl-7-azaindolyl-3-rnethylene)-1, 3-oxazol-5-one is synthesized, and it is converted to 1-phenyl-4-methyl-7-azatryptophane, 1-phenyl-4-methyl-7-azaindolyl-3-acetic acid,1-phenyl-3-(,-dihydroxypropyl)-4-methyl-7-azaindole, and 1-phenyl-4-methyl-7-azaindolyl-3-pyrotartaric acid.For Part XVIII see [1].     

Synthesen von Derivaten des 1-Phenyl-1,2,3,4-tetrahydrochinolins

Zusammenfassung 1-Phenyl-1,2,3,4-tetrahydrochinolinderivate mit Substituenten (Methyl, Äthyl, Chlor, Methoxyl) in Stellung 6 und/oder 4 wurden dargestellt: Cyclisierung der entsprechenden -(Diphenylamin-N)-propionsäuren lieferte die 4-Oxoverbindungen. Die 4-Aminoderivate wurden durch Reduktion der 4-Hydroximinoverbindungen hergestellt.

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1-Phenyl-1,2,3,4-tetrahydroquinoline derivatives with substituents (methyl, ethyl, chloro, methoxyl) in position 6 and/or 4 were synthesized: cyclization of the corresponding diphenylaminopropionic acids yielded the 4-oxo compounds. The 4-amino derivatives were prepared by reduction of the 4-hydroximino compounds.

     

1-Aryl-6-azauracile, 5. Mitt.: Die Synthese von 1-(β-Pyridyl)-6-azauracil-5-carbonsäure und einiger ihrer Derivate

Zusammenfassung Analog wie in vorherigen Mitteilungen^1–4 wurden -Pyridyl-hydrazono-cyanacetylcarbamidsäureäthylester (1), 1-(-Pyridyl)-5-cyan-6-azauracil (2), 1-(-Pyridyl)-6-azauracil-5-carbonsäure (3), deren Thioamid (4), und Amidoxim (5), welches in 1-(-Pyridyl)-5-[5-methyl-1,2,4-oxdiazolyl(3)]-6-azauracil (6) überge-führt wurde, hergestellt.

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-Pyridylhydrazono-cyanacetylcarbamic acid ethyl ester (1), l-(-pyridyl)-5-cyano-6-azauracil (2), 1-(-pyridyl)-6-azauracil-5-carboxylic acid (3), its thioamide (4) and amidoxime (5) were prepared as described in preceding communications. (5) was converted into l-(-pyridyl)-5-[5-methyl-1,2,4-oxdiazolyl(3)]-6-azauracil (6).

     

Complexation of the Non-steroidal Anti-inflammatory Drug Loxoprofen with Modified and Unmodified β-Cyclodextrins

The inclusion complex of the anti-inflammatory drug, loxoprofen, with -cyclodextrin-(CD), sulfated -CD, and glycerol ether -CD was studied by UV-VIS absorption and ¹H-NMR spectroscopy in solution. The inclusion complex of loxoprofen with -CDs was prepared by freeze-drying, and then characterized in the solid state by thermal analysis, X-ray diffraction, FT-IR and FT-Raman spectroscopy, and scanning electron microscopy (SEM). Furthermore, a physical mixture of loxoprofen/-CD (1/1, mol-%) in the solid state was also characterized. The solubility of the loxoprofen increased on addition of -CDs. The solubility enhancement of the loxoprofen with -CDs is in the following order: glycerol ether -CD > sulfated -CD > -CD.     

1-Phenyl-5(6)-methyldihydrouracils and their transformations

The reaction of aniline with methacrylic and crotonic acids gave N-phenyl-- or -methyl--alanines, which were converted to the corresponding 1-phenyl-5(6)-methyl- and 1-phenyl-2-thioxo-5(6)-methyldihydrouracils by the action of urea or thiocyanates in an acidic medium. The dihydrouracils were converted to ureido acids by the action of alkalis and to N-phenyl--alanine hydrazides by the action of hydrazine. 1-Phenyl-2-thioxo-5-methylhexahydropyrimidine was isolated in the reduction of the thioxodihydrouracil. The dihydro- and thioxodihydrouracils react with phosphorus pentasulfide to give 4-thioxo- and 2,4-dithioxodihydrouracils. 1-Phenyl-5(6)-methyldihydrocytosines were obtained from the 4-thioxodihydrouracils. The thioxodihydrouracils were subjected to bromination; 1-(4-bromophenyl)-5(6)-methyldihydrouracils were obtained from 1-phenyl-5(6)-methyldihydrouracils, and 1-phenyl-2-thioxo-5-bromo-5-methyldihydrouracil, which was converted to a uracil by dehydrobromination, was obtained from 1-phenyl-2-thioxo-5-methyldihydrouracil. 1-Phenyl-2-thioxo-5-methyluracil was also obtained by dehydrogenation of 1-phenyl-2-thioxo-5-methyldihydrouracil with sulfur.Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 8, pp. 1097–1101, August, 1981.     

7-Azaindole derivatives

The Bischler-Napiralski reaction is used to synthesize 1-phenyl-3, 9-dimethyl-5, 6-dihydro-12-aza--carboline, and its 5-methyl and 5-ethyl derivatives, from 1-phenyl-4-methyl-3-aminoalkyl-T-azaindoles. 5, 6-Dihydro-12-aza--carbolines prepared by sodium borohydride reduction are converted into 1-phenyl-3, 9-dimethyl-3, 4, 5, 6-tetrahydro-12-aza--carboline and its 5-methyl and 5-ethyl derivatives. 1-Phenyl-9-methyl-12-azaharman is synthesized by palladium dehydrogenation of 1-phenyl-3, 9-dimethyl-5, 6-dihydro-12-aza--carboline.For Part XVII see [1].     

Über spasmolytisch wirksame 1-Phenyl-isochinoline und Bis-(phenyläthyl)-amine mit Guajacyl-gruppierung

Zusammenfassung Die Synthese des 1-Phenyl-6-methoxy-7-oxy-isochinolins, des1-(3-Methoxy-4-oxy-phenyl)-6-methoxy-7-oxy-isochinolins sowie des1-(3,5-Dimethoxy-4-oxy-phenyl)-6-methoxy-7-oxy-isochinolins wird beschrieben. Als weitere Spasmolytika wurden das Bis-(3-methoxy-4-benzyloxy--phenyläthyl)-amin, dessen N-Methylderivat und das Bis-(3-Methoxy-4-oxy--phenyläthyl)-amin dargestellt. Vereinfachte Synthesen der Ausgangsprodukte, Benzylsyringasäure, Syringaaldehyd und Benzylsyringaaldehyd, wurden ausgearbeitet. K. Kratzl undG. Billek, Mh. Chem.83, 1409 (1952).     

Structure of psolusoside B — A nonholostane triterpene glycoside of the holothurian genus Psolus

The structure of psolusoside B — a minor triterpene oligoglycoside from the holothurianPsolus fabricii and the main glycoside fromPsolus sp. has been determined by the methods of partial acid hydrolysis, methylation,¹³C NMR, and FAB mass spectrometry as 20S-acetoxy-3-{2-O-[O--D-glucopyranosyl-(1 4)-O--D-glucopyranosyl]-4-O-(6-O-sulfato--D-glucopyranosyl)--D-xylo-pyranosyloxy}holosta-7,25-diene-18,16-carbolactone. 3-[O-(3-O-Methyl-6-O-sulfato--D-glucopyranosyl)-(1 3)-O-(6-O-sulfato--D-glucopyranosyl)-(1 4)-O--D-quinovopyranosyl-(12)--D-xylopyranosyloxy]holosta-9(11),25-dien-16-one (psolusoside A), known previously forPsolus fabricii, has been identified in a holothurian —Psolus sp. — from Kraternaya Bay (island of Ushishir).Pacific Ocean Institute of Bioorganic Chemistry, Far Eastern Branch, Academy of Sciences of the USSR, Vladivostok. Translated from Khimiya Prirodnykh Soedinenii, No. 3, pp. 361–368, May–June, 1989.     

Thermal decomposition of alkylcyclohexane mixtures

Thermal decomposition of model alkylcyclohexane mixtures with different ratios of components has been investigated. The possibility to estimate the yield of reaction products by calculating the relative activities of a group of hydrocarbons is shown.

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Liquid phase CO+H2 reactions in presence of ruthenium catalysts

Several effects on the hydrogenation of carbon monoxide in propanol in presence of ruthenium catalysts are examined. The homologation reaction is not observed, only propyl formate and propyl acetate are produced with any ruthenium catalyst. The pH-value is an important parameter: in acid media, the yield of propyl formate is noticeably increased indicating different catalytic active species. The addition of cesium salts is also benefitial for formate formation. This is not the case when water is associated with propanol as solvent. Finally, no ethylene glycol is detected. The process is found to be homogeneous and methanol seems to be the precursor of methyl formate.

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, . , . : , . . , . . , -, .

     

NMR Spectral Assignment of Per-substituted Key-Intermediates of β-Cyclodextrin and Implications in the Structures of the Derivatives

The compounds, 6-per-O-(t-butyldimethylsilyl)--cyclodextrin(1), 2,3-per-O-benzyl-6-per-O-(t-butyldimethylsilyl)--cyclodextrin(2), 2,3-per-O-benzyl--cyclodextrin (3),2,3,6-per-O-benzyl--cyclodextrin (4),2,3,6-per-O-benzoyl--cyclodextrin (5), are used as keyintermediates in the synthesis of selectively substituted -CD derivatives. Simple and assignable ¹H and ¹³C NMR spectra (chemical shifts and coupling constants) were obtained for compounds1–4 indicating C₇ symmetry, ⁴C₁ glucose conformation and major arrangement of H6, H6' atoms at the primary side. The derivative 5, however, gave very broad peaksat room temperature. The peaks could partially be assigned at 270 K, but the broadening was still present at 220 K. This implies that there exist several conformers of similar energyand C₁ symmetry that continuously interchange, since there is not a single type of stabilizing interaction thatpredominates. We attributed this phenomenon to the presence of the carbonyl group, which probablydisfavors - stacking and induces random arrangements of the aromatic rings.     

Improvement of Solubility and Dissolution of 19-Norprogesterone via Inclusion Complexation

In an effort to modify the solubility and dissolution rate of the contraceptive steroid, 19-norprogesterone in order to improve its bioavailability, the cyclodextrin complexation approach was chosen. In solution, the complex formation with -cyclodextrin (-CD), hydroxyethyl -cyclodextrin (HE--CD) and hydroxypropyl -cyclodextrin (HP--CD) was confirmed by using solubility, UV, IR and ¹H-NMR spectrophotometric techniques. The phase solubility diagrams were categorized as A_L-type. The complexing affinity of the CDs investigated were ranked as follows: -CD > HP--CD > HE--CD. The complexation thermodynamic parameters were obtained from the temperature dependence of the dissociation constants. In the solid state, differential scanning calorimetery (DSC) and optical microscopy methods were utilized to characterize the complexes. Dissolution studies showed that such molecularly encapsulated forms offered a marked improvement in the dissolution rate compared to the parent drug.     

The triterpene glycosides ofpatrinia intermedia roem et schult

Conclusions It has been established that patrinoside D₁ is the -D-glucopyranosido(13) -D-xylopyranosido(12) -L-rhamnosido(14)--D-xylopyranoside (13) of oleanolic acidKhimiya Prirodnykh Soedinenii, Vol. 5, No. 2, pp. 84–89, 1969     

The Effect of Cyclodextrins on the Photochemical Stability of 7-Amino-4-methylcoumarin in Aqueous Solution

The effect of -, - and -cyclodextrin onthe photochemical stability of 7-amino-4-methylcoumarin (C120)was studied. Using spectroscopic techniques (UV/Vis absorption spectroscopy, fluorescence, fluorescence anisotropy and circular dichroism) combined with HPLC/MS and MS analysis it was demonstrated that addition of -cyclodextrin to the aqueoussolution of C120 markedly inhibits the photodegradation of that dye. This results from theformation of an inclusion complex between C120 and -cyclodextrin.     

Comparative study on inclusion complexations of antiinflammatory drug flurbiprofen with β-cyclodextrin and methylated β-cyclodextrins

Abstruct Some physicochemical properties of methylated -cyclodextrins, i.e., heptakis(2,6-di-O-methyl)--cyclodextrin (DM--CyD) and heptakis(2,3,6-tri-O-methyl)--cyclodextrin (TM--CyD) were compared with those of natural -cyclodextrin (-CyD). Inclusion behaviors of -CyD and methylated -CyDs in water and in solid state were studied by solubility analysis, spectroscopies (UV, CD,¹³C-NMR and IR), X-ray diffractometry and thermal analysis, using an antiinflammatory drug flurbiprofen (FP) as a guest molecule. The spectral data suggest that the inclusion mode of FP-TM--CyD is somewhat different from those of FP--CyD and FP-DM--CyD. The solid complexes of FP with - and methylated -CyDs were obtained in molar ratio of 11, and their dissolution behavior and release from suppository base were examined. The data are presented suggesting that DM--CyD is particularly useful for improving the pharmaceutical properties of FP in various dosage forms.     

Poisoning effect of carbon monoxide on the desorption process of hydrogen from palladium

The desorption of H₂ from clean and CO-poisoned Pd wires was studied by a temperature programmed desorption technique. Poisoning effect of CO on H₂ desorption process can be accounted for in terms of blockage of the surface sites for the recombination of H atoms.

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H₂ , CO, - . CO H₂ , , , .

     

Strukturelle Abwandlungen an partiell silylierten Kohlenhydraten mittels Triphenylphosphan/Azodicarbonsäurediethylester, 4. Mitt.: Transformationen an Mannose und Galaktose

Reaction of methyl -D-galactopyranoside (1) with two equivalents oft-butyldimethylchlorosilane yields methyl 2,6-bis-O-(tBDMSi)--D-galactopyranoside (1 b), methyl 3,6-bis-O-(tBDMSi)--D-galactopyranoside (1 c) and methyl 4,6-bis-O-(tBDMSi)--D-galactopyranoside (1 d). Likewise methyl -D-mannopyranoside (6) affords methyl 2,6-bis-O-(tBDMSi)--D-mannopyranoside (6 d) and methyl 3,6-bis-O-(tBDMSi)--D-mannopyranoside (6 b), which can be isomerised withTPP/DEAD to methyl 4,6-bis-O-(tBDMSi)--D-mannopyranoside (6 f). Methyl 6-O-(tBDMSi)--D-galactopyranoside (1 a) and methyl 6-O-(tBDMSi)--D-mannopyranoside (6 a) can be prepared from1 or6 with one equivalent oft-butyldimethylchlorosilane.Without an external nucleophile the sugar derivatives1 a and1 b react withTPP/DEAD to form the 3,4-carbonato--D-galactopyranosides1 h and1 i and the 3,4-carbonato-2-O-ethoxycarbonyl--D-galactoside (1 j). In contrast to the formation of the compound1 i by means ofTPP/DEAD the reaction of1 a withTPP and Di-t-butyl-azodicarboxylate (DTBAD) yields the 2,3-anhydro--D-taloside (4 b) and only a small amount of1 i. The epoxide4 b can be cleaved withp-nitrobenzoylchloride/pyridine to the 3-chloro-3-deoxy-2,6-di-O-p-nitrobenzoyl--D-idoside (5). Reaction of1 c and1 d withTPP/DEAD yields the 2,3-anhydro--D-gulopyranoside (2), which can be transformed with NaN₃/NH₄Cl to the 2-azido-2-deoxy--D-idopyranoside (3).Likewise6 a and6 d can be converted to the 3,4-anhydro--D-talosides (7 a and7 b). Reaction of7 b or6 d withTPP/DEAD/NH₃ leads to 3,4-anhydro-2-azido-2-deoxy--D-galactopyranoside (8) and 3-azido-3-deoxy--D-altropyranoside (10), resp.The epoxide7 b is opened with NaN₃/NH₄Cl to the 4-azido-4-deoxymannosides (11 a and11 c) and the 3-azido-3-deoxy--D-idopyranoside (12), while the epoxide8 affords the 2,4-di-azido-2,4-dideoxy--D-glucopyranoside (9).Structures were elucidated by¹H-NMR-analysis of the corresponding acetates.

H. H. Brandstetter undE. Zbiral, Helv., im Druck.     

Polymorphism of (+)N-tosyl-L-glutamic acid

It has been shown that polymorphism is the reason for the occurrence of (+)N-tosyl-L-glutamic acid 1 with various melting points. 1 occurs in two crystalline forms: and . Form -1 (prisms) having a melting point of 145–147°C is chemically pure and stable. Form -1, however, is unstable and is formed as a result of the stabilizing effect of an organic solvent not introduced into the structure of the crystal. At about 125°C the forms is transformed to the form. The melting point of the form depends on the amount and type of solvent contained in the crystal, which, during measurement cannot leave the system.     

Reactions of 1,2,4-Triazines with Nucleophiles. 6. Use of SNH Methodology for the Direct Introduction of Cyclic Diketone Residue into the 1,2,4-Triazine Ring FORENAME = D. N.

3-R-6-Phenyl-1,2,4-triazine 4-oxides react with cyclic -diketones (dimethylbarbituric acid, dimedone, and indan) in both acidic (substrate activation) and basic conditions (nucleophile activation) with formation of ^H-adducts, intermediates in the nucleophilic substitution of hydrogen (S_N ^H) in 3-R-5-Nu-4-hydroxy-6-phenyl-4,5-dihydro-1,2,4-triazines. Oxidative aromatisation of these intermediates or auto-aromatisation of acylated (benzoyl chloride) at the NOH -adducts with elimination of benzoic acid gave the corresponding substituted 1,2,4-triazine 4-oxides or 1,2,4-triazines.