Preparation of 9-aryl (or heteroaryl)methylidene-10-(methoxyimino)-phenanthrenes and their thermal electrocyclisation to fused quinolines

o-Quinone methanide N-methoxyimines 6a-c, 7a-c, 11a-b and 12a , easily prepared from the reaction of 10-(methoxyimino)phenanthrene-9-one ( 3 ) with phosphonium salts 5a-c, 10a-b in the presence of lithium hydroxide, are thermally converted into dibenzo[f,h]quinolino[2,3-x]fused compounds 9a-c and 13a-b , in high yield.     

New antifungal 1,2,4-triazoles with difluoro(heteroaryl)methyl moiety

New 1,2,4-triazoles (1) having a difluoro(heteroaryl)methyl moiety were designed and synthesized via 1-aryl-2,2-difluoro-2-(heteroaryl)ethanones (2), which were prepared by two routes starting from the reaction of ethyl 2,2-difluoro(heteroaryl)acetate with phenyllithiums (Route A) and from the reaction of chlorodifluoro(heteroaryl)methane with benzaldehydes (Route B). The compounds 1 except for 1g show antifungal activities against yeasts and filamentous fungi in vitro, especially (+)-1f have equal or superior activities compared to those of itraconazole.     

Synthesis of Dialkyl 1,4-Dihydro-2,6-dimethyl-4-(heteroaryl)-pyridine-3,5-dicarboxylates as Calcium Channel Antagonists

The Hantzsch condensation of the heteroarylcarboxaldehydes 3a-c with alkyl acetoacetates 4a-c and alkyl 3-aminocrotonates 5a-b afforded the respective dialkyl 1,4-dihydro-2,6-dimethyl-4-(heteroaryl)-pyridine-3,5-dicarboxylates 6a-f possessing a C-4 4-quinolinyl, 8-quinolinyl or 1-oxido-4-pyridinyl substituent Calcium channel antagonist structure-activity relationships acquired indicate that i) the position of the quinolyl nitrogen atom was not a determinant of activity, ii) increasing the size of the C-3 and C-S alkyl ester substituents decreases potency and iii) a C-4 1-oxido-4-pyridinyl substituent abolishes activity. The most active, and equipotent C-4 4-quinolinyl 6a and 8-quinolinyl 6b analogs, were approximately 8-fold less potent calcium channel antagonists than the reference drug nifedipine.     

Photooxygenation of pyrazin-2(1h)-ones

1-Alkyl-5,6-diphenylpyra2in-2(1H)-ones (1a-b) reacted with singlet oxygen in dichloromethane to afford the stable endoperoxide (1a-b), while in methanol to afford the 1:1-adduct (3a-b) of the endoperoxide (2a-b) and methanol.     

Novel synthesis and application of mixed acetals (acetyl methyl acetals)

A novel synthetic method for mixed acetals (acetyl methyl acetals) by electrolysis of hemithioacetals derived from methoxy- (phenylthio)methane is newly developed. Synthetic application of these mixed acetals as an aldehyde equivalent is also demonstrated.     

Synthesis of 1-beta-O-acyl glucuronides of diclofenac, mefenamic acid and (S)-naproxen by the chemo-selective enzymatic removal of protecting groups from the corresponding methyl acetyl derivatives

Using a straightforward chemo-enzymatic procedure, 1-beta-O-acyl glucuronides of three non-steroidal anti-inflammatory drugs, diclofenac (DF) 5, mefenamic acid (MF) 6 and (S)-naproxen (NP) 7, were prepared. Caesium salts of these carboxylic acid drugs reacted with commercially available methyl 2,3,4-tri-O-acetyl-1-bromo-1-deoxy-alpha-D-glucopyranuronate 4 to give exclusively the corresponding 1-beta-O-acyl glucuronides 8-10 in moderate yields. The protecting acetyl (for -OH group) and methyl ester (for -CO2H group) groups of each sugar moiety were easily removed to provide the corresponding free 1-beta-O-acyl glucuronides 1-3 in high yields. Deprotection was achieved through effective enzyme-catalysed chemo-selective hydrolyses of the acetyl groups using lipase AS Amano (LAS), and of the methyl ester group using esterase from porcine liver (PLE).     

Gd-complexes of macrocyclic DTPA conjugates of 1,1'-bis(amino)ferrocenes as high relaxivity MRI blood-pool contrast agents (BPCAs)

We report the synthesis of macrocyclic DTPA conjugates of 1,1'-bis(amino)ferrocenes (1a-b) and their Gd-complexes [Gd(L)(H(2)O)] (2a-b, L = 1a-b) for use as new MRI blood-pool contrast agents. High R(1) relaxivity in HSA as well as high thermodynamic and kinetic stabilities is observed for 2a.     

The thermal degradation of poly(methyl vinyl ketone) and poly(methyl isopropenyl ketone)

The degradations have been studied by thermal volatilization analysis and thermogravimetry, with infrared and ultraviolet spectroscopic investigations of products. Under temperatureprogrammed heating conditions, PMVK first splits out water from adjacent side groups by a random process, giving a fused ring system as the first formed product. As the temperature is raised, chain scission occurs, leading eventually to a total weight loss as great as 90 per cent. This scission process appears to involve fission of bonds between adjacent ring structures, rather than breakdown of the rings themselves; it is accompanied by the production of small amounts of methane and carbon monoxide. The residue remaining above 500° is stable to temperatures greater than 800°, and is presumably a form of carbon.     

Antidiabetische wirkstoffe. III. 4,5,6-Trisubstituierte 2-(4-toluidino)pyrimidine

The condensation of 4-tolyiguanidine ( 1 ) with the β-kiketones 2a-b yields the 2-(4-toluidino)pyrimidines 3a-b .     

The photolysis of 3,3-dimethylbutan-2-one (methyl t-butyl ketone) and the decomposition of the acetyl radical

The photolysis of 3,3-dimethylbutan-2-one (MTBK) has been studied in the gas phase at 408 and 326 K, mainly with light of 313 nm wavelength. At the higher temperature, the major products were methane, ethane, isobutane, isobutene, neopentane, tetramethylbutane, and carbon monoxide. At 326 K, in addition to these products, appreciable quantities of acetaldehyde, acetone, and biacetyl were detected. Quantum yields were determined using acetone and pentan-3-one as actinometers. A conventional mechanism is able to explain most of the experimental data. At 326 K, the results may be interpreted to yield a value for the rate constant for decomposition of the acetyl radical. Some theoretical calculations are reported on the acetyl radical decomposition and some earlier experimental work on this radical reevaluated.     

Enantioselective synthesis of (2-pyridyl)alanines via catalytic hydrogenation and application to the synthesis of L-azatyrosine

[reaction: see text] A novel method for the synthesis of (2-pyridyl)alanines 2a-b was developed by converting (2-pyridyl)dehydroamino acid derivatives 1a-b to the corresponding N-oxides 3a-b followed by asymmetric hydrogenation using (R,R)-[Rh(Et-DUPHOS)(COD)]BF(4) [(R,R)-6] catalyst and subsequent N-oxide reduction in 80-83% ee. This methodology was applied to the total synthesis of L-azatyrosine [(+)-12], an antitumor antibiotic, starting from (5-benzyloxy)-2-pyridylmethanol (7), in >96% enantiomeric purity.     

Photochemical reactions of 1-methyl-4,6-diaryl-2(1H)-pyrimidinones in the presence of thiols

Photochemical reactions of 1-methyl-4,6-diaryl-2(1H)pyrimidinones 1a-b in the presence of thiols 2 are described. Irradiation of 1-methyl-4,6-diaryl-2(1H)-pyrimidinones 1a-b in benzene in the presence of thiols 2 gave the unexpected 2:1-adducts, 3-methyl-4,6-diaryl-5-aralkylthio-6-(1′-methyl-4′,6′-diaryldihydro-pyrimidin-2-on)yl-1,3-diazabicyclo[2.2.0]hexan-2-ones 3-6, of 1 and 2, whereas irradiation of 1a-b alone in benzene resulted in recovery of the unchanged 1a-b.     

Organotellurium(IV) complexes: synthesis and molecular structure of 2,6-diacetylpyridine (C,N,O) tellurium(IV) trichloride

The reaction of TeCl₄ with 2,6-diacetylpyridine in methylene chloride or tetrahydrofuran gives a new type of organotellurium (IV) compound. An X-ray structure determination showed that the organic radical bonds to the tellurium as a tridentate ligand via a methylene carbon of one of the acetyl groups, the pyridine nitrogen, and the carbonyl oxygen of the second acetyl group. Analogous organotellurium trichloride complexes involving C,O coordination have been formulated for the condensation products of TeCl₄ with 2-acetylcyclohexanone and 3-acetyl-7-methoxycoumarin, while C,N coordination occurs in the condensation product of TeCl₄ and 2-acetylpyridine.     

A new route to the improved synthesis of 1-(alkoxymethyl)-5-alkyl-6-(arylselenenyl)uracils

A new route to C-6-selenenyl analogs of compound 1a from 5-alkyl-6-chlorouracils 6a-b has been described. A mild and highly efficient synthesis of 1-(alkoxymethyl)-5-alkyl-6-(arylselenenyl)uracils 8a-e has been accomplished from 6a-b in good yields using a two step procedure. Silylation of 5-alkyl-6-chlorouracils 6a-b using N,O-bis(trimethylsilyl)acetamide followed by regioselective alkylation of the silylated intermediate with ethyl or benzyl chloromethyl ether in dichloromethane afforded the desired 1-(alkoxymethyl)-5-alkyl-6-chlorouracils 7a-d in 88–94% yields. Compounds 7a-d readily underwent addition-elimination reaction with an appropriate arylselenol in the presence of ethanolic sodium hyroxide to produce the corresponding 1-(alkoxymethyl)-5-alkyl-6-(arylselenenyl)uracils 8a-e in excellent yields (94–99%).     

氰乙基醋酸纤维素乙酰基含量分析

研究了Eberstadt皂化滴定法分析氰乙基醋酸纤维素中乙酰基含量的适用性。控制合适的测试条件,可以使测试结果的精度达到±0.23％,基本上达到分析醋酸纤维素的精度。红外分析、残重分析和混合物分析表明在测定过程中,氰乙基也参加了反应,但氰乙基的反应对乙酰基含量的测定结果没有影响。     

The synthesis of N-[2-(D-glucos-3-O-yl)propionyl]-l-alanine and N-[(d-glucos-3-O-yl)acetyl]-l-alanine

N-[2-(D-Glucos-3-O-yl)propionyl]-L-alanine ( 7a ) was synthesized, which has a glucose residue instead of N-acetylglucosamine residue in the muramyl peptide. N-[(D-Glucos-3-O-yl)acetyl]-L-alanine ( 7b ) was also synthesized as a glycolyl analog of 7a in order to determine the relationship between the structure of propionyl moiety in the carbohydrate analog ( 7a ) and the adjuvant activity. These simple analogs are compounds prepared for the purpose of introduction into a synthetic polymer with the view of producing polymeric drugs.     

A total synthesis of the methyl glycoside of ganglioside GM(1)

The total synthesis of the methyl glycoside of GM(1) (1b) has been accomplished. The key step in the synthesis involves the sulfonamidoglycosidation reaction, which is used to create a beta-linkage leading to a GalNAc residue joined to the C4 hydroxyl group of a galactose unit of a C3 sialylated lactosyl moiety. The "proximal hydroxyl" directing effect, which has been postulated before, manifests in this context as well leading to the preponderant formation of the beta-glycoside. Together with asialo GM(1) and other substructures, the GM(1) methyl glycoside has been submitted for biological assays as potential ligands for bacterial and viral infection sites.     

Copper(II) binding by fragments of alpha-synuclein containing M1-D2- and -H50-residues; a combined potentiometric and spectroscopic study

Stability constants and ligand donor sets of the copper(II) complexes of the NH2-29-56(L1)(AA30GKTKEGVLYV40GSKTKEGVVH50GVATVA56-NH2), NH2-M29-D30-56(L2) and Ac-M29-D30-56(L3) fragments of alpha-synuclein were determined in aqueous solution for 1 : 1 metal-to-ligand molar ratio in the pH range 2.5-10.5. The tyrosine residue in the 39th position of the alpha-synuclein fragments does not take part in the coordination of the metal ion. The potentiometric and spectroscopic data (UV-Vis, CD, EPR) show that acetylation of the amino terminal group induces significant changes in the coordination properties of the L3 fragment compared to that of the L2 peptide. When the amino group is blocked (L3) the imidazole nitrogen of the histidine residue acts as an anchoring site and at higher pH the 3N {N(Im),2N-} and 4N {N(Im),3N-} complexes are formed. The L1 peptide at physiological pH forms in equilibrium 3N {NH2,N-,CO,N(Im)} and 4N {NH2,2N-,N(Im)} complexes. For the L2 peptide the coordination of the copper(II) ions starts from the N-terminal Met residue and with increasing of pH the Asp residue in second position of amino acid sequence coordinates and stabilizes significantly the 2N complex as a result of chelation through the beta-carboxylate group. At physiological pH the 3N {NH2,N-,beta-COO-,N(Im)} coordination mode dominates. At pH above 6 the results for the L2 fragment suggest the formation of 3N and 4N complexes (in equatorial plane) and the involvement of the lateral NH2 group of Lys residue in the axial coordination of Cu(II) ion. In CD spectra sigma (epsilon-NH2-Lys) --> Cu(II) charge transfer transition is observed. The stability constants for the L2 fragment of alpha-synuclein of the 4N {NH2,2N-,N(Im)} and {NH2,3N-} complexes are higher about 1.5 and 0.7 orders of magnitude, respectively, by comparison to those of the L1 peptide. This increase may be explained by the involvement of the epsilon-NH2 group of Lys residue in the coordination sphere of metal ion.     

Rodlike molecules and singlet energy transfer(1)(,)(2)

In continuing our investigations on rodlike molecules composed of bicyclo[2.2.2]octane units, we studied the effect of interposing a single aromatic ring in the rod. Thus, two [3]-rods were synthesized with the two outer units being bicyclooctyls, the central unit being benzenoid, and with one terminal unit bearing an alpha-naphthyl moiety and the other terminus bearing an acetyl or benzoyl group. Excitation of the alpha-naphthyl group led to fluorescence emission by both the naphthyl and the acetyl units. However, compared to the [1]- and [2]-rods previously studied, transmission of singlet excitation proved to be less efficient as determined by the fluorescence emission and also by the singlet lifetimes obtained from single photon counting measurement. Transmission to the benzoyl group proved more rapid than to the acetyl moiety. In assessing the factors controlling energy transmission, Delta-density determinations were employed to describe the distribution of electronic excitation in such systems. It was observed that despite most of the energy being located in the terminal chromophores, some is distributed in the bicyclooctyl units. The extent of this distribution provides a guide to the facility of through-bond energy transfer. Evidence is presented that energy transfer in the short rods is mainly through-bond while in the longer rods Forster through-space transfer is involved.     

Ion dissociation and conduction of Nafion/modified oligo(oxyethylene) composite films

In order to improve the ionic conductivity of solid polymer electrolyte by controlling ion(alkali metal ion)–dipole(ether oxygen) interaction, two kinds of modification were adopted on oligo(oxyethylene) (OOE). One is the capping of terminal hydroxyl groups of OOE with methyl or acetyl groups. The other is the replacement of the center ethylene group of OOE with methylene or propylene group. Ion–dipole interaction was analyzed by measuring the ion dissociation, ion conduction and T_g of Nafion/modified OOE composite films. The modification of the end groups was more effective than that of the center group in increasing ionic conductivity. The methyl group is superior to the acetyl group as the end group of OOE for lithium ion conduction.