C-10 substituted 19-norsteroids—VIII 10-cyanosteroids with an oxygen at C-3

A sythetic sequence leading to 3-keto-10-cyano steroids is described. A number of 10-cyano and 10β-cyano ring A ketols have been prepared, and their rearrangements observed. The effect of the 10-cyano group on the rearrangement and conformation of ring A ketols is discussed.     

Synthesis of 3-cyano-2-methylpyridines substituted with heteroaromatics

A series of title compounds were easily prepared by the sonication of α,β-unsaturated carbonyl compound in acetonitrile in the presence of potassium t-butoxide.     

Synthesis of substituted 2-amino-3-cyano-4-methylpyrroles

A facile route for the synthesis of substituted 2-amino-3-cyano-4-methylpyrroles from N-acetyl-α-amino ketones and malononitrile is reported.     

Synthesis of novel C-2 substituted pyrimidine nucleoside analogs

A series of 2-(2-oxoalkylidene)-4(1H)-pyrimidinone nucleoside analogs were synthesized by the addition of the lithium enolates of methylketones to 2,5′- and 2,2′-anhydrouridines and to 2,5′-anhydrothymidines. Alternatively, 2-thiouridine was alkylated with bromomethyl ketones to yield 2-(2-oxoalkyl)thio-4(1H)-pyrimidinone ribofuranosides in good yields. These intermediates were subsequently transformed into the title compounds via an Eschenmoser sulfur extrusion reaction. The 2-(2-oxoalkylidene)-4-(1H)-pyrimidinone nucleoside analogs exhibit enol proton signals in their ¹H nmr spectra indicative of hydrogen bonding between N-3 and keto oxygen. These structures offer functional groups with potential for Watson-Crick hydrogen bonding.     

Mass spectra of substituted Δ2-1,2,4-oxadiazolines—I

The electron impact fragmentation of four Δ²-1,2,4-oxadiazolines with substituents at positions 3 and 5 has been examined. The direct analysis of daughter ions and high resolution mass measurements provided valuable information regarding certain ions. The present study clearly demonstrates that the substitution of phenyl or a substituted phenyl group for alkyl at C-3 and alkyl in place of a phenyl substituent at C-5 in the oxadiazoline system alters the fragmentation modes considerably.     

Heterocycles from substituted amides. VII Oxazoles from 2-isocyanoacetamides

Certain heretofore unknown tertiary α-isocyanacetanilides 1 are reported for the first time, prepared by methods necessarily different from those employed to prepare the previously cited aliphatic α-isocyano-acetamides 2 . Like 2, 1 has been shown to readily undergo dialkylation with alkyl halides. Moreover, 1 also gives rise to oxazole and oxazoline derivatives upon reaction with acyl halides and aldehydes, respectively, resembling the similarly activated α-isocyano esters and sulfones. Further, in a demonstrable ring-chain tautomeric equilibration, apparently restricted to tertiary amides, 1 readily cyclizes, providing the only known synthesis of 5-amino-2,4-unsubstituted oxazoles 3 . In other examples 4-chloro and 4-alkyl-5-amino-oxazoles are produced. The materials and reactions are characterized, and compared with previous related studies.     

C-2 Arylamino substituted purine ara-carbocyclic nucleosides as potential anti-cytomegalovirus agents

There are reports in the literature that placement of an arylamino side chain at the C-2 position of purine nucleosides produces compounds capable of inhibiting DNA polymerase. To evaluate the potential of this class of compounds as antiviral agents that act by inhibiting viral DNA polymerase, ara-carbocyclic purine nucleosides possessing a 4-(l-butyl)phenylamino and a 3,5-dichlorophenylamino substituent at C-2 were chosen as the prototype structures and have been prepared from 2,4,6-trichloropyrimidine in 6 steps. For the antiviral analysis, human cytomegalovirus served as the principal virus since it expresses a virally specific DNA polymerase. None of the compounds showed activity towards this virus, but they were found to display some toxicity towards one or more cell lines.     

Stereochemische untersuchungen an C-10-disubstituierten C-9-hydroxyphäophorbiden der a-reihe

The diastereomeric 9-hydroxy pheophorbides 3a, b-1, 2 and 4a, b-1, 2 were prepared by reduction of the 10-alkoxy pheophorbides 1a, b and 2a, b with NaBH₄. Their absolute configuration at C-10 was determined by NMR- and ORD/CD-measurements as well as chemical correlation, the configuration at C-9 by IR- and mainly NMR-spectroscopy. For this purpose, the NMR-spectra of the 9-hydroxy pheophorbides 3a, b-1, 2 had completely to be assigned with the aid of the selectively deuterated alcohols 5a, b-1, 2. The configuration at C-10 is stable under the conditions of the alkaline reduction while C-9 partially epimerizes. The acidic alcoholysis of 3a, b-1, 2, however, proceeds by equilibration at C-10 and almost complete retention at C-9. The H-bonds between the 9-OH group and the C-10 substituents (-COOCH₃, -OCH₃ were investigated by NMR and IR spectroscopy.     

Macrolide antibiotics—VII The structure of neomethymycin

Degradation experiments are described which establish rigorously structure (II) for neomethymycin (C₂₅H₄₃NO₇). This antibiotic belongs, therefore, to the macrolide group and differs from methymycin (I) only in the location of one hydroxyl group, which results in marked changes in chemical behavior. The two antibiotics appear to have the same absolute configuration at the relevant asymmetric centers as inferred by the isolation of a common degradation product and the general similarity of certain rotatory dispersion curves. The position of the hydroxyl group at C-12 in neomethymycin is noteworthy from a biogenetic standpoint.     

Chemosensor properties of 7-hydroxycoumarin substituted cyclotriphosphazenes

The newly synthesized cyclotriphosphazene cored coumarin chemosensors 5, 6, and 7 were successfully characterized by ¹ H NMR, ³¹ P NMR, and MALDI-TOF mass spectrometry. Additionally, the photophysical and metal sensing properties of the targeted compounds were determined by fluorescence spectroscopy in the presence of various metals (Li ⁺ , Na ⁺ , K ⁺ , Cs ⁺ , Mg ²⁺ , Ca ²⁺ , Ba ²⁺ , Cr ³⁺ , Mn ²⁺ , Fe ³⁺ , Co ²⁺ , Al ³⁺ , Hg ⁺ , Cu ²⁺ , Zn ²⁺ , Ag ⁺ , and Cd ²⁺ ) . The fluorescence titration results showed that compounds 5, 6, and 7 could be employed as fluorescent chemosensors for Fe ³⁺ ions with high sensitivity. The complex stoichiometry between final cyclotriphosphazene chemosensors and Fe ³⁺ ions was also determined by Job’s plots.     

Lycopodium alkaloids—VII Lycofoline and related bases

Lycofoline and its naturally occurring acetyl derivatives have been correlated to acrifoline. The structures and sterochemistry of these bases is discussed.     

Synthesis and Antitumor Activity of C-2／C-10 Modified Analogues of Docetaxel

Four 10-propionyl docetaxel analogues (lla-d) with 2α-amido substituents were prepared, and their antitumor activity against three solid tumor cell lines and their drug-resistant counterparts were determined.     

Regiospecific, enantiospecific total synthesis of C-19 methyl substituted sarpagine alkaloids dihydroperaksine-17-al and dihydroperaksine

The optically active tetracyclic ketone 8 was converted into the pentacylic core 14 of the C-19 methyl substituted N(a)-H sarpagine and ajmaline alkaloids via a critical haloboration reaction. The ketone 14 was then employed in the total synthesis of 19(S),20(R)-dihydroperaksine-17-al (1) and 19(S),20(R)-dihydroperaksine (2). The key regioselective hydroboration and controlled oxidation-epimerization sequence developed in this approach should provide a general method to functionalize the C(20)-C(21) double bond in the ajmaline-related indole alkaloids.     

Le diptérocarpol—II Stéréochimie en C-13 et en C-17

Various reactions of ring D of dipterocarpol (hydroxy-dammarenone-II) show this triterpene to have the configuration 13β, 17H, in accordance with biogenetic speculations.     

Struktur-Reaktivitätsuntersuchungen mit heterosubstituierten Nitrilen—VII: 13C-, 14N- und 19F-NMR-Spektroskopische Untersuchungen an Verbindungen vom Typ Ar?X?CN

The chemical shifts of aromatic nitriles of the general structure para-Y? C₆H₄? X? CN with X = O, S, Se and N(CH₃) have been investigated by the ¹³C NMR technique. For cyanates (X = O) the ¹⁴N shifts and for Y = F the ¹⁹F shifts were likewise measured. The chemical shifts and the corresponding ¹³C shift increments Δ_n have been found to correlate with the appropriate substituent constants σ_R⁰, σ_p⁰ and σ_I, as well as with the π-electron densities calculated in the PPP approximation.     

Identification of 4,5-asymmetrically substituted 1-(N-isoimido)-1,2,3-triazoles by benzene induced shifts in NMR spectra—VII

Proton chemical shifts, as well as solvent shifts induced by benzene, can be used for the structure determination of 4,5-asymmetrically substituted 1-(N-isoimido)-1,2,3-triazoles, derived from the oxidation of α-diketone bisaroylhydrazones. The geometry of the postulated ‘collision complex’ is discussed and an attempt is made to estimate theoretically the induced shifts of some of the protons.     

Synthesis and anti-HIV-1 activity of novel 10-thiaisoalloxazines,a structural analog of C-5 and/or C-6 substituted pyrimidine acyclonucleoside

A series of novel 10-thiaisoalloxazine derivatives bearing an alkoxymethyl or benzyloxymethyl moiety at the N-1 position has been synthesized through the bromination of 1-substituted-5-hydroxyuracils and subsequent condensation with aminobenzenethiol in a one-pot reaction. Contrary to the previous report, the formation of intermediary 5,6-diethoxy-5-hydroxy-5,6-dihydrouracil seems to be not the necessary factor for the formation of the thiaisoalloxazines, since the reaction proceeds in tetrahydrofuran (THF) or acetonitrile far more smoothly than in ethanol. The anti-human immunodeficiency virus (HIV)-1 activity of the resulted thiaisoalloxazine derivatives was evaluated in lymphocyte cells based on the inhibitory activity against the viral-induced cytopathic activity. Among the derivatives, compounds 6, 7, and 8 bearing an alkoxymethyl moiety at the N-1 position exhibited modest inhibitory activity towards the cytotopathic effect of HIV-1.