Synthese von (+)-Aspicilin mit Bausteinen aus nachwachsenden Rohstoffen

Synthesis of (+)-Aspicilin Using Building Blocks from Renewable Resources The 18-membered lichen macrolide (+)-aspicilin ( 1 ) is easily built up from compounds 14 , 16 , 3 , and 24 following the C₃ + C₇ + C₆ + C₂ = C₁₈ pattern (see Schemes). The synthesis requires 15 steps and gives 1 in 13% overall yield from D -mannose ( 2 ). The latter compound provides the stereogenic centers C(4), C(5), and C(6). The stereogenic center C(17) is supplied by building block 14 (from (?)-(S)-ethyl lactate).     

N‐[(R)‐1‐(2‐Hydr­oxy‐5‐methyl­phen­yl)­eth­yl]‐N‐[(R)‐1‐(2‐meth­oxy‐5‐methyl­phen­yl)‐2‐phenyl­eth­yl]aminium chloride

The title compound, C₂₅H₃₀NO₂⁺·Cl⁻, has been synthesized, and the crystal structure shows that it is mainly stabilized through inter­molecular N—H·Cl and O—H·Cl and intra­molecular N—H·O hydrogen bonds. The absolute configuration of the new stereogenic center (the C atom adjacent to the N atom on the phenol side) was determined to have an R configuration.     

(R)‐N‐[(R)‐1‐(2‐Hydroxy‐5‐methyl­phenyl)‐2‐phenyl­ethyl]‐2‐methyl‐1‐phenyl­propyl­ammonium chloride

In the title compound, C₂₅H₃₀NO⁺·Cl⁻, the mol­ecules are linked by a combination of inter­molecular N—H⋯Cl and O—H⋯Cl hydrogen bonds and intra­molecular N—H⋯O hydrogen bonds. The absolute configuration of the new stereogenic centre (the C atom adjacent to the N atom on the phenol side) is determined to have an R configuration.     

Analogs of Cinchona Alkaloids Incorporating a 9,9′-Spirobifluorene Moiety

The Cinchona alkaloid analogs (+)- and (?)- 5 with a quinuclidine-2-methanol residue attached to C(2) of a 9,9′-spirobifluorene moiety were prepared as a racemic mixture by reacting lithiated 2-bromo-9,9′-spirobifluorene 7 with (2-ethoxycarbonyl)quinuclidine (±)- 6 to give ketone (±)- 8 , followed by diastereoselective reduction with diisobutylaluminum hydride (DIBAL-H). The absolute configuration at C(9) and C(8), i.e., at the methanol bridge and the adjacent quinuclidine C-atom, in the two enantiomers of 5 is identical to the configuration at the corresponding centers in (?)-quinine ( 1 ) and (+)-quinidine ( 2 ), respectively. For the optical resolution of (±)- 5 , a chiral stationary phase for HPLC was prepared by covalently bonding quinine via a thiol spacer to a silica-gel surface. The enantiomer separation was accomplished at an α value of 1.61 with (±)- 5 being eluted last, in agreement with ¹H-NMR studies in CDCl₃ which showed that (+)- 5 underwent a more stable host-guest association with quinine than (?)- 5 . ¹H{¹H} Nuclear Overhauser effect (NOE) difference spectroscopical analysis of the host-guest associations with quinine in CDCl₃, combined with computer-model examinations, allowed the assignment of the absolute configurations as (+)-(8R,9S)- 5 and (?)-(8S,9R)- 5 . A detailed conformational analysis displayed excellent agreement between the results of computational methods (Monte Carlo multiple minimum simulations, analyses of the total energy as a function of the flexible dihedral angles in the molecule) and ¹H{¹H}-NOE difference spectroscopical data. It was found that (?)- 5 and (+)- 5 differ significantly in their conformational preference from their natural counterparts quinine ( 1 ) and quinidine ( 2 ). Whereas the natural alkaloids prefer the ‘open’ conformation, with the quinuclidine N-atom pointing away from the quinoline ring, analog (±)- 5 adopts preferentially (by ca. 4 kcal mol^?1) a ‘closed’ conformation, in which the quinuclidine N-atom points into the cleft of the 9,9′-spirobifluorene moiety. Since the basic quinuclidine N-atom in the ‘closed’ conformation is sterically shielded from forming strong H-bonds, the new Cinchona alkaloid analogs form less stable host-guest associations via H-bonding than quinine or quinidine.     

Dendryphiellin A,the First Fungal Trinor-eremophilane. Isolation from the marine deuteromycete Dendryphiella salina (SUTHERLAND) PUGHet NICOT

The novel metabolite dendryphiellin A ( = (+)-(1R,2S,8aR)- 1,2,6,7,8,8a-hexahydro-7-hydroxy-1,8a-dimethyl-6-oxonaphthalen-2-yl (6R*, 2E,4E)-8-hydroxy-6-methylocta-2,4-dienoate; (+)- 1 ) is isolated from cultures of the marine deuteromycete Dendryphiella salina. There is no precedent in fungi for trinor-eremophilanes or for branched C₉ carboxylic acids, the two classes of compounds constituting (+)-1. The structure is secured by NMR spectroscopy and hydrolysis of (+)-1 to give the side-chain moiety ((6R*,2E,4E)-8-hydroxy-6-methylocta-2,4-dienoic acid ( 2 )) intact, whilst the trinor-ermophilane moiety is decomposed. The absolute configuration at the trinor-eremophilane moiety is established from exciton coupling between the dienone and the diene-ester functions.     

Total Synthesis of (+)‐Gracilamine Based on an Oxidative Phenolic Coupling Reaction and Determination of Its Absolute Configuration

The enantioselective total synthesis of (+)‐gracilamine ( 1 ) is described. The strategy features a diastereoselective phenolic coupling reaction followed by a regioselective intramolecular aza‐Michael reaction to construct the ABCE ring system. The configuration at C3a in 1 was controlled by the stereocenter at C9a, which was selectively generated (91 % ee) by an organocatalytic enantioselective aza‐Friedel–Crafts reaction developed by our research group. This synthesis revealed that the absolute configuration of (+)‐gracilamine is 3aR, 4S, 5S, 6R, 7aS, 8R, 9aS.     

Synthese von (+)-(5S, 6S)-Azafrin-methylester; absolute Konfiguration von Aeginetinsäure and von weiteren vicinalen Apocarotin-diolen

Synthesis of (+)-(5S, 6S)-Azafrin Methyl Ester; Absolute Configuration of Aeginetic Acid and of Further Vicinal Apocarotenediols We describe the synthesis of a series of optically active vicinal apo-β-carotenediols. Thus, starting from (+)-(5S, 6S)-5,6-dihydroxy-5,6-dihydro-β-ionone ( 2 ) we have prepared the (Z/E)-isomeric (+)-C₁₅-esters 7 and 8 , the (+)-retinoic derivatives 14 , 15 , 18 , 19 and (+)-methyl azafrinate ( 22 ), the enantiomer of the naturally occur-ring compound (s. Scheme 1). Our synthesis also establishes the absolute configura-tion of aeginetic acid ( 24 ), aeginetoside ( 25 ) and aeginetin ( 26 ), compounds isolated from the root parasite Aeginetia indica by Indian and Japanese workers (s. Scheme 2). The presented synthesis of optically active methyl azafrinate confirms our previous assignment [14] of the absolute configuration of azafrin ( 1a ), which was based on degradative evidence.     

Application of the gold(I)-Catalyzed aldol reaction to a stereoselective synthesis of (2S, 3R, 4R, 6E)-3-Hydroxy-4-methyl-2-(methylamino)oct-6-enoic Acid ( = MeBmt), Cyclosporin's unusual amino acid

The title compound 8 was prepared in three steps starting from the optically pure aldehyde (2R, 4E)-2-methyl-hex-4-enal ( 3 ), thus constituting the shortest synthetic approach reported. Two of the three stereogenic centers in the product were generated in a coupling reaction of 3 with ethyl isocyanoacetate, catalyzed by a gold(I)/chiral ferrocenylphosphine system, giving the dihydrooxazole 5 in 85% diastereoselectivity (mismatchedcase). The weak effect of double stereodifferentiation in this reaction (matched case 90% ds) is discussed. N-Methylation and hydrolytic ring opening of 5 gave the protected form 7 of MeBmt, The X-ray diffraction study carried out on 7 confirms the absolute configuration of the two stereogenic centers formed in the gold(I)-catalytic reaction.     

High Syn Selectivity of a SE′ Reaction: Acylation of an Optically Active 1,1-Disilyl-2-alkene. Preliminary communication

The disilane/disilylmethane rearrangement of an optically active disilanyl sulfide 9B was used to prepare an optically active disilylalkene 10 whose absolute configuration was established by X-ray analysis of the bromo derivative 13 (P2₁, a = 7.847 (3) Å, b = 9.487 (3) Å, c = 20.010 (8) Å, β = 82.28° (3), Z = 2). Acylation of 10 furnished an optically active ketone 14 , which was degraded to 16 , a compound of known absolute configuration. The enantiomeric excess of 10 was determined by alkylation with an optically active lithium compound and that of 14 by an optically active NMR.-shift reagent. The S_E′ reaction 10 → 14 was thus shown to proceed with 94% (97% syn/3% anti) stereoselectivity.     

(+)-(1S, 3S, 6S, 8S)-und (−)-(1R, 3R, 6R, 8R)-4, 9-Twistadien: Synthese und Bestimmung der absoluten Konfiguration

(+)-(1S, 3S, 6S, 8S)-and (?)-(1R, 3R, 6R, 8R)-4, 9-Twistadiene: Synthesis and Absolute Configuration A synthesis and the determination of the absolute configuration of (+)-(1S, 3S, 6S, 8S)- and (?)-(1R, 3R, 6R, 8R)-4, 9-twistadiene ((+)- and (?)- 4 , respectively) is described. Their chiroptical properties are compared with those of saturated twistane ((+)- and (?)- 5 ) as well as with those of the unsaturated and saturated 2, 7-dioxatwistane analogs (+)- and (?)- 9 , and (+)- and (?)- 10 , respectively, which also are compounds of known absolute configurations.     

(R)-(+)-[VCD(+)945]-4-Ethyl-4-methyloctane, the simplest chiral saturated hydrocarbon with a quaternary stereogenic center

Enantiopure (R)-(+)-[VCD(+)945]-4-ethyl-4-methyloctane, the simplest chiral saturated hydrocarbon with a quaternary stereogenic center, was synthesized by the use of MαNP acid method, and its absolute configuration was first unambiguously determined by the ¹H NMR anisotropy, X-ray crystallography, and VCD methods.     

Synthesis and absolute configuration of natural 8-hydroxyl-9-angeloyloxythymol

8-Hydroxyl-9-angeloyloxythymol, isolated from Eupatorium fortuneri Turcz, was synthesized for the first time. The synthesis was achieved through a seven-step route, using m-cresol as the starting material and Sharpless asymmetric dihydroxylation to install the quaternary stereogenic center. The enantio-enriched synthetic sample showed spectroscopic data consistent with those of the natural product and thus confirmed the gross structure assigned previously. By comparing the sign for optical rotations of the synthetic and the natural samples, the absolute configuration for the natural product was also assigned.     

Crystal and molecular structure and the absolute configuration of N-phenyl-N′-(1-phenylethyl)methanephosphonodiamidate

The structural investigation of the product of the reaction of methanephosphonodichloridate with R(+)-1-phenylethylamine and aniline in the presence of triethylamine [3] was performed. The obtained compound C₁₅H₁₉N₂OP ( 1 ) crystallizes in monoclinic system, space group P2₁ with a = 10.466(1) Å, b = 6.984(3) Å, c = 10.471(2) Å, β = 95.43(1)°, V = 762.0(9) ų. Z = 2, and R = 0.037. The absolute configuration at the P and C8 atoms was determined by means of X-ray crystallography as R_p and R_c8, respectively.     

Weitere Beiträge zur Synthese von (+)-Aspicilin

Further Contributions to the Synthesis of (+)-Aspicilin There are two reasons to try to find out. whether the initial and final parts of the ‘photochemical synthesis’ of the 18-membered lichen macrolide (+)-aspicilin ( 5a ) can be improved (cf. Schemes 1 and 2). This synthesis acts as an indicator for the utility of the earlier introduced photolactonization and as a source of large-ring-sized lactones, objects for computer-assisted conformational analysis.     

The absolute chirality of (+)-12-Bromo-[2.2]metacyclophane-4-carbonitrile

The absolute configuration of (+)-12-bromo-[2.2]metacyclophane-4-carbonitril [(+)-4 e] was determined by theBijvoet X-ray diffraction method as(R) _p (Fig. 1). This result allows the unambigous assignment of the absolute chiralities of all optically active 4-monosubstituted, 4,14-homodisubstituted, 4,12- and 4,14-heterodisubstituted [2.2]metacyclophanes chemically correlated with (+)-4 e. The result is compared with those obtained by other methods for establishing the absolute configuration.Stereochemistry of Planar Chiral Compounds, Part 8. Part 7:Krieger, Ch., Lehner, H., Schlögl, K., Mh. Chem.107, 195 (1976).     

First total synthesis of (−)-aplyolide A

The first total synthesis of (−)-aplyolide A², (16S)-methyloxacyclohexadeca-(5Z,8Z,11Z,14Z)-tetraen-2-one, 1 is reported. The synthesis is based on three consecutive couplings of terminal alkynes with propargylic halides and proves the absolute configuration of the stereogenic center of the natural product.     

Chiral Alkoxy Side Chains from (-)-Amino Acids in Mediating Asymmetric Synthesis of Tricarbonyl(cyclohexadienyl)iron Complexes

The asymmetric induction in the complexation reaction of (S)-1-methyl-2-(5-methyl-cyclohexa-1,4-dienylmethyloxy)-pyrrolidine 5 and (S)-2-(2-N,N-dimethylamino-1-propanoxy)-5-methylcyclohexa-1,4-diene 6 having heteroatom adjacent the stereogenic center has been investigated. The diastereoselectivity was determined directly from the diastereotopic peaks in the ¹H NMR or by chemical correlation with 9 . The conversion of η-1,4-complexes 7a and 8a to 9 proceeded with high retention of configuration while that of the η-2,5-Fe(CO)₃ complexes 7b and 8b undergoes considerable racemization.     

235. Information on the sesquiterpenoid C 12 -Ketones from the essential oil of Vetiveria zizanioides (L.) Nash

Two new C₁₂-ketones, (+)-(1S, 10R)-1,10-dimethylbicyclo[4.4.0]dec-6-en-3-one ( 5 ) and (+)-(6S, 10S)-6,10-dimethylbicyclo[4.4.0]dec-1-en-3-one ( 6 ), have been isolated from Reunion vetiver oil (Vetiveria zizanioides (L.) Nash). Structure and absolute configuration of 5 were established by a four-step synthesis from (+)-isonootkatone ((+)-α-vetivone) ( 1 ). The structure of 6 followed from its spectroscopic properties and was confirmed by direct comparison with an authentic racemic sample. The absolute configuration of 6 was established by chemical correlation with (+)-α-eudesmol ( 13 ).     

Stoffwechselprodukte von Mikroorganismen. 237. Mitteilung. (2S, 3R, 4R, 6R)-2,3,4-Trihydroxy-6-methylcyclohexanon aus zwei Actinomyceten-Stämmen

(2S, 3R, 4R, 6R)-2,3,4-Trihydroxy-6-methylcyclohexanone from Two Strains of Actinomycetes A tetrazolium-blue positive compound was isolated from two strains of acinomycetes. Its constitution and relative configuration 1 were determined by spectroscopic methods, and the absolute configuration by degradation to (+)-(R)-methylsuccinic acid.     

Chemical constituents from the bark of bauhinia purpurea and their NO inhibitory activities

Abstract

Phytochemical studies led to the isolation of a new phenylpropanoid glucoside, named purpuroside (1), along with eight known compounds (2–9) from the bark of Bauhinia purpurea. The structure of the new compound was elucidated on the basis of its spectroscopic data. The absolute configuration of compound 2 was verified by X-ray diffraction analysis. Compounds 1, 2, 7, 8, and 9 inhibited NO production in mouse peritoneal macrophages with IC₅₀ values from 35.5 to 63.0?μM.