Synthesis ofS-(+)-hydroprene

A novel path toS-(+)-hydroprene (1) starting from the technical gradeS-(+)-dihydromyrcene (2, e.e. 50%) is proposed. The latter was selectively transformed intoS-3,7-dimethyloctanal (5) in three steps including hydroalumination. The reactions of5 with allyl- or methallylmagnesium chloride followed, respectively, either by oxygenation in the presence of PdCl₂/CuCl or by ozonolysis, affordS,E-6,10-dimethyl-3-undecen-2-one (7) which was treated with ethoxyethynylmagnesium bromide to give the title juvenile hormone analogue in 23% overall yield.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No 1, pp. 110–112, January, 1993.     

Synthesis ofS-(+)-methoprene

An optically active juvenile hormone analogue,S-(+)-methoprene (1), is synthesized in six steps from technical gradeS-(+)-3,7-dimethyl-1,6-octadiene ((+)-dihydromyrcene, e.e. –50%) by a novel procedure which begins with selective hydroalumination-oxidation to giveS-(-)-citronellol. This alcohol is oxidized to giveS-(-)-citronellal which on reaction with allylmagnesium chloride affords 6S, 10-dimethyl-1,9-undecadien-4 R/S-ol (5). Smidt-Moiseev oxygenation of 5 followed by dehydration leads to 6S, 10-dimethyl-3E,9-undecadien-2-one. The latter on treatment with isopropoxyethynylmagnesium bromide is transformed into isopropyl 3,7S,11-trimethyl-2E/Z,4,E,10-dodecatrienoate which upon Brown solvomercurationreduction in MeOH gives1 in 14% overall yield.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 1, pp. 108–109, January, 1993.     

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.     

Synthesis of some 5′-O-amino acid derivatives of uridine as potential inhibitors ofUDP-glucuronosyltransferase

Summary In an attempt to develop potential inhibitors ofUDP-glucuronosyltransferase, some 5-O-amino acid derivatives of uridine were synthesized. N-protectedL-amino acids were coupled at the 5-O-position of 2,3-O-isopropylideneuridine by esterification employing the method of symmetrical anhydrides in presence of 4-dimethylaminopyridine, 5-O-(N-benzyloxycarbonyl-O-tert.butyl-L-threonl)-23-O-isopropylideneuridine (1), 5-O-(N-tert.butyloxycarbonyl-O-benzyl-L-seryl)-2,3-O-isopropylideneuridine and (2), 5-O-(N-tert.butyloxycarbonyl-L-valyl)-2,3-O-isopropylideneuridine (3), and 5-O-(N-tert.butyloxycarbonyl-L-valyl)-2,3-O-isopropylideneuridine (4) were obtained in good yield after column chromatography on silica gel. The treatment of2 withTFA/CH₂Cl₂ (6:1) at room temperature for 30 min led to a selective removal of theBoc group without deblocking of the 2,3-O-isopropylidene group of uridine. Treatment of2 withTFA/H₂O (5:1) at room temperature for 1 h, however, released bothBoc and 2,3-isopropylidene groups. TheZ group of1 was deprotected by catalytic hydrogenolysis over 10% Pd/C/ammonium formate.

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Synthese von 5-O-Aminosäurederivaten des Uridins als potentielle Inhibitoren derUDP-Glukuronosyl-Transferase

Zusammenfassung In einem Versuch, potentielle Inhibitoren derUDP-Glukuronosyl-Transferase zu entwickeln, wurden einige 5-O-Aminosäurederivate des Uridins synthetisiert. N-GeschützteL-Aminosäuren wurden durch Veresterung mit der 5-O-Position des 2,3-isopropylidenuridins gekuppelt (Methode der symmetrischen Anhydride in der Gegenwart von 5-Dimethylaminopyridin). Solcherweise wurden 5-O-(N-Benzyloxycarbonyl-O-tert.butyl-L-threonly)-2,3-O-isopropylidenuridin (1), 5-O-(N-tert.Butyloxycarbonyl-O-benzyl-L-seryl)-2,3-O-isopropylidenuridin (2), 5-O-(N-tert.Butyloxycarbonyl-L-leucyl)-2,3-O-isopropylidenuridin (3) und 5-O-(N-tert.Butyloxycarbonyl-L-valyl)-2,3-O-isopropylidenuridine (4) nach Säulenchromatographie (Kieselgel) in guter Ausbeute hergestellt. Die Behandlung von2 mitTFA/CH₂Cl₂ (6:1) bei Zimmertemperatur (30 min) führte zu einer selektiven Abspaltung derBoc-Gruppe ohne Deblockierung der 2,3-O-Isopropylidengruppe des Uridins. Eine Behandlung von2 mitTFA/H₂O (5:1) bei Zimmertemperatur für 1 Stunde führte hingegen zur Abspaltung sowohl derBoc als auch der 2,3-O-Isopropylidengruppe. DieZ-Gruppe von1 wurde durch katalytische Hydrogenolyse auf 10% Pd/C/Ammoniumformiat abgespalten.

     

A spectrophotometric determination of the formation constants of the inclusion complexes ofα- andβ-cyclodextrins with the azonium and ammonium tautomers of methyl orange and methyl yellow

The color fading caused by the addition of-cyclodextrin or-cyclodextrin to an aqueous solution of a tautomeric mixture of methyl orange or methyl yellow is studied spectrophotometrically at pH 1.1 and 25.0°C. A model involving 1 : 1 stoichiometry has been used to analyze the spectrophotometric data. The addition of a cyclodextrin shifts the tautomeric mixture towards the side of the ammonium tautomer. An expression allowing the calculation of the tautomeric equilibrium constant of the inclusion complexes is derived. The formation constants of the inclusion complexes of the individual tautomers are determined. Both- and-cyclodextrins bind the ammonium tautomer stronger than the azonium tautomer. The inclusion complexes of-cyclodextrin are more stable than the corresponding ones of-cyclodextrin.     

Diastereoselectivity in theLewis acid mediated aldol reaction of chiral α, β-epoxyaldehydes with a ketene silyl acetal

Summary The Lewis acid mediated aldol reaction of chiral , -cis andtrans epoxyaldehydes1 and2 withtert-butyl ketene silyl acetal proceeds mainly withanti diastereofacial preference. The best results were obtained forcis epoxyaldehyde1 in the presence of catalytic amounts of BiCl₃·1.5 eq. ZnI₂ (anti:syn 13:1), whereas the poorest stereoselectivity was observed when an excess of LiClO₄ was used (anti:syn 1:1). The more stable epoxyaldehyde conformers were determined and the diastereofacial preference was found to be in agreement with a nucleophilic attack on the energetically more favoured conformers.

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Diastereoselektivität derLewis-Säure-katalysierten Aldolreaction zwischen chiralen , -Epoxyaldehyden und einem Ketensilylacetal

Zusammenfassung DieLewis-Säure-katalysierte Aldolreaktion der chiralen , -cis- und -trans-Epoxyaldehyde1 und2 mittert-Butylketensilylacetal verläuft stereoselektivanti. Die besten Ergebnisse wurden für dencis-Epoxyaldehyd1 in Gegenwart katalytischer Mengen BiCl3·1.5 eq. Znl₂ erhalten (anti:syn 13:1). Die geringste Stereoselektivität trat auf, wenn LiClO₄ im Überschuß eingesetzt wurde (anti:syn 1:1). Das beobachtete Verhalten steht mit einem nucleophilen Angriff am energetisch günstigeren Konformeren im Einklang.

     

2,5,6,7,8-Pentasubstituted (S)- and (R)-[2-chroman-2-yl]ethanols as intermediates for the synthesis of α-tocopherol and its chiral analogs

In the presence of lipase from the yeast Candida cylindracea, partial acetylation of (±)-2-[6-benzyloxy-2,5,7,8-tetramethylchroman-2-yl]ethanol with vinyl acetate gives S-(+)-acetate whose alkaline hydrolysis affords (S)-(–)-alcohol. Repeated enzymatic acetylation of the residual alcohol up to 39% conversion afforded the R-enantiomer. The enantiomeric alcohols were oxidized to (S)- or (R)-aldehydes having the same sign of []_D as the original alcohols. These alcohols were converted into S-(+)- and R-(–)-enantiomers of the antioxidant MDL-73404, a hydrophilic analog of -tocopherol.     

Synthese,Reaktionen und NMR-Spektren von 2-Brom-3-oxo-1-alkenyl- und 3-Oxo-1-alkinyl-phosphonsäure-dialkylestern

Dialkyl (E)-3-oxo-1-alkenylphosphonates (1), on reaction with bromine and subsequent HBr-elimination, yield the isomeric -bromovinyl derivatives (Z)-3 and (E)-3 and the alkinylphosphonates4. -Bromovinyl compounds3 can also be obtained by reaction of1 withNBS in aqueous solution. The configuration of the -disubstituted vinylcompounds is assigned from their¹³C-NMR spectra. Both bromovinyl compounds3 and alkinylderivatives4 are used for regioselective syntheses of acylsubstituted pyrazolylphosphonates5.

     

Enhanced reactivity of secondary hydroxyl groups in the O-alkylation of carbohydrate-related primary-secondaryvic-glycols. Regioselective 2-O-benzylation of 1,3:2,4-di-O-ethylidene-D-glucitol

Partial O-alkylation of 1,3:2,4-di-O-ethylidene-D-glucitol (1a), 1,2-O-isopropylidene-3-O-methyl--D-glucofuranose (1b), andR-(+)-1-O-benzylglycerol (1c) with benzyl chloride in a KOH/DMSO system results in products of monoalkylation at the secondary (4a–c) and at the primary hydroxyl (2a–c) in ratios of over 955 (a), 21 (b), and 11 (c), whereas (±)propane-1,2-diol (1d) gives only the product of 1-O-benzylation (2d). A qualitatively similar result is observed upon O-alkylation of diols (1a–e) with 2-methoxyethanol tosylate.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 4, pp. 776–781, April, 1993.     

Lipase-mediated deracemization of secondary 1-phenyl-substituted propargylic alcohols of different topology

Acetylation of (±)-1-phenylnon-2-yn-1-ol, (±)-1-phenylhept-1-yn-3-ol, and (±)-1-phenylundec-4-yn-3-ol ((±)-5) in the presence of lipase from Candida cylindracea (CCL) proceeds slowly to give products with ee 20%. The acetates of these alcohols are hydrolyzed in the presence of porcine pancreatic lipase (PPL) equally unsatisfactorily. The (⁶-arene)tricarbonylchromium complex of alcohol (±)-5 is acetylated in the presence of CCL up to 22% conversion to give (R)-acetate whose oxidative decomplexation followed by saponification results in alcohol (R)-(–)-5 with ee 95%. The configuration of alcohols (–)-5 and (+)-5 was determined by NMR spectroscopy of their esters with (R)- and (S)-Mosher"s acids.     

Thermal and BF<Subscript>3</Subscript>⋅Et<Subscript>2</Subscript>O-catalyzed cleavage of 1-hydrohexafluoroisobutenyloxytrimethylsilane. Perfluoromethacrolein,its isomers,dimers, and homopolymers

During vacuum pyrolysis in a quartz or steel tube, 1-hydrohexafluoroisobutenyloxytrimethylsilane (1) eliminates fluorotrimethylsilane to give perfluoromethacrolein, which was detected by NMR. Similar pyrolysis of silane 1 over KF results in E- and Z--hydrotetrafluoromethacryloyl fluorides. At 20 °C, perfluoromethacrolein undergoes homopolymerisation and/or cyclodimerization to yield 4,4-difluoro-2-pentafluoroisopropenyl-5-trifluoromethyl-4H-1,3-dioxin, which rearranges into E-7,7,7-trifluoro-2,6-bis(trifluoromethyl)-4-oxahepta-2,5-dienoyl fluoride under the action of BF₃Et₂O. The same fluoride is also formed, together with fluorotrimethylsilane, directly from silane 1 under the action of BF₃Et₂O.Published in Russian in Izvestiya Akademii Nauk. Seriya Khimicheskaya, No. 8, pp. 1629–1635, August, 2004.Deceased     

Synthesis of the grapevine moth sex pheromone by Grignard—Schlosser cross-coupling: The effect of the electrophile structure on the stereoisomeric ratio in the reaction products

1-Acetoxy-2E,4Z-heptadiene (4) and 1-bromo-3E,5Z-octadiene (5) were obtained with 90 and 88–92 % configurational purity, respectively, starting from 2,4-heptadiyn-1-ol or 3,5-octadiyn-1-ol. The Li₂CuCl₄-catalyzed cross-coupling of the allylic acetate4 with 5tert-butoxypentylmagnesium chloride affords 1-tert-butoxy-7E,9Z-dodecadiene (11) contaminated with 25 % of minor stereoisomers in 54–60 % overall yield. Under similar conditions, the homoallylic bromide5 reacts with 4-tert-butoxybutylmagnesium chloride to give in 50–52 % yield another sample of diene11 containing 17 % of minor stereoisomers. If the latter coupling is carried out with enyne8 instead of5 followed bycis-hydrogenation of the triple bond in the resulting product, the configurational purity of diene11 is as high as 84.7 % (45 % overall yield). The reaction of11 with Ac₂O in the presence of FeCl₃ leads directly to the target 7E,9Z-dodecadienyl acetate (1) with somewhat lower configurational purity than that of the starting ether11.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 6, pp. 1133–1137, June, 1993.     

Chiral β-hydroxycarbonyl compounds based on (−)-menthone: structure and behavior in liquid crystalline systems

It has been established by X-ray structural analysis that 2-(1-biphenyl-4-yl-1-hydroxy)methyl-p-menthan-3-one, one of the products of the reaction of (–)-menthone triisopropyloxytitanium enolate with 4-phenylbenzaldehyde, has a 1R,2S,4S,1S configuration. In crystals, this -hydroxyketone adopts a chair conformation with equatorial methyl and isopropyl groups and an axial 2-(1-biphenyl-4-yl-1-hydroxy)methyl substituent. Unlike the stereoisomeric compound with the 1R,2S,4S,1S configuration, the exocyclic fragment of which has an intramolecular >C=O...H-O- hydrogen bond in crystals and solutions, in the crystals of the 1R,2S,4S,1S ketol under study, molecules are linked by a network of cooperative -O-H...O-H...O-H... hydrogen bonds. Based on the results of molecular mechanics calculations and experimental data of¹H NMR and IR spectroscopy, conformations of molecules of this compound, which are in equilibrium in solution, have been characterized. Based on data on spatial structures of stereoisomeric -hydroxyketones and the character of H-bonds formed by these compounds, the characteristic features of the effect of these chiral alloying additives on the supramolecular structure and macroscopic properties of liquid crystalline systems have been interpreted.The results of a study of stereoselectivity of the reactions of different (–)-menthone enolates with aromatic aldehydes will be published later.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 7, pp. 1247–1255, July, 1995.The work was supported by the Foundation for Basic Research of the State Science and Engineering Committee of Ukraine (Project No. 93-3.2/75).     

Triterpene glycosides ofScheffleropsis angkae. II. Structure of glycosides L-E1, L-E2, L-K1, and L-K2

The structures of four triterpene glycosides from leaves ofScheffleropsis angkae (Araliaceae) are established using chemical and NMR methods. The structures 3-O--D-glucopyranosyl-(1-3)-O--L-arabinopyranosides of oleanic and ursolic acids and their 28-O--L-rhamnopyranosyl-(1-4)-O--gentiobiosyl ethers are proposed for L-E₁, L-E₂, L-K₁, and L-K₂, respectively. L-K₁ and L-K₂ are new triterpene glycosides.Translated from Khimiya Prirodnykh Soedinenii, No. 3, pp. 239–241, May–June, 2000.     

Ein einfacher Weg zu α-substituierten (E)-3-Oxo-1-alkenylphosphonsäureestern

Zusammenfassung -Substituierte -Acylvinylphosphonate3 mitE-Konfiguration [R ²CO-CH=C(R ¹)-P(O)(OR)₂], werden in guten Ausbeuten durchWittig-Reaktion von Acylphosphonsäureestern1 [R ¹CO-P(O)(OR)₂,R ¹=Alkyl oder Aryl] mit (2-Oxoalkyliden)triphenylphosphoranen2 [R ²CO-CH=PPh ₃,R ²=Alkyl, O-Alkyl oder CH₂ X (X=Br, OMe, CO₂ Et)] erhalten.

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A convenient route to -substituted dialkyl (E)-3-oxo-1-alkenylphosphonates

-Substituted dialkyl (E)--acylvinylphosphonates [R ²CO-CH=C(R ¹)-P(O)(OR)₂,3], are easily obtained in good yields byWittig-reaction of dialkyl acylphosphonates1 [R ¹CO-P(O)(OR)₂,R ¹=alkyl or aryl) with 2-oxoalkylidene triphenylphosphoranes2 [R ²CO-CH=PPh ₃,R ²=alkyl, O-alkyl and CH₂ X (X=Br, OMe, CO₂ Et)].

     

The effect of mechanical grinding on the formation and crystallinity changes of the inclusion complex of acetaminophen andβ-cyclodextrin

The effect of mechanical grinding on the physicochemical properties of acetaminophen in the presence of three additives,- or-cyclodextrin and microcrystalline cellulose, was studied by using TLC, powder X-ray diffraction analysis, infrared spectroscopy and differential scanning calorimetry. The results indicate that the crystallinity of physical mixtures of acetaminophen and the described additives decreased with increased grinding time and formed an amorphous state when mixtures containing- or-cyclodextrin were ground with acetaminophen. We also found that the acetaminophen molecules could be included step-by-step into the cavity of-cyclodextrin molecules and formed an amorphous inclusion complex.-Cyclodextrin and microcrystalline cellulose did not form an inclusion complex with acetaminophen, but acted only to decrease the crystallinity of the ground mixtures. The mechanical grinding efficiency for acetaminophen was improved in the order of-cyclodextrin -cyclodextrin > microcrystalline cellulose.This paper is part XI of Drug Interaction in Pharmaceutical Formulations.     

Ein einfacher Zugang zu (R)-γ-Amino-β-hydroxybuttersäure (GABOB) aus natürlichem (2S, 4R)-4-Hydroxyprolin

The oxidative decarboxylation sequence (1a 2a 3a 4a 5a) affording -aminobutanoic acid (5a) is adapted to the synthesis of its hydroxy derivative5b. A facile high yield conversion of (2S, 4R)-4-hydroxyproline-methylester-hydrochloride (7) to (R)-GABOB (5b) on a preparative scale is reported with the hydroxypyrrolidone8 as the intermediate.

     

β,β-Dinitro derivatives ofN-alkyl-N′-alkoxydiazene-N-oxides

Methods of synthesis ofN-alkyl-N-alkoxydiazene-N-oxides containing a carbonyl group in the -position of alkyl or alkoxy radicals were developed. ,-Dinitro derivatives ofN-alkyl-N-alkoxydiazene-N-oxides were synthesized for the first timevia nitration of oximes obtained from the ketones.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 8, pp. 1534–1538, August, 1995.     

Chain entanglement,mechanical properties and drawability of poly(lactide)

The observed brittle fracture behavior of amorphous polylactides seems to be contradicted by the low value ofC =2 determined for poly(L-lactide) by Flory and coworkers. Such very flexible polymer chains deform by shear yielding, and fracture in a ductile manner. In this study,C was estimated in a number of ways, resulting in much higher values ofC =11.7 andC =9.1 for poly(L-lactide) and L- and D-lactide copolymers, respectively. These high values ofC and the low entanglement density account for the brittle fracture behavior of amorphous poly(lactide), as well as for the maximum attainable draw ratios of poly(L-lactide) networks and melt spun fibers. Bulk polymerized poly(L-lactide) networks, where crystallization during polymerization impedes severe entangling, could be hot-drawn most effectively to draw ratios of 8–16, resulting in very strong materials with tensile strengths of 550–805 MPa. By comparison, amorphous, non-crystallizable L/D lactide networks, which do not crystallize during polymerization, could be drawn less, to =7. These materials with strengths up to 460 MPa could, nevertheless, be oriented much more effectively than linear, amorphous L/D lactide copolymers.     

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.