Photolyse von 2-oxo-[2-13c]-1-diazocyclohexan. Ein beitrag zum oxiren-problem

The synthesis of 2 - oxo - [2 - ¹³C] -1 - diazocyclohexan (10) starting with K¹³CN is described. Photolysis of 10 in dioxan-water yields cyclopentancarboxylic acid containing all the label in the carboxy group, which has been proved by C-13 NMR spectroscopy and electron impact induced fragmentation. The absence of isotope scrambling in the photolytic ring contraction excludes an oxiren participation.     

Chemie der pleuromutiline—II : Synthese des 12-desvinylpleuromutilins

Oxidation of the AB-trans-anellated Pleuromutilin-derivative 7¹ with Ozone followed by decarbonyl- ation gave the corresponding desvinyl-compound 10. A 1,5-hydride shift between C-3 and C-11 leads to the title compound 11. The 12-methyl group of10 was assigned the α-configuration on the basis of chemical and spectroscopic data.     

Syntheses and conformational analyses of new naphth[1,2-e][1,3]oxazino[3,2-c]quinazolin-13-ones

The syntheses of naphth[1,2-e][1,3]oxazino[3,2-c]quinazolin-13-one derivatives (3a–f) were achieved by the solvent-free heating of benzyloxycarbonyl-protected intermediates (2a–f) with MeONa. For intermediates 2a–f, prepared by the reactions of substituted aminonaphthols with benzyl N-(2-formylphenyl)carbamate, not only the expected trans ring form B and chain form A¹, but also the rearranged chain form A² as a new tautomer were detected in DMSO at room temperature. The quantity of A² in the tautomeric mixture was changed with time.Conformational analyses of the target heterocycles 3a–f by NMR spectroscopy and accompanying theoretical calculations at the DFT level of theory revealed that the oxazine ring preferred a twisted chair conformation and the quinazolone ring was planar. Besides the conformations, both the configurations at C-7a and C-15 and the preferred rotamers of the 1-naphthyl substituent at C-15 were assigned, which allowed evaluation of the aryl substituent-dependent steric hindrance in this part of the molecules. Configurational assignments were corroborated by quantifying the ring current effect of 15-aryl in terms of spatial NICS.     

Synthesis and absolute configuration of two diastereoisomeric (1R,2S,3R)-and (1S,2S,3R)-2-amino-1-(2-furyl)-1,3-butandiols

The synthesis of (1R, 2S, 3R) and (1S, 2S, 3R)-2-(N-benzoylamino)-1-(2-furyl)-1, 3-butandiols (15) and (16) from D-threonine is described. The assignment of absolute configuration of the newly formed asymmetric center at C-1 was based on the ¹H-NMR spectra of O-isopropylidene derivatives 17 and 18.     

Aufkl?rung der 1H- und 13C-NMR-spektren sowie der kristallstruktur unges?ttigter glycosylphosphonate und konformationsberechnungen an modellen1

By application of a modified LAOCN-3 program a complete elucidation of the ¹H NMR spectra of 2,3-unsaturated glycosyl phosphonates 1–5 could be achieved. The exactly determined ⁿJ(H, H) and novel ⁿJ(C, P) coupling constants are discussed, and permit a conclusive deduction of the conformations. The ¹³C NMR spectra of 1 to 6 can be fully interpreted. By a close inspection of chemical shifts as well as ¹J(C-H) and ⁿJ(C, P) coupling constants the conformational assignment is supported. For all the derivatives the correlations ¹J(C-1,H_e)>¹J(C-1, H_a) and ¹J(C-1, P_e) >¹J(C-1, P_a) can be used for the assignment of anomers. The crystal structure of 1 is in accordance with this assignment of anomers and displays an unexpected conformation. Calculations by MINDO-3 in resembling model compounds serve to elucidate such conformative effects.     

Addition conjuguée dans le thf-hmpt d'arylacétonitriles lithies aux cyclohexèn-2 ones substituées: intervention des facteurs stériques et électroniques

The reaction of lithiated arylacetonitriles 2a-c with 2-cyclohexenones 3-9 in THF-HMPA (80:20 v/v) at ?70° leads in all cases but one to δ-ketoalkylnitriles, resulting from 1,4-addition. The only case where some 1,2-addition takes place is the reaction of 2a with 4,4-dimethyl 2-cyclohexenone 7. The formation of allylic alcoholates, products of 1,2-addition, is shown to be reversible in this solvent mixture. However, in several cases, kinetic control of 1,4-addition is demonstrated. The rate of formation of 1,4-addition products depends upon the arylacetonitrile substituents: 2a >2b >2c (i.e. the higher lying the nucleophile HOMO the faster the reaction). It is also sensitive to the cyclohexenone substituents; although methyl on C-2 and gem-dimethyl on C-5 or t-butyl on C-4 have small influence on the reaction rate, methyl on C-3 or gem dimethyl on C-4 induce a noticeable rate decrease. The addition, of 2b on 4-t-butyl 2-cyclohexenone 8 leads, at the early stage, to a predominating isomer 15b, to which the trans diaxial configuration of the substituents has been attributed by 250 MHz ¹H NMR. A single transition state model, reagent-like, where the nucleophile approaches the C-C bond by the less hindered face of the 2-cyclohexenone in a 1,2-diplanar conformation, the CN substituent being directed towards the C=0 group, accounts for all the substituent effects and the stereoselectivity observed.     

Méthylène-indolines,indolénines et indoléniniums—XIII: L'hydroxy-16 déhydro-1 vincadifformine,intérmédiaire dans le réarrangement biomimétique de la vincadifformine en vincamine

The title compound is a crucial intermediate in the biomimetic conversion of vincadifformine 1 into vincamine 7. Its configuration at C-16 is established by a combination of chemical and spectroscopic evidence. Iodine oxidation converts 14 into the bridged lactam 18, thus proving a β configuration for the hydroxy group at C-16. The same reaction applied to vindoline 19 gives 21 identical with one of the compounds obtained by microbiological transformation of 19. The ¹³C NMR spectra of derivatives 3 and 8 (obtained by oxidation of vincadifformine) show that oxidation proceeds with introduction of the substituent at C-16, with a β-configuration. The alcohol 3 however, posesses a different conformation due to strong hydrogen bonding with N-4.     

13C nuclear magnetic resonance spectroscopy of atisine and veatchine-type C20-diterpenoid alkaloids from aconitum and garrya species

¹³C NMR spectra of the atisine- and veatchine-type alkaloids, as well as certain of their derivatives, have been obtained by the Fourier transform technique at 25.03 MHz. With the help of single-frequency off-resonance proton decoupling techniques, additivity relationships, and the effects induced by certain structural changes, self-consistent assignments of nearly all the resonances have been made. The ¹³C NMR spectra are also analyzed to identify skeletal features of the atisine and veatchine-type alkaloids of use in the structure determination of new C₂₀-diterpenoid alkaloids. On the basis of the ¹³C NMR analysis of atisine and veatchine as well as a temperature-dependence study of atisine, the existence of C-20 epimers in these alkaloids is demonstrated. A ¹³C NMR study of the behavior of the oxazolidine ring of atisine in non-ionic and ionic solvents indicates that the C-20 epimers of atisine do not exist in an equilibrium mixture in solution and are not interconvertible via a zwitterion as reported earlier.     

Partial synthesis of a marine secosterol from Gersemia fruticosa: Preparation of the intermediate precursor 3β,6α-diacetoxy-24-methyl-12-oxo-5α-chol-9,11-en-24-oate

The conversion of desoxycholic acid (2) into the title compound 14 by 13 respectively 17 steps is described herein, including stereoselective construction of C-3 and C-6 hydroxy moieties and introduction of a Δ^9,11 double bond by dehydrogenation. 14 is believed to serve as a putative precursor for the synthesis of secosterol 1, isolated from the soft coral Gersemia fruticosa.     

Zum Mechanismus der Photochemie des Benzfurazans

Mechanistic studies on the photochemical reactions of benzfurazan . From other works it is known that irradiation of benzfurazan ( 1 ) in methanol gives the carbaminacid-ester 4 , whereas in benzene the azepinederivative 3 is obtained (Scheme 1). The compounds 5–8 (Scheme 2) have been proposed as intermediates. In our investigations we detected and characterized by means of UV.- and IR.-spectroscopy the two species 5 and 8 . Irradiation of 1 with 350 nm light at room temperature in a strongly polar solvent (e.g. H₂O) yields exclusively 5 (Fig. 1) with a quantum yield of 0.48. In non polar solvents (e.g. hexane) 5 isomerizes in a second photochemical step to 8 (quantum yield 0.43) (Fig. 3). Thermally, 5 can be converted back to 1 . The rate constant for this reaction at room temperature is 2 · 10^–5s^–1. The transformation 5 → 8 was also investigated at low temperature. There was no direct evidence for any intermediates of the type oxazirene ( 6 ) or nitrene ( 7 ). However, the formation of azepine 3 upon irradiation of 5 in benzene suggests as intermediate the nitrene 7 which could be converted into 8 in a fast thermal reaction (Scheme 3).     

Carbon-carbon coupling in [3-13C1]tryptophan

Carbon-carbon coupling constants have been observed in [90% 3-¹³C₁]tryptophan and used to assign the ¹³C resonances of the indole ring. The results support a reassignment of C-5 and C-6 recently suggested on the basis of the reassigment of the corresponding resonances in indole. Coupling constants are compared with theoretical values obtained using a finite perturbation theory Blizzard-Santry program, and excellent agreement is obtained for the ¹J(CC) values. The calculations predict that the Fermi contact contribution is dominant for all ⁿJ(CC) couplings to C-3.     

5-epi-Deoxyrhamnojirimycin is a potent inhibitor of an α-l-rhamnosidase: 5-epi-deoxymannojirimycin is not a potent inhibitor of an α-d-mannosidase

Whereas deoxyrhamnojirimycin (LRJ) 1 shows no significant inhibition of naringinase (an α-l-rhamnosidase), its C-5 epimer 2 is a potent and specific inhibitor of the enzyme and demonstrates the value of unambiguous chemical synthesis of such materials in the evaluation of their biological properties. In contrast, moderately weak inhibition towards an α-d-mannosidase is shown by both deoxymannojirimycin (DMJ) 5 and its C-5 epimer 6. Mimics of l-rhamnose which are recognised by enzymes that synthesise or process l-rhamnose may inhibit either the biosynthesis of the sugar or its incorporation into mycobacterial cell walls, providing new strategies for the treatment of diseases such as tuberculosis and leprosy. Molecular modelling studies provide a rationale for the surprisingly potent activity of the C-5 epimer 2 compared with LRJ 1 and support a general hypothesis that potent piperidine glycosidase inhibitors mimic the ⁴H₃ conformation of the relevant glycopyranosyl cation intermediate.     

A short route to the phthalideisoquinolines and the 13-hydroxylated protoberberines

CrO₃ oxidation of 2′-hydroxymethylpapaverine (2) yields the aromatic phthalideisoquinoline 3. Catalytic reduction of 3 gives the erythro-norphthalideisoquinoline 7 and the threo analog 9. Respective N-methylation furnishes the erythro-phthalideisoquinoline 8, and the threo isomer 10. The nor compounds 7 and 9 can be converted in hydroxylic base to the lactam alcohols 11 and 12, respectively; but 12 tends to dehydrate to the oxyprotoberberine 15. LAH reduction of 11 and 12 affords in turn the 13-hydroxyprotoberberines 13 and 14. Three fractors affect the conformation of the phthalideisoquinolines, namely the relative stereochemistry at C-1 and C-9, substitution on nitrogen, and substitution at C-8.     

Copper(II), iron(III) and cobalt(III) complexes of the pendent-arm cyclam derivative 6,6,13-trimethyl-13-amino-1,4,8,11-tetraazacyclotetradecane

The interaction of Cu(II), Fe(III) and Co(III) with 6,6,13-trimethyl-13-amino-1,4,8,11-tetraazacyclotetradecane (L ³ ) incorporating a pendent amine group has led to isolation of the new octahedral complexes [Cu(HL ³ )(ClO₄)₂]Cl·H₂O (1), [Fe(L ³ )Cl](S₂O₆)·H₂O (2), [Co(L ³ )Cl](ClO₄)_1.5Cl_0.5·0.25H₂O (3), [Co(HL ³ )Cl₂](ClO₄)₂·H₂O (4) and [Co(L ³ )Cl]₂(S₂O₄)(ClO₄)₂ (5). In (1) the copper ion occupies the macrocyclic cavity of protonated (–NH₃ ⁺) L ³ which is present in its trans-III configuration; weakly bound ClO₄ ^? ligands occupy the axial positions. The X-ray structure of (2) showed that Fe(III) occupies the N₄-macrocyclic cavity of L ³ in a trans-III configuration, with the pendent amine group binding in an axial position. The remaining axial position is occupied by a Cl^? ligand. Chromatography of the product obtained from the reaction of Na₃[Co(CO₃)₃] with L ³ yielded three fractions. Fraction 1 yielded crystals (3) composed of three crystallographically independent species incorporating cations of type [Co(L ³ )Cl]²⁺ with very similar structures; in each case the macrocyclic ring nitrogens of L ³ are bound to the Co(III) in an asymmetric cis-fashion. Fraction 2 yielded the trans-III octahedral cationic complex (4) incorporating L ³ in its protonated form. The Co(III) complex (5) from fraction 3 shows a different coordination arrangement to the products from fractions 1 or 2. The macrocyclic ring coordinates in its trans-III form, but the axial sites in this case are occupied by the pendent-NH₂ group and a Cl^? ligand.     

Enantiospecific synthesis of the sugar amino acid (2S,5S)-5-(aminomethyl)-tetrahydrofuran-2-carboxylic acid

An enantiospecific synthesis of the tetrahydrofuran amino acid (2S,5S)-5-(aminomethyl)-tetrahydrofuran-2-carboxylic acid 1 is reported. The sugar enone 2-(S)-octyl 6-O-acetyl-3,4-dideoxy-α-d-glycero-hex-3-enopyranosid-2-ulose 2a, derived from galactose, was employed as a chiral precursor. The enone 2a was converted by chemical manipulation of the functional groups into the 6-azido-2-O-tosyl-3,4,6-trideoxy-d-erythro-hexono-1,5-lactone 9 as key intermediate. Methanolysis of 9 induced the opening of the lactone and the attack of the hydroxyl group at C-5 to C-2 with the displacement of the tosylate. This reaction led to the formation of the tetrahydrofuran ring of methyl (2S,5S)-5-(azidomethyl)-tetrahydrofuran-2-carboxylate 10, which was readily converted into 1. The overall yield of the sequence was 35%, and all the intermediates and the final product have been fully characterized. In addition, the preferential conformations in solution of lactone 9 and target molecule 1 have been established.     

17α-Konfigurierte 20-methylpregnan-derivate

A mixture of 1a+1b (17α), obtained by C-17-epimerization of pregnenolone (1a) was converted into 3a+3b by Wittig-reaction. 3a+3b were acetylated to a mixture of 4a+4b, from which 4b was isolated by cristallization of 3a and following AgNO₃-chromatography of the mother-liquors. Δ²⁰⁽²²⁾ → Δ¹⁷-doublebond-isomerization occurs by hydrogenation (Pd/C) of 3a (17β) to give 5. Hydrogenation (Pt-catalyst) of 4b (17α) leads to 8b, which was converted into the 20-methylpregnane-derivatives 7b, 9b–13b. By comparison with the 17β epimers 1a–4a, 7a–13a a spectroscopic determination of the relative configuration on C-17 of 17-alkylsubstituted steroids was possible.     

New findings in the alkylation and N-deprotection of (4S)-4-methyl-2-benzyl-2,4-dihydro-1H-pyrazino[2,1-b]quinazoline-3,6-diones

Alkyl halides behave differently to benzyl halides in C-1 alkylation of the title compounds. The syn and anti 1,4-disubstituted diastereomers thus obtained show different regioselectivity by further alkylation leading to the 1,4,4- and 1,1,4-trisubstituted compounds, respectively. Alkylation is always directed anti with respect to the bulkier substituent at C-1 or C-4. Debenzylation attempts on 2-benzyl-derivatives 1b by treatment with HCOOH and C/Pd or H₂/C–Pd/MeOH/H⁺ led to C-1 oxidised or 7,8,9,10-tetrahydro-derivatives. Deprotection of 2-p-methoxybenzyl- and 2-(2,4-dimethoxybenzyl)-derivatives with CAN and with TFA/anisole, respectively, was successful, but in the latter case epimerization at C-1 occurred.     

Imino-enamine tautomerism and dynamic prototropy in 1-imino-3-amino-1H-indens

The tautomeric structures and dynamic prototropic behavior of the products 1 and 2 obtained in the condensation reaction of 1,3-indandione and 2-pyridyl-1,3-indandione with p-toluidine, respectively, were investigated by ¹H NMR spectroscopy and X-ray analysis. In the solid state, compound 1 is in an imino-enamine tautomeric form, whereas in solution it coexists with an imino-imino tautomeric form. Dynamic 1,5-prototropic interconversion of the imino-enamine form was revealed to be very fast at room temperature by temperature-dependent ¹H NMR spectra. For 2, the imino-enamine form is the only species present in solution. The hydrogen of the enamine NH is hydrogen-bonded intramolecularly with the nitrogen in the pyridine ring. When the temperature is raised, the NH proton enters into dynamic 1,5-migration, which is accompanied by internal rotation around the pivot bond, which changes the hydrogen-bonding sites. For the condensation product 3 of 2-(2-quinolyl)-1,3-indandione with p-butylaniline, dynamic behavior similar to that found in 2 was observed also in ¹³C NMR spectra.     

The stereochemistry of 2,4-disubstituted γ-butyrolactones and 2,4,6-trisubstituted-5,6-dihydro-4H-1, 3-oxazines

2,4-Disubstituted butyrolactones and 2,4,6-trisubstituted-5,6 dihydro-4H-1,3-oxazines show similar features in their ¹H and ¹³C- NMR spectra. Two geminal ring hydrogens of cis isomers give rise to a complex ABXY spectra when the substituent is alkyl or aryl. In spectra of trans isomers these patterns are degenerated. When R is OMe(in 4) or OCOMe (in 6) the difference in chemical shifts of geminal protons and vicinal coupling constants cannot be used for diagnosis. In ¹³C spectra ring carbons C-2 and C-3 in lactones and C-4 and C-5 in oxazine of trans isomers show a small but consistent shift to higher fields.     

Long range carbon—carbon coupling in olefins. 4-13C-4-propyl-3-heptene and 1-13C-1-methylcyclohexene

All ¹³C—¹³C splittings involving the C-4 carbon of 4-propyl-3-heptene and the C-1 carbon of 1-methylcyclohexene were determined from the appropriately labeled (> 90%-¹³C) derivatives. The observed trends in coupling constants continue to offer additional means of carbon chemical shift assignments and to provide mechanistic information regarding the nature of long range carbon—carbon coupling.