Stereospezifische Fragmentierungen in den Massenspektren von Cyclohexandiaminen und Bis(aminomethyl)cyclohexanen. 33. Mitteilung über massenspektrometrische Untersuchungen,,

Stereospecific Fragmentations in the Mass Spectra of Cyclohexanediamines and Bis(aminomethyl)cyclohexanes The mass spectral behaviour, especially loss of NH₃, of the six isomeric cyclohexanediamines 1--3 (cis and trans each, Scheme 1) as well as of the six isomeric bis(aminomethyl)cyclohexanes 4--6 (cis and trans each, Scheme 6) has been investigated. The cis- and trans-compounds of the 1,2-isomers 1 and 4 show very similar spectra, because of the ease of ring cleavage at C(1)–-C(2) and the similar geometrical relations in all ring conformations. The cis- and trans-compounds of both the 1,3- and 1,4-isomers 2, 3, 5 and 6 show striking differences in their mass spectra due to stereospecific elimination of NH₃ from the molecular ion.     

Bortrifluorid-katalysierte Umsetzungen von 3-Amino-2H-azirinen mit Aminosäure-estern und Aminen

Boron-Trifluoride-Catalyzed Reactions of 3-Amino-2H-azirines with Amino-acid Esters and Amines After activation by protonation or complexation with BF₃, 3-amino-2H-azirines 1 react with the amino group of α-amino-acid esters 3 to give 3,6-dihydro-5-aminopyrazin-2(1H)-ones 4 by ring enlargement (Scheme 2, Table 1). The configuration of 3 is retained in the products 4 . With unsymmetrically substituted 1 (R¹ ≠ R²), two diastereoisomers of 4 (cis and trans) are formed in a ratio of 1:1 to 2:1. With β-amino-acid esters 5 and 7 , only openchain α-amino-imidamides 6 and 8 , respectively, are formed, but none of the seven-membered heterocycle (Scheme 3). Primary amines also react with BF₃-complexed 1 to yield α-amino-imidamides of type 9 (Scheme 4, Table 2). Compound 9b is characterized chemically by its transformation into crystalline derivatives 10 and 12 with 4-nitrobenzoyl chloride and phenyl isothiocyanate, respectively (Scheme 5). The structure of 12 is established by X-ray crystallography. Mechanisms for the reaction of activated 1 with amino groups are proposed in Schemes 6 and 7.     

1,3‐Thiazolidine‐dicarboxylates from Thioketones and Thermally Generated Azomethine Ylides

The reaction of 9H‐fluorene‐9‐thione ( 1 ) with the cis‐ and trans‐isomers of dimethyl 1‐(4‐methoxyphenyl)aziridine‐2,3‐dicarboxylate (cis‐ and trans‐ 2 , resp.) in xylene at 110° yielded exclusively the spirocyclic cycloadduct with trans‐ and cis‐configurations, respectively (trans‐ and cis‐ 3 , resp.; Scheme 1). Analogously, less‐reactive thioketones, e.g., thiobenzophenone ( 5 ), and cis‐ 2 reacted stereoselectively to give the corresponding trans‐1,3‐thiazolidine‐2,4‐dicarboxylate (e.g., trans‐ 8 ; Scheme 2). On the other hand, the reaction of 5 and trans‐ 2 proceeded in a nonstereoselective course to provide a mixture of trans‐ and cis‐substituted cycloadducts. This result can be explained by an isomerization of the intermediate azomethine ylide. Dimethyl 1,3‐thiazolidine‐2,2‐dicarboxylates 14 and 15 were formed in the thermal reaction of dimethyl aziridine‐2,2‐dicarboxylate 11 with aromatic thioketones (Scheme 3). On treatment of 14 and 15 with Raney‐Ni in refluxing EtOH, a desulfurization and ring‐contraction led to the formation of azetidine‐2,2‐dicarboxylates 17 and 18 , respectively (Scheme 4).     

The Absolute Configuration of (+)‐Ethyl cis‐1‐Benzyl‐3‐hydroxypiperidine‐4‐carboxylate and (+)‐4‐Ethyl 1‐Methyl cis‐3‐Hydroxypiperidine‐1,4‐dicarboxylate; a Revision

Discrepancies between chiroptical data from the literature and our determination of the structure of the title compounds (+)‐ 5 and (+)‐ 9a were resolved by an unambiguous assignment of their absolute configuration. Accordingly, the dextrorotatory cis‐3‐hydroxy esters have (3R,4R)‐ and the laevorotatory enantiomers (3S,4S)‐configuration. The final evidences were demonstrated on both enantiomers (+)‐ and (?)‐ 5 by biological reduction of 4 by bakers' yeast and stereoselective [Ru^II(binap)]‐catalyzed hydrogenations of 4 (Scheme 2), by the application of the NMR Mosher method on (+)‐ and (?)‐ 5 (Scheme 3), as well as by the transformation of (+)‐ 5 into a common derivative and chiroptical correlation (Scheme 4).     

Determination of absolute configuration using vibrational circular dichroism spectroscopy: phenyl glycidic acid derivatives obtained via asymmetric epoxidation using oxone and a keto bile acid

The (+)-enantiomers of the o-Br, m-F and p-CH₃ derivatives of trans phenyl glycidic acid have been obtained from the corresponding trans cinnamic acid derivatives using Oxone and the tri-keto bile acid dehydrocholic acid. Vibrational circular dichroism (VCD) spectroscopy of their methyl esters has been used to determine their absolute configurations. In each case, the absolute configurations of both methyl ester and parent acid were shown to be (2S,3R)-(+)/(2R,3S)-(−).     

Über die Stereospezifität der α-Alkylierung von β-Hydroxycarbonsäureestern. Vorläufige Mitteilung

About the Stereospecific α-Alkylation of β-Hydroxyesters It was found, that dianions derived from β-hydroxyesters with lithium diisopropylamide (LDA) at ?50 to ?20° were alkylated stereospecifically (Scheme 1). The stereospecificity was 95–98%, the threo-compound (threo -2, -3 and -4) being the main product. This was proved for threo -2 and -3 by preparing the β-lactones 7 and 8 , respectively, which were pyrolyzed to trans-1, 4-hexadiene (9) and trans-1-phenyl-2-butene (10) , respectively (Scheme 2). Moreover, the acid threo -6 from threo -3 was converted by dimethylformamide-dimethylacetal to cis-1-phenyl-2-butene (11) (s. footnote 6). The alkylation of α-monosubstituted β-hydroxyesters also turned out to be stereospecific. Reduction of 16 and 18 with actively fermenting yeast furnished (+) -17 and (+) -2. respectively (Scheme 4), which were each mixtures of the (2R, 3S)- and the (2S, 3S)-isomers. Alkylation of (+) -17 with allyl bromide yielded after chromatography (2S, 3S) -19 and of (+) -2 with methyl iodide (2R, 3S) -19 , the oxidation of which finally gave (S)-(?) -20 and (R)-(+) -20 , respectively.     

Synthesis of Coumarins and Derivatives. Part 1. Biomimetic synthesis of esculetin and halogenated derivatives

Esculetin ( 1 ) and the novel compounds 5-chloroesculetin ( 5 ) and 5-bromoesculetin ( 6 ) were obtained from a light-induced cyclization of trans-caffeic acid ( 3 ) catalyzed by [FeNa(edta)] and/or H₂SO₄, HCI, or HBr (Scheme 1). The experimental conditions for trans-cis-isomerization of the cinnamic-acid derivative 3 and subsequent non-enzymatic cyclization were described. The photoperiod and the presence of air and iron-chelate catalyst are shown to be important parameters that markedly affect yields. The reactions probably occur by a free-radical mechanism involving a photo-initiated one-electron redox process (Scheme 2).     

Konkurrenz von Endoperoxid- und Hydroperoxid-Bildung bei der Umsetzung von Singulett-Sauerstoff mit cyclischen,konjugierten Dienen. Teil I

Competition of Endoperoxide and Hydroperoxide Formation in the Reaction of Singlet Oxygen with Cyclic, Conjugated Dienes Rose-bengal-sensitized photooxygenation of (?)-(R)-α-phellandrene ( 1 ) in MeOH at room temperature yielded a complex mixture of products, contrary to previous reports describing cis-(3S, 6R)-epidioxy-p-menthene ( 2 ) and trans-(3R, 6S)-epidioxy-p-menthene ( 3 ) as the only products. The mixture was separated by prep. HPLC (silica gel, pentane/Et₂O 9:1). Besides the known endoperoxides 2 (yield 39%) and 3 (26%), all those hydroper-oxides, which can be deduced from an ene reaction of ¹O₂ with 1 , were isolated, i.e. 4β-p-mentha-2,5-dien-1β-yl hydroperoxide ( 4 ) (14%), 4β-p-mentha-2,5-dien-1α-yl hydroperoxide ( 5 ) (9%), (2R, 4R)-p-mentha-1(7), 5-dien-2-yl hydroperoxide ( 6 ) (2,1%), (2S, 4R)-p-mentha-1(7),5-dien-2-yl hydroperoxide ( 7 ) (1,5%) and (1R)-p-mentha-3,6-dien-yl hydroperoxide ( 8 ; 1,5%; Scheme 1). Furthermore, the constant cis/trans ratio for all diastereoisomeric pairs ( 2 / 2 , 4 / 2 , 6 / 2 ) was striking. With the help of the two possible conformers 1a and 1b of the starting material a model of a common first step for endoperoxide as well as for hydroperoxide formation is developed. A photooxygenation at ?50° supports this model. The absolute value of the cis/trans ratio changes in the same way for the endoperoxides and the hydroperoxides.     

Semi-preparative high-performance liquid chromatographic separation of ceralure and related isomers

Summary A semi-preparative high-performance liquid chromatographic procedure on 5-m silica was developed for the isolation of gram quantities of ethyltrans-5-iodo-trans-2-methylcyclohexane-1-carboxylate (B₁) and ethyltrans-4-iodo-trans-2-methylcyclohexane-1-carboxylate (B₂) for comparative evaluation as male Mediterranean fruit fly,Ceratitis capitata, attractants and for NMR studies. This procedure can also be used analytically to determine the content of B₁ (the attractive isomer) in ceralure, the ethyl 4- and 5-iodo-trans-2-methylcyclohexane-1-carboxylate mixture. 1,1-Dimethylethylcis-5-iodo-trans-2-methylcyclohexane-1-carboxylate (A) and 1,1-dimethylethylcis-4-iodo-trans-2-methylcyclohexane-1-carboxylate (C) were isolated and converted to their ethyl esters, thus supplying the fourtrans-isomers of ceralure.     

Optisch aktive 4,5-Epoxy-4,5-dihydro-α-ionone und Synthese der stereoisomeren 4,5:4′,5′-Diepoxy-4,5,4′,5′-tetrahydro-ϵ,ϵ-carotine und der sterische Verlauf ihrer Hydrolyse

Optically Active 4,5-Epoxy-4,5-dihydro-α-ionones; Synthesis of the Stereoisomeric 4,5:4′,5′-Diepoxy-4,5,4′,5′-tetrahydro-?,?-carotenes and the Steric Course of their Hydrolysis We prove that epoxidation with peracid of α-ionone, contrary to a recently published statement, predominantly leads to the cis-epoxide. Acid hydrolysis affords a single 4,5-glycol whose structure, established by an X-ray analysis, shows that oxirane opening occurred with inversion at the least substituted position (C(4)). Stable cis-and trans-epoxides are prepared by epoxidation of the C₁₅-phosphonates derived from α-ionone. Both the racemic and optically active form are used for the synthesis of the 4,5:4′,5′-diepoxy-4,5,4′,5′-tetrahydro-?,?-carotenes having the following configuration in the end groups: meso-cis/cis, meso-trans/trans, rac-cis/trans, rac- and (6R, 6′ R)-cis/cis, rac- and (6R, 6′R)-trans/trans, rac- and (6R, 6′R)-cis/trans, and (6R, 6′ R)-cis/?. Acid hydrolysis of the cis/cis-epoxycarotenoids under relatively strong conditions occurs again with inversion at C(4)/C(4′) in case of the cis/cis-epoxycarotenoids, but at C(5)/C(5′) in case of the trans/trans-epoxycarotenoids. An independent synthesis of this 4,5,4′,5′-tetrahydro-?,?-carotene-4,5,4′,5′-tetrol is presented. The irregular results of the oxirane hydrolysis are explained by assumption of neighbouring effects of the lateral chain. 400-Mz-¹H-NMR data are given for each of the stereoisomeric sets. In the visible range of the CD spectra, the (6R, 6R′)-epoxycarotenoids compared with (6R, 6R′)-?,?-carotene exhibit an inversion of the Cotton effects.     

Absolute Konfiguration von Loroxanthin (=(3R, 3′R, 6′R)-β, ϵ-Carotin-3, 19, 3′-triol)

Absolute Configuration of Loroxanthin (=(3R, 3′R, 6′R)-β, ?-Carotene-3, 19, 3′-triol) ‘Loroxanthin’, isolated from Chlorella vulgaris, was separated by HPLC. methods in two major isomers, a mono-cis-loroxanthin and the all-trans-form. Solutions of the pure isomers easily set up again a mixture of the cis/trans-isomers. Extensive ¹H-NMR. spectral measurements at 400 MHz allowed to establish the 3′, 6′-trans-configuration at the ?-end group in both isomers and the (9E)-configuration in the mono-cis-isomer. The absolute configurations at C(3) and C(6′) were deduced from CD. correlations with synthetic (9Z, 3R, 6′R)-β, ?-carotene-3, 19-diol ( 5 ) and (9E, 3R, 6′R)-β, ?-carotene-3, 19-diol ( 6 ), respectively. Thus, all-trans-loroxanthin ( 3 ) is (9Z, 3R, 3′R, 6′R)-β, ?-carotene-3, 19, 3′-triol and its predominant mono-cis-isomer is (9E, 3R, 3′R, 6′R)-β, ?-carotene-3, 19, 3′-triol ( 4 ). Cooccurrence in the same organism and identical chirality at all centers suggest that loroxanthin is biosynthesized from lutein ( 2 ).     

Stereochemical control in microbial reduction. Part 31: Reduction of alkyl 2-oxo-4-arylbutyrates by baker's yeast under selected reaction conditions

Treatment of baker's yeast with phenacyl chloride in an aqueous–organic solvent has been proven to be an effective method of inhibiting the enzymes that afford (S)-enantiomers of α-hydroxy esters in the reduction of α-keto esters. The procedure is effective for the whole-cell system to produce the (R)-product with high chemical yield and high enantiomeric excess.     

Ⅱ conjugation in the butadiene

The π electronic delocalization in trans-C4H6 and cis-C4H6 has been investigated in the frame of ab initio valence bond theory with 6-31G basis set. The result shows that the Csp2-Csp2 single bond length (1.506 A) is only about 0.024 A shorter than the Csp3-Csp3 bond, thus the central bond length shortening would be mainly due to π conjugation. The theoretical resonance energies of the trans-C4H6 and cis-C4H6 are 8.48 and 7.44 kcal/mol, respectively.     

Investigations on organoantimony compounds : XVII. Preparation and properties of heterocyclic trans-dichloro-β-diketonato-cis-diorganoantimony(V) compounds. Influence of stereochemistry on β-diketonate ligand exchange reactions in octahedral dichloro-β-diketonatodiorganoantimony(V) compounds

A series of heterocyclic trans-dichloro-β-diketonato-cis-diorganoantimony(V) compounds of the type R₂SbCl₂X (R₂ = (CH₂)₄, (CH₂)₅, o,o′−C₆H₄C₆H₄, o,o′−C₆H₄CH₂C₆H₄; X = Acac, Dpm) has been synthesized. The stereochemistry of these compounds has been deduced from PMR spectroscopic and molecular dipole moment data. Since the cis-dichloro-β-diketonato-trans-diorganoantimony(V) compounds R₂SbCl₂Acac (R = Me, Et, Ph) were known previously, a set of both cis- and trans-diorgano main group organometallic complexes has thus been made available, which allows a comparative study of the influence of stereochemistry on the strength of metal—ligand interactions in this type of octahedral d¹⁰ metal complex. β-Diketonate—ligand exchange reactions have been studied by PMR spectroscopy, and a marked influence of stereochemistry observed. trans-Dichloro-β-diketonato-cis-diorganoantimony(V) compounds undergo ligand exchange only slowly, if at all, whereas cis-dichloro-β-diketonato-trans-diorganoantimony(V) compounds react instantaneously. Both PMR chemical shift data and IR spectroscopic data point to the occurrence of a stronger antimony-β-diketonate interaction in trans-dichloro-β-diketonato-cis-diorganoantimony than in cis-dichloro-β-diketonato-trans-diorganoantimony compounds. This can be understood in terms of the hybridization of the antimony valence orbitals. The results are in line with the assumption that Sb---O bond rupture is the rate-determining step in β-diketonate ligand exchange.     

Hydrogenation of 2- tert -butylphenol over Ni catalyst

The hydrogenation of 2-tert-butylphenol was studied in regard to possibilities of influencing selectivity, namely the ratio ofcis- andtrans-isomers of 2-tert-butylcyclohexanol in the final reaction mixture. The hydrogenation reactions were carried out using the catalyst Ni/Al₂O₃. During the hydrogenations, a higher content of thecis-isomer was attained, when simultaneously the final reaction mixture contained 2-tert-butylcyclohexanone. The content of this intermediate, which primarily hydrogenated to thecis-isomer, increased with a decreased pressure and after the addition of acetic acid into the reaction mixture.     

The Course of the Catalytic Hydrogenation/Isomerization Reaction of Steroidal Ring B Olefins in the 13β- and 13α-Series

The course of the catalytic hydrogenation and isomerization (H₂/Raney-Ni/dioxane or H₂/Pd/C/EtOH) of Δ^5.7-, Δ⁷-, Δ⁸-, and Δ⁸⁽¹⁴⁾-steroid olefins was shown to depend strongly on the configuration at C(13). The known hydrogenation/isomerization of reactions of Δ^5.7-dienes in the 13β-series to Δ⁷-(H₂/Raney-Ni/dioxane) and Δ⁸⁽¹⁴⁾-olefins (H₂/Pd/C/EtOH) were also confirmed in the 3β, 19-epoxy-13β- and 3-Oxo-19-acetoxy-13β-steroid series (e.g. 32 → 35 → 37 , Scheme 3). On the other hand, in the corresponding 13α-steroid series the same reactions afforded the Δ⁷-. and the Δ⁸-olefins (mixture of products with H₂/Raney-Ni/dioxane; quantitatively the Δ⁸-compounds with H₂/Pd/C/EtOH; s. e.g. Scheme 3). A similar dependence on the C(13) configuration was observed in the allylic oxidation of these olefins with SeO₂ (Fieser's test, see Table), and in the acid catalyzed opening of the 7α, 8α-epoxides (e.g. 60 → 62 + 63 in the 13β-series, and 56 → 64 + 65 in the 13α-series, Scheme 8).     

Isomerism of copper(II) coordination compounds with hydroxamic acids

The structure of Cu^II complexes with hydroxamic acids Cu[R¹N(O)−(O)CR²]₂, where R¹=Ph, R²=Me; R¹=Me, R²=Ph, was studied by ESR spectroscopy. In toluene solutions and low-temperature glasses, the complexes exist as two forms, which were identified ascis-andtrans-isomers. The proportions of the isomers were determined. Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 4, pp. 726–729, April, 1999.     

Chromatographic Resolution of 7 of 8 Stereoisomers of Vitamin K1 on an Amylose Stationary Phase Using Supercritical Fluid Chromatography

In a previous report, it was shown that the trans-isomers of the 2′–3′ double bond on the side chain of vitamin K₁ (phylloquinone) represented 88.65 % of a specific sample, while the cis-isomer represented 11.35 %. However, the side chain contains 2 chiral centers, indicating there are 8 possible stereoisomers. Seven of these 8 stereoisomers were partially resolved in 20 min, on a RegisPack 4.6 × 250 mm, 5 μm column, using 5 % methanol in CO₂, at 2 mL/min, 30 °C, 150 bar. This is the first reported separation of these enantiomers by supercritical fluid chromatography, and, apparently, the first separation, by any technique, on a widely available commercial chiral stationary phase. The chiral separation produced one dominant peak, accounting for approximately 58 % of the total area, most likely due to 2′,3′-trans-4R,11R-philloquinone. Three other peaks each accounted for 9.7, 13.4, and 10.3 % of the total area, for a total of an additional ±33.4 %. These 4 peaks account for ≈91.4 % of the total area, in near agreement with the achiral findings for the separation of the trans-isomers. Three smaller, broad, poorly quantified peaks, collectively accounted for 8.1 % of the total area. Mass balance suggests these 3 small peaks are all cis-enantiomers, leaving approximately 3.2 % of the total area, representing the 4th cis-enantiomer, unaccounted for, and likely a co-elution with one of the 4 larger peaks.     

Transformations of pyridine and deuteropyridine under the action of trimethallylborane and alcohols. Synthesis oftrans- andcis-2,6-dimethallyl-1,2,3,6-tetrahydropyridines and theirN-derivatives

Reductivetrans-2,6-dimethallylation of pyridine and deuteropyridine with trimethallylborane in the presence of alcohols proceeds at room temperature,i.e., under substantially milder conditions than the analogous reaction with the participation of triallylborane.trans-2,6-Di(2-methylallyl)-1,2,3,6-tetrahydropyridine (3) was obtained in a yield of 87%. When heated with trimethallylborane (130–135°C, 2.5 h), compound3 underwent isomerization tocis-2,6-di(2-methylallyl)-1,2,3,6-tetrahydropyridine (4). Hydrogenation oftrans- (3) andcis-isomers (4) yieldedtrans- andcis-2,6-diisobutylpiperidines, respectively. The heterocycles obtained wereN-functionalized by reactions with MeI, PhCH₂Cl, ethylene oxide, and perfluoropropyloxirane. The stereochemistry of thecis- andtrans-isomers (3 and4) was established based on the NMR spectra of theirN,N-dimethyl salts and the products of the reaction with ethylene oxide.trans-2,6-Dimethallyl-2,3,4,5,6-pentadeutero-1,2,3,6-tetrahydropyridine and a number of its derivatives were prepared from the complex of trimethallylborane with C₅D₅N. A probable mechanism of the reductivetrans-2,6-diallylation of pyridines with allylboranes in the presence of alcohols is discussed. This article is dedicated to Prof. W. Siebert (Heidelberg) on the occasion of his 60th birthday. Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 7, pp. 1361–1370, July, 1997.     

Preparation of Bicyclo[3.3.0]octane-2,8-dione- and Declain-1,8-dione-Derivatives

Alkylation of bicyclo[3.3.0]octane-2,8-dione ( 1 ), which is prepared by a modification of the procedure described in the literature, gives the methyl- and propynyl-derivatives 6 and 7 (Scheme 1). In addition to the method described previously (Scheme 2), 9-methyl-cis-decalin-1,8-dione 9 is obtainable stereoselectively either by cyclization of keto-acid 16 , or by aldol cyclization of keto-aldehyde 26 and oxydation of the resulting alcohols 24 and 25 (Scheme 4). The β-keto-alcohols 24 and 25 undergo a base-catalyzed isomerization; the trans-decalin isomers 27 and 28 are not detected in this equilibrium mixture (Schemes 4 and 5)l. Monoreduction of cis-dione 9 gives the endo-alcohol 25 , while 27 is the favored product of the reductin of trans-dione 10 (Scheme 4). Optically pure (+)- 25 can be prepared from (9S,10R)-monoacetal 29 (Scheme 5).