Chemical composition of the pods of Albizia polyphylla

In this study, we report for the first time the presence of alkaloids belonging to β-carboline type in the pods of the endemic Albizia polyphylla from Madagascar. Three major alkaloids were isolated and structurally identified as: 1-methyl-β-carboline, (+)-(R)-1-methyl-1,2,3,4-tetrahydro-β-carboline and (–)-(S)-1,2-dimethyl-1,2,3,4-tetrahydro-β-carboline.     

Studies on the Alkaloids of Formosan Lauraceous Plants XVIII Alkaloids of Neolitsea Buisanensis Yamamoto Et Kamikoti and Neolitsea Aurata (Hay.) Koidz

Two alkaloids, laurolitsine (V) and litsericine (VII), were isolated from the woods of Neolitsea buisanersis. Six alkaloids were isolated from the woods of Neolitsea aurata and five of them were laurolitsine (V), litsericine (VII), N–methyllitsericine (VIII), (+)–anonaine (IX), and (–)-roemerine (X) (Table I).     

Enantioselective Synthesis of 3- Azabicyclo[4.3.0]nonane Alkaloids

The stereospecific synthesis of the monoterpene alkaloids (?)-α-skytanthine ((?)- 2 ), (?)-N -demethyle-δ-sky-tanthine((?)- 7 ), and (+)-epidihydrotecomanine (+)- 4 was achieved from a common intermediate 22 , which in turn was obtained from (1R,4S,1′S)-2-(1′-phenylethyl)-2-azabicyclo[2.2.1]hept-5-ene (10) ,via a ketene aza-Claisen rearrangement. The piperidine derivative (+)- 31 , formally the aza-analogue of (+)-isoiridomyrmecin, was also obtained from the same intermediate 22 .     

Enantioselective Catalysis Coupled with Stereodivergent Cyclization Strategies Enables Rapid Syntheses of (+)‐Limaspermidine and (+)‐Kopsihainanine A

Enantioselective Pd‐catalyzed allylic alkylations of dihydropyrido[1,2‐a ]indolone (DHPI) substrates were used to construct the C20‐quaternary stereocenters of multiple monoterpene indole alkaloids. Stereodivergent Pictet–Spengler and Bischler–Napieralski cyclization/reduction cascades furnish the cis‐ and trans ‐fused azadecalin subunits present in Aspidosperma and Kopsia alkaloids, respectively, en route to highly efficient syntheses of (+)‐limaspermidine and (+)‐kopsihainanine A.     

Macrocyclic Spermine Alkaloids from Verbascum: The (E/Z)-Isomeric Pairs (−)-(S)-Verbasitrine/(−)-(S)-Isoverbasitrine and (+)-(S)-Verbametrine/(+)-(S)-Isoverbametrine: Isolation,Structure Elucidation,and Synthesis

The isolation and structure elucidation of the 17-membered macrocyclic spermine alkaloids (−)-(S)-verbasitrine ( 2 ), (−)-(S)-isoverbasitrine ( 4 ), (+)-(S)-verbametrine ( 6 ), and (+)-(S)-isoverbametrine ( 8 ) is presented. The synthesis of their racemates is described.     

Enantioselective syntheses of 2,5-disubstituted pyrrolidines based on iridium-catalyzed allylic aminations--total syntheses of alkaloids from amphibian skins

A broadly applicable route to trans‐2,5‐disubstituted pyrrolidines has been developed. Key steps are an asymmetric iridium‐catalyzed allylic amination, a Suzuki–Miyaura coupling, and an intramolecular aza‐Michael addition. Enantiomeric excesses in the range of 93–99 % ee have been achieved. Total syntheses of the alkaloids (?)‐ 225 C , (+)‐ and (?)‐ 223 H (xenovenine), (+)‐ 223 AB , (+)‐ 195 B , and (+)‐ 223 R have been carried out as applications.     

Über Alkaloide aus Laurelia novae-zelandiae A. CUNN. 5. Mitteilung über natürliche und synthetische Isochinolinderivate

From an extract of Laurelia novae-zelandiae A. CUNN . the aporphine alkaloids (?)-pukateine (I), (?)-pukateine methyl ether (II), (?)-roemerine (IV), (?)-mecambroline (V), (+)-boldine (VII), (+)-isoboldine (VIII), (+)-laurolitsine (IX), and the proaporphine alkaloid (+)-stepharine (X) were isolated. Compounds II and V were up to now not described as natural alkaloids. These and the alkaloids IV, VII, VIII, IX and X are new for L. novae-zelandiae.     

粪箕笃中两个新颖的含硝基莲花氏烷型生物碱

Two unusual nitro-substituted hasubanan-type alkaloids, stephalonines J （1） and K （2）, together with ten known alkaloids, protostephanine, dehydrostephanine, （-）-stephanine, （-）-isolaureline, R-roemeroline, （＋）-pronuciferine, （ ＋）-stephafine, （ ＋ ）-N-acetylstephafine, （ ＋ ）-lirioferine, and （ ＋ ）-norlirioferine, were isolated from the whole plant of Stephania longa. Their structures were characterized mainly by spectroscopic methods including IR, MS, and NMR experiments, and the structures of 1 and 2 were further confirmed through chemical correlations with the known alkaloids stephalonines A （1a） and B （2a）, respectively.     

«Alkaloide» in tierischem und menschlichem Gewebe. 6. Mitteilung [1] [2]. Synthese und absolute Konfiguration chiraler 2, 3, 10, 11 - Tetrahydroxy-8-methyl-berbine [3]

Synthesis and absolute configuration of chiral 2, 3, 10, 11-tetrahydroxy-8-methylberbines [3] . The synthesis and absolute configuration of the four optically active berbines Xa, b and XIa, b are described. These compounds consitute potential ‘alkaloids’ obtained by condensation of either R-(+) or S-(?)-norlaudanosoline (THP, III) with acetaldehyde, a major metabolite of ethanol.     

Synthesis of Aristotelia-Type Alkaloids. Part XIII. Total syntheses of (+)-makonine, (+)-aristotelinone,and (+)-11,12-didehydroaristoteline

The oxidative transformation of synthetic (+)-aristoteline ((+)- 6 ) into other metabolites which had been isolated from Aristotelia species was investigated. Thus, treatment of (+)- 6 with I₂ as the single oxidant furnished the naturally occurring indole alkaloids (+)-makonine ((+)- 9 ),(+)-aristotelinone ((+)- 11 ), or (+)-11, 12-didehydroaristoteline ((+)- 7 ) in good yields, the selectivity of the oxidation process depending on the chosen reaction conditions.     

Palladium-catalyzed asymmetric allylic substitution of 2-arylcyclohexenol derivatives: asymmetric total syntheses of (+)-crinamine, (-)-haemanthidine, and (+)-pretazettine

Much interest has been shown in Amaryllidaceae alkaloids as synthetic targets due to their wide range of biological activities. Over 100 alkaloids have been isolated from members of the Amaryllidaceae family; most of them can be classified into eight skeletally homogeneous groups. We have succeeded in the first asymmetric total syntheses of the crinane-type alkaloids (+)-crinamine (1), (-)-haemanthidine (2), and (+)-pretazettine (3). The starting cyclohexenylamine 14 was obtained from allyl phosphonate 11c by palladium-catalyzed asymmetric amination in 82% yield and with 74% ee. The product was recrystallized from MeOH. Interestingly, (-)-14 with 99% ee was obtained from the mother liquor (74% recovery). Intramolecular carbonyl-ene reaction of (-)-10 proceeds in a highly stereoselective manner to give hexahydroindole derivative 9 as the sole product. In the Lewis-acid-catalyzed carbonyl-ene reaction, an interesting rearrangement product, 20, was isolated in high yield. From 9, (+)-crinamine was synthesized. Thus, the asymmetric total synthesis of (+)-crinamine was achieved in 10 steps from 11c, and the overall yield is 19%. The total synthesis of (-)-haemanthidine was also achieved from 9 by a short sequence of steps.     

Alkaloid studies. VI. lithium aluminum hydride reduction of apoyohimbine and the synthesis of 3,4,5,6-tetradehydroyohimbane-16-methanols

Catalytic reduction of apoyohimbine ( 1 ), prepared from yohimbine and thionyl chloride in pyridine, gives methyl yohimbane-16α-carboxylate ( 2 ) after equilibration with methoxide. LAH reduction of 2 or β-yohimbine O-tosylate ( 3 ) gives yohimbane-16α-methanol ( 4a ). LAH reduction of 1 affords yohimbane-16α-carboxaldehyde ( 5 ), yohimb-16-ene-16-methanol ( 6a ) and yohimbane-16β-methanol ( 7a ). Structural assignments 6a and 7a are confirmed by mass spectral measurements. Pmr spectra of 4a, 6a and 7a and their O-acetates 4b, 6b and 7b are discussed. LAH reduction of apo-α-yohimbine ( 8 ) affords alloyohimb-16-ene-16-methanol ( 9 ). Dehydrogenation of 4a with palladium black and maleic acid gives 3,5,4,5,6-tetradehydroyohimbane-16α-methanol ( 10 ) iodide, and 7a gives 3,4,5,6-tetradehydroyohimbane-16β-methanol ( 11 ) iodide and picrate. Properties of 10 and 11 differ from those of melinonine E.     

Syntheses of (+)- and (–)-Methyl 8-Epinonactate and (+)- and (–)-Methyl Nonactate

In four synthetic steps, (+)- and (–)-methyl 8-epinonactate ((+)- and (–)− 4 ) have been derived from (+)- and (–)-7-oxabicyclo[2.2.1]heptan-2-one ((+)- and (–)− 9 ), respectively. The (+)- and (–)-methyl nonactate ((+)- and (–)− 3 ) were obtained from (+)- and (–)− 4 , respectively, by Mitsunobu displacement reactions. Optical resolution of (±)− 9 via chromatographic separation of the corresponding N-methyl-S-alkyl-S-phenylsulfoximides 24 and 25 yielded the starting materials (+)- and (–)− 9 , respectively.     

Cheritamine,A New N-Fatty Acyl Tryptamine and Other Constituents from the Stems of Annona cherimola

A new N-fatty acyl tryptamine, cheritamine ( 30 ), along with thirty-two compounds including nineteen benzenoids, p-hydroxybenzadehyde ( 1 ), p-hydroxybenzoic acid ( 2 ), methylparabene ( 3 ), 3-chlorobenzoic acid ( 4 ), vanillin ( 5 ), isovanillin ( 6 ), vanillic acid ( 7 ), isovanillic acid ( 8 ), methyl vanillate ( 9 ), methyl isovanillate ( 10 ), syringaldehyde ( 11 ), syringic acid ( 12 ), 3,4,5-trimethoxybenzoic acid ( 13 ), trans-methyl p-coumarate ( 14 ), ferulic acid ( 15 ), p-dihydrocoumaric acid ( 16 ), 3-(4-hydroxy-3,5-dimethoxyphenyl)-1,2-propanediol ( 17 ), 3,4,5 -trimethoxyphenyl-β-D-glucopyranoside ( 18 ) and thalictoside ( 19 ); one p-quinone, 2,6-dimethoxy-p-quinone ( 20 ); one purine, uridine ( 21 ); eight alkaloids, nicotinic acid ( 22 ), thalifoline ( 23 ), doryphornine ( 24 ), (–)-norstephalagine ( 25 ), (-)-romucosine ( 26 ), (+)-pronuciferine ( 27 ), (+)-norisocorydine ( 28 ) and oxoasimilobine (29) and three steroids, β-sitosterol-D-glucoside ( 31 ), stigmasterol-D-glucoside ( 32 ) and 6′-(β-sitosteryl-3-O-β-glucopyranosidyl)hexadecanoate ( 33 ), are isolated from the stems of Annona cherimola. These compounds were characterized and identified by physical and spectral evidence.     

Conformational Studies of Marine Polyhalogenated α-Chamigrenes Using Temperature-dependent NMR spectra inverted-chair and twist-boat cyclohexane moieties in the presence of an axial halogen atom at C(8)

α-Chamigren-3-one (+) -8 bearing an axial CI-atom at C(8) exists as a largely dominant conformer with Me—C(5) at the envelope-shaped enone ring pointing away from CI_ax?C(8) at the cyclohexane ring (= B) in the ‘normal’ chair conformation, as shown by ¹H-NMR. In contrast, the α-chamigren-3-ols (+) -9 and (+) -10 , obtained from hydride reduction of (+) -8 , show a temperature-dependent equilibrium of conformers where the major conformers have ring B in the inverted-chair (and twist-boat for (+) -9 ) conformation to avoid repulsions between Me?C(5) and CI_ax–C(8) (Scheme 1). This is in agreement with the conformation of the epoxidation product (+) -12 of (+) -9 where Me–C(5) is pushed away from CI_ax–C(8) in a ring-B chair similar to that of (+) -8 (Scheme 2). Introduction of a pseudoequatorial Br-atom at C(2) of (+) -8 , as in enone (+) -15 (Scheme 3), does not affect the conformation; but a pseudoaxial Br? C(2) experiences repulsive interactions with H_eq–C(7), as shown by the ¹H-NMR data of the isomeric enone (+) -16 where the ‘normal’-chair conformer Cβ -16 is in an equilibrium with the inverted chair conformer ICβ -16 (Scheme 3). These results and the accompanying paper allow a unifying view on the conformational behavior of marine polyhalogenated α-chamigrenes. This view is supported by the acid-induced isomerization of α-chamigrene (+) -9 (inverted chair) to β-chamigrene (+) -17 (‘normal’ chair; Scheme 4), the driving force being the lesser space requirement of CH₂?C(5) than of Me–C(5). This explains why β-chamigrenes are so common in nature.     

The Constituents from the Stems of Annona cherimola

Thirty-five compounds including twenty-one alkaloids, lysicamine ( 1 ), liriodenine ( 2 ), atherospermidine ( 3 ), oxoxylopine ( 4 ), oxoanolobine ( 5 ), oxoglaucine ( 6 ), (-)-anonaine ( 7 ), (-)-asimilobine ( 8 ), (-)-xylopine ( 9 ), (-)-anolobine ( 10 ), (-)-norisocorydine ( 11 ), (+)-laurotetanine ( 12 ), (+)-isocorydine ( 13 ), (-)-N-methylasimilobine ( 14 ), (+)-N-methyllaurotetanine ( 15 ), (-)-norushinsunine ( 16 ), (-)-ushinsunine ( 17 ), (-)-N-formylanonaine ( 18 ), (+)-stepharine ( 19 ), (+)-orentaline ( 20 ), and (-)-kikemanine ( 21 ); four kauranes, ent-kaur-16-en-19-oic acid ( 22 ), 16β-hydroxy-17-acetoxy-ent-kauran-19-al ( 23 ), 17-acetoxy-16β-ent-kauran-19-oic acid ( 24 ), and 16β-hydroxy-17-acetoxy-ent-kauran-19-oic acid ( 25 ); two amides, N-trans-femloyltyramine ( 26 ), and N-trans-caffeoyltyramine ( 27 ); one purine, adenosine ( 28 ); one lactam amide, squamolone ( 29 ); and six steroids, β-sitosterol ( 30 ), stigmasterol ( 31 ), β-sitostenone ( 32 ), stigmasta-4,22-dien-3-one ( 33 ), 6β-hydroxy-β-sitosterone ( 34 ), and 6β-hydroxystigmasterone ( 35 ) are isolated from the stems of Annona cherimola. These compounds were characterized and identified by physical and spectral evidence. Among them, (-)-norisocorydine (11) was elucidated as a new enantiomer with a levorotary configuration, which is isolated for the first time.     

Über die Synthese der Pilocarpus-Alkaloide Isopilosin und Pilocarpin,sowie die absolute Konfiguration des (+)-Isopilosins

A novel synthesis for rac-pilosinine ( 6 rac) and transformation of (+)-pilosinine ( 6 ) into the pilocarpus alkaloids (+)-isopilosine ( 9 ) and (+)-pilocarpine ( 18 ) are described. By correlation via 5 with 18 the absolute configuration of (+)-isopilosine ( 9 ) is established.     

Synthesis of (+)-(S)-Streptenol A and Biomimetic Synthesis of (2R,4S)- and (2S,4S)-2-(Pent-3-enyl)piperidin-4-ol

(+)-(S)-Streptenol A is synthesized by coupling a 1,3-dithiane with an optically pure epoxide. The absolute configuration of (+)-(S)-streptenol A is thereby correlated with that of (S)-malic acid. Stereoselective reduction of an oxime that could easily be prepared from streptenol A gave the (3S,5R)- and (3S,5S)-aminostreptenols, and after cyclization, configurationally pure 2,4-functionalized piperidine alkaloids.     

Alcaloides indoliques—CV: Préparation de dérives du yohimbane à partir de la corynanthéine. Réaction de prins intramoléculaire

Three yohimbane derivatives, 17,19β-dihydroxy yohimbane 2a and 2b and 19β-chloro-β-yohimbine 3, have been prepared starting from corynantheine. The reaction involved is a Prins cyclisation reaction, the mechanism of which is compared to the biosynthetic route proposed for yohimbane-type indole alkaloids.     

Synthetic approach to natural products by Claisen rearrangement of glyceraldehyde derivatives

For the purpose of organic syntheses of some corynanthe-type indole alkaloids, sesquiterpenes, and steroids, optically active intermediates cyclopentanone 3-allylalcohol, α-methylene-γ-butylo lactones andtrans-hydrindanone-propionic acid, were synthesized from (R)- and (S)-isopropylideneglyceraldehyde derived fromD-mannitol andLascorbic acid, respectively, utilizing Claisen rearrangement as a key reaction. Actually total syntheses of natural alkaloids, (-)-antirhine, (+)-dihydroantirhine and (-) dihydrocorynantheol were accomplished.