A Total Synthesis of (±)- Aphidicolin: Regio- and stereoselective conversion of 3α,18-Di-O-benzyl-17-nor-14-aphidicolen-16-one into (±)-aphidicolin

A regio- and steroselective conversion of the totally synthetic 3α, 18-di-O-benzyl-17-nor-14-aphidicolen-16-one (5), into (±)-aphidicolin 1 , by hydroxylation of the 2-methylidenebicyclo[3.2.1] oct-3-ene derivative 6 is described. Compound 5 was a key intermediate in our previously described total synthesis of 2 , which represented a formal synthesis of 1 .     

Formale Totalsynthese von (±)-Isocomen durch Anwendung der α-Alkinon-Cyclisierung

Formal Total Synthesis of (±)-Isocomen by Application of the α-Alkinon Cyclization A total synthesis of the racemic form of the sesquiterpene isocomene ( A ) was accomplished by application of the cyclopentenone anellation B→D (Scheme 1) which includes the α-alkynone cyclization C→D , a gas-phase flow thermolytic process. Starting with the known product 2 (Scheme 3) of the anellation B→D , the elaboration of ring C of A proceeded in 9 steps to the α-alkynone 16 (Scheme 5) which was cyclized at 540° selectively to give the angularly fused triquinane 4 (77%). A two-step procedure then led to 5 (Scheme 6), a last but one intermediate in a known total synthesis of (±)- A . The conversion of 16 to 4 also demonstrated the compatibility of an acetoxy function with the anellation sequence B→D .     

Synthesis and Properties of 1, 1-Dihalogenocycloprop[b]Anthracenes

The synthesis of 1, 1-difluoro-1H-cycloprop[b]anthracene ( 3 ) is described. The key step of the synthesis is the cycloaddition of 1,2-dichloro-3,3-difluorocyclo-propene ( 6 ) to 2,3-dimethylidene-1,2,3,4-tetrahydronaphthalene ( 5 ). The ¹³C-NMR. spectrum of 3 is assigned on the grounds of C,F-coupling constants, selective H-decoupling and the resulting residual C,H-coupling. The 1, 1-dichloro derivative 4 was synthesized by the same route, but could not be isolated pure. Experiments for the reduction to 1H-cycloprop[b]anthracene ( 2 ) and for the ionization of 3 or 4 to the cation 16 failed.     

An Efficient Stereoselective Synthesis of (±)-Sweroside and (±)-secologanin aglucone O-methyl ethers. Preliminary communication

A seven-step stereoselective synthesis of (±)-sweroside aglucone O-methyl ether ( 16a ) was achieved in 27% overall yield from 1, 4-cyclohexadiene ( 4 ) and methyl diformylacetate ( 5 ). Secologanin aglucone O-methyl ether ( 18a ) was then formed from 16a in 90% overall yield by a straightforward process. The key step in the synthesis was a [2+2]-enone-photoannelation of 4 and 5 to form the key intermediate 6 which possessed the desired cis-fused ring configuration, and all the caron atoms needed to complete the synthesis of 16a and 18a .     

Diazoaldehyde Chemistry. Part 1. Transdiazotization of Acylacetaldehydes in Neutral-to-Acidic Medium. A Direct Approach to the Synthesis of α-Diazo-β-oxoaldehydes

First ever non-deformylating transdiazotization of acylacetaldehydes was achieved: the reactions of 2-azido-l-ethylpyridinium tetrafluoroborate ( 4 ) with acylacetaldehydes 3 proceeded partially without deformylation to yield 16 new α-diazo-β-oxoaldehydes 1 along with diazomethyl ketones 2 , especially in the presence of NaOAc (Scheme 1, Tables 1 and 2). The product distribution was substituent-dependent and could be correlated quantitatively. This new diazotization reaction appears as an alternative, direct, and more general method for the synthesis of these diazooxoaldehydes. α-Oxocycloalkanecarbaldehydes 5 gave only traces (if any) of α-diazocycloalkanones 7 , and rearrangement products 6 were isolated (Scheme 2). Mechanisms of the reactions are discussed (Schemes 4 and 5).     

Total Synthesis of (±)-3-Deoxy-7,8-dihydromorphine, (±)-4-Methoxy-N-methylmorphinan-6-one and 2,4-Dioxygenated (±)-Congeners

A total synthesis of racemic 3-deoxy-7,8-dihydromorphine ((±)- 2 ) and 4-me-thoxy-ALmethylmorphinan-6-one ((±)- 3 ) is described. The key intermediate was 2,4-dihydroxy-N-formylmorphinan-6-one (11) , obtained from 3,5-dibenzyloxy-phenylacetic acid (4) in 41.8% overall yield. Bromination of 11 , and treatment with aqueous N_aOH-solution afforded, after N-deblocking and reductive N-methylation with concomitant removal of the aromatic bounded Br-atom, the morphinanone 14. Elimination of the HO–C(2) group in 14 was accomplished by hydrogenolysis of its N-phenyltetrazolyl ether 15 , to give 3-deoxy-6,0-didehydro-7,8-dihydromorphine (16). Reduction of 16 with L-Selectride at low temperature provided (±)- 2 in high yield. The ether 15 directly afforded, under more vigorous reduction conditions, 4-hydroxy-N-methylmorphinan-6-one (17). and after O-methylation of 17 , the methyl ether (±)- 3 was obtained. A (1:l)-mixture of 4-hydroxy-2-methoxy-N-methylmor-phinan-6-one (28) and its 2-hydroxy-4-methoxy isomer 30 svere obtained by Grewe-cyclization of a mono-methoxylated aromatic precursor similar to that which afforded 11. The 2,4-dioxygenated N-methylmorphinan-6-ones 29 , 31 and 38 were also prepared and characterized.     

Synthesis of 3-methyl-[1,2,4] -triazepino[6,5,4-jk] carbazol-4(3H)one

The title compound ( 14 ), a representative of a novel ring system, was prepared from 9H-carbazole-1-carboxylic acid 1-methylhydrazide ( 7 ) and triethyl orthoformate. Attempted cyclization of 7 with triethyl orthoacetate led only to 9H-carbazole-l-carboxylic acid 2-(l-ethoxyethylidene)-l-methylhydrazide ( 16 ). Treatment of 16 with trifluoroacetic acid gave 9H-carbazole- 1 -carboxylic acid ( 12 ). A postulated mechanism for this transformation was supported by studies with model compounds. A new synthesis of 1 -benzoyl-2-methylhydrazine ( 24 ), using 1-acetyl-1-methylhydrazine ( 22 ) as a synthon, is described.     

Synthesis of (±)-Pyrenolide B

In the synthesis of the title compound 12 , the important intermediate 7 was obtained in good yield from the easily available ethyl 5, 5-ethylenedioxy-2-oxocyclohexane-1-carboxylate ( 1 ) via ring enlargement of the bicyclic enol ether 5 (Scheme). Its reduction (NaBH₄ in EtOH) and subsequent protection with (t-Bu)Me₂Si resulted in the highly functionalized ten-membered lactone 9 . Introduction of the (Z)-configurated double bond, followed by deprotection and elimination of H₂O, gave (±)-pyrenolide B ( 12 ) in 16% overall yield.     

Synthesis of 1-substituted 3-nitroquinolin-4(1H)-ones

A versatile synthetic method for preparing 1-substituted 3-nitroquinolin-4(1H)-ones from corresponding 2-fluoro-α-nitroacetophenones is demonstrated by the synthesis of 6,7-difluoro derivatives 7a-c . The method involves sequential treatment of the starting nitroacetophenone with triethyl orthoformate and the appropriate amine, followed by a nucleophilic cyclization reaction under mild conditions. The C-7 fluorine atom of 7 can be displaced by cyclic amines. Substituted 6-fluoro-7-(4-methyl-1-piperazinyl)-3-nitroquinolin-4(1H)-ones 8a-c were prepared in this way.     

Synthesis and Structure of 1-tert-Butyl-3-R-tetrazolium Salts

An effective method was developed for the synthesis of 1,3-disubstituted tetrazolium salts by the quaternization of 2-monosubstituted tetrazoles, including functionally substituted compounds, with tert-butanol in 72% perchloric acid. An X-ray diffraction investigation of examples of this series of salts - 1-tert-butyl-3-(1-methylvinyl)- and 1,3-di-tert-butyltetrazolium perchlorates - was carried out.     

Synthesis and reactions of 2-amino-7, 8-dimethoxy-1h-3-benzazepines. Competitive formation of 2-amino-1h-3-benzazepines vs. 2-benzylimidazoles

A short synthesis of 2-amino-7, 8-dimethoxy-1H-3-benzazepine ( 1a ) from 3, 4-dimethoxyphenylacetonitrile ( 8a ) is reported. The synthesis of several other 2-amino-1H-3-benzazepines 1 is also discussed. Conditions which favor the formation of 1 versus the formation of the isomeric 2-benzylimidazoles 11 are evaluated. Several reactions of 1a are also described.     

Synthesis of 3H[1,2]diazepino[5,6-b]indole and 3H[1,2]diazepino[4,5-b]indole derivatives

The synthesis of two new derivatives of 3H[1,2]diazepino[5,6-b]indole, 5 and 11 , and one new derivative of 3H[1,2]diazepino[4,5-b]indole, 16 , are described. Compound 5 was obtained by the reaction of methyl 2-(3-methoxycarbonyl-1-methylindole)acetate 2 , with hydrazine. Compound 11 was obtained in two ways from ethyl 2-(1-methylindole)acetate ( 8 ) by formylation and reaction with hydrazine. Compound 16 was obtained treating 3-(2-ethoxycarbonylindole)acetonitrile ( 14 ) with hydrazine.     

Synthesis of 6-substituted 3-cyano-5-nitropyridine-2(1H)-thiones

The reactions of 1-substituted 2-nitro-3-phenylaminoprop-2-en-1-ones with cyanothioacetamide afforded the corresponding 6-substituted 3-cyano-5-nitropyridine-2(1H)-thiones, which were used for the synthesis of 6-substituted 3-cyano-2-methylthio-5-nitropyridines and 7-substituted 4-hydroxy-8-nitropyrido[2",3":4,5]thieno[2,3-b]pyridin-2(1H)-ones.     

Synthesis of (E)-5-oxo-2-(3-α and 3β-hydroxy-1-octenyl)-1-(4-N-pyrrolidine-2-butynyl)pyrrolidine

The synthesis of an oxotremorine analog, (E-5-oxo-2-(3α and 3β-hydroxy-1-octenyl)-1-(4-N-pyrrolidino-2-butynyl)pyrrolidine, is reported.     

Novel Synthesis of 1-(1,2,3,5,6,7-Hexahydro- s-indacen-4-yl)-3-[4-(1-hydroxy-1-methyl-ethyl)-furan-2-sulfonyl]urea,an Anti-inflammatory Agent

Abstract

A novel synthesis of the anti-inflammatory agent 1-(1,2,3,5,6,7- hexahydro-s-indacen-4-yl)-3-[4-(1-hydroxy-1-methyl-ethyl)-furan-2-sulfonyl] urea 1 is described. Sulfonamide 5 was prepared starting from ethyl 3-furoate 2. Key steps were a one-pot sulfonylation with chlorosulfonic acid in methylene chloride followed by pyridinium salt formation and reaction with phosphorus pentachloride to provide ethyl 2-(chlorosulfonyl)-4-furoate 7. This sulfonyl chloride was treated with ammonium bicarbonate to form sulfonamide 8, followed by treatment with excess methyl magnesium chloride to provide 4-(1-hydroxy-1-methyl-ethyl)-furan-2-sulfonamide 5. 4-Isocyanato-1,2,3,5,6,7-hexahydro-s-indacene 16 was prepared from indan in five steps. The formation of the desired sulfonyl urea was carried out both with the isolated isocyanate 16 and via an in situ method.     

Recent Applications of α-Metalated Isocyanides in Organic Synthesis

Being both nucleophilic and electrophilic, α-metalated isocyanides can add to polar double bonds, forming heterocycles. They are also synthons for α-metalated primary amines. This article describes recent or improved procedures for their use in organic synthesis: (1) In heterocyclic syntheses to give 2-oxazolines, 2-imidazolines, 2-thiazolines, oxazoles and oligooxazoles, thiazoles, triazoles, imidazolinones, pyrroles, 5,6-dihydro-1,3-oxazines and -thiazines, and (via cycloaddition with nitrones) 2-imidazolidinones. (2) In the field of formylaminomethylenation, for example transformation of estrone methyl ether and a keto sugar into the corresponding α-formylaminoacrylic esters, and the conversion of aldehydes and ketones by 3- and 4-pyridyl-methyl isocyanides into N-(1-pyridyl-1-alkenyl)formamides and their hydrolysis to 3- and 4-acylpyridines. (3) In connection with the use of α-metalated isocyanides as synthons for α-metalated primary amines, the author demonstrates how they may be used for preparation of 1,2- and 1,3-amino alcohols, 1,2-diamines, 2,3-diaminoalkanoic acids and for synthesis of higher amino acids starting from simple amino acids.     

BiBr3-Mediated Intramolecular Aza-Prins Cyclization of Aza-Achmatowicz Rearrangement Products: Asymmetric Total Synthesis of Suaveoline and Sarpagine Alkaloids

An intramolecular aza-Prins cyclization of aza-Achmatowicz rearrangement products was developed in which bismuth tribromide (BiBr₃) plays a dual role as an efficient Lewis acid and source of the bromide nucleophile. This approach enables the facile construction of highly functionalized 9-azabicyclo[3.3.1]nonanes (9-ABNs), which are valuable synthetic building blocks and a powerful platform for the synthesis of a variety of alkaloid natural products and drug molecules. Suitable substrates for the aza-Prins cyclization include 1,1-disubstituted alkenes, 1,2-disubstituted alkenes, alkynes, and allenes, with good to excellent yields observed. Finally, we showcase the application of this new approach to the enantioselective total synthesis of six indole alkaloids: (−)-suaveoline ( 1 ), (−)-norsuaveoline ( 2 ), (−)-macrophylline ( 3 ), (+)-normacusine B ( 4 ), (+)-N_a-methyl-16-epipericyclivine ( 5 ) and (+)-affinisine ( 6 ) in a total of 9–14 steps. This study significantly expands the synthetic utility of the aza-Achmatowicz rearrangement, and the strategy (aza-Achmatowicz/aza-Prins) is expected to be applicable to the total synthesis of other members of the big family of macroline and sarpagine indole alkaloids.     

Total Synthesis of (±)‐Aspidophylline A

A total synthesis of aspidophylline A, a pentacyclic akuammiline‐type monoterpene indole alkaloid, is described. The synthesis features: 1) rapid access to a fully functionalized dihydrocarbazole through the desymmetrization of readily available 2‐allyl‐2‐(o‐nitrophenyl)cyclohexane‐1,3‐dione; 2) an intramolecular azidoalkoxylation of an enecarbamate to install both the furoindoline ring and the azido functionality; and 3) an intramolecular Michael addition for the construction of the 2‐azabicyclo[3.3.1]nonane ring system.     

Total Synthesis of Dimethyl Glolosiphone A via α-Carbonyl Radical Spiro-Cyclization

A general approach toward spiro[4.4]nonane structure based on the α-carbonyl radical cyclization has been developed. Efficient total synthesis of dimethyl gloiosiphone A ( 2 ) was achieved. Thus, alkylation of the anion of dimethylhydrazone of cyclopentanone with 5-iodopent-1-yne followed by hydrolysis gave ketone 4 . Iodination of 4 via its TMS-enol ether yielded iodo ketone 7 . Radical spiro-cyclization of 7 gave spiro ketone 10 . Iodination of 10 afford iodo spiro ketone 23 . Oxidation and iodination of 23 gave compound 24 . Methylation of 24 furnished methoxy iodo enone 25 . Substitution of iodide in 25 with methoxide produced dimethoxy enone 26 . Allylic oxidation of 26 gave diketone 27 . Treatment of 27 with OsO₄ and N-methylmorpholine N-oxide gave dihydroxy ketone 28 . Methylation of the primary alcohol group in 28 afforded dimethyl gloiosiphone A ( 2 ).     

Total Synthesis of Actinorhodin

The enantioselective total synthesis of actinorhodin ( 1 ) is described. The synthesis features 1) dual benzyne reactions en route to the monomer, 2) the trans‐selective installation of the side chain, and 3) a regioselective oxidative dimerization.