Protecting group-free total synthesis of (-)-lannotinidine B

The first total synthesis of (-)-lannotinidine B, a unique tetracyclic constitutent of Lycopodium annotinum, has been accomplished in 10 steps with 23% overall yield. The completed short and efficient synthesis is characterized with three highly chemo- and/or stereoselective reductive-amination steps to furnish the desired trans-fused 6/6 bicycle and the aza seven-membered ring system, and a direct intramolecular acyloin condensation to deliver the cyclopentanone moiety, as well as successful application of a protecting group-free strategy and an optimal redox order.     

Synthesis,stability and bonding situation of tris-, bis- and mono[9-(azuleno[1,2-b]thienyl)]methyl cations

Stable tris-, bis- and mono[9-(azuleno[1,2-b]thienyl)]methyl cations (7a, 8a and 9a) and their derivatives, with a 6-isopropyl substituent on each azuleno[1,2-b]thiophene ring (7b, 8b and 9b) were prepared by the hydride abstraction reaction of the corresponding methane derivatives. The bonding situation of these compounds including the methane derivatives was examined by analysis of the 3J(H,H) values for the seven-membered ring from the 1H NMR spectra. The methane derivatives exhibited a significant alternating pattern in the 3J(H,H) values, which indicated that the pi-system of the azulene core is perturbed by the fused thiophene ring, showing a tendency towards a localized heptafulvene substructure. The 3J(H,H) values of 7b and 8b in the seven-membered ring revealed that the alternating C-C bond lengths in the azulene core still existed. The cations 9a and 9b, which exhibited nearly equal 3J(H,H) values in the seven-membered ring, exhibit the development of a delocalized tropylium substructure in the azulene core. X-ray crystal analysis of 6-isopropylazuleno[1,2-b]thiophene revealed substantial bond-length alternation in the seven-membered ring. Significant bond-length equalization in the seven-membered ring was also confirmed by the X-ray crystal analysis of 9b. The stability of these carbocations was examined by measurement of the pKR+ values and the redox potentials, which revealed that the bond-length alternation in the azulene core does not significantly affect the stability of the carbocations.     

Gold(I)-catalyzed cycloisomerization of 1,7- and 1,8-enynes: application to the synthesis of a new allocolchicinoid

Gold(I)-catalyzed cycloisomerization of 1,7- and 1,8-enyne propargylic acetates afforded cyclopropyl derivatives containing seven- and eight-membered rings, respectively. This reaction was used for the synthesis of a new allocolchicinoid having a cyclopropane ring fused to the B seven-membered ring at the C6-C7 positions.     

Biomimetic synthesis of (+/-)-galanthamine and asymmetric synthesis of (-)-galanthamine using remote asymmetric induction

(+/-)-Galanthamine (1) was synthesized in excellent yield by applying PIFA-mediated oxidative phenol coupling of N-(4-hydroxy)phenethyl-N-(3',4',5'-trialkoxy)benzyl formamide (15b) as a key step. Because of the symmetrical characteristics of the pyrogallol moiety in the substrate (15b), the phenol coupling resulted in a sole coupling product except for volatile components from the oxidizing agent. On the basis of the successful results of the above strategy, (-)-galanthamine (1) was synthesized by employing a novel remote asymmetric induction, where conformation of the seven-membered ring in the product of the phenol coupling was restricted by forming a fused-chiral imidazolidinone ring with D-phenylalanine on the benzylic C-N bond of the tri-O-alkylated gallyl amino moiety. The conformational restriction and successive debenzylation of the protected hydroxyl groups on the pyrogallol ring caused diastereoselective cyclization to yield a cyclic ether having the desired stereochemistry for the synthesis of (-)-1.     

Bisamides derived from azulene-1,3- and -5,7-dicarboxylic acids as new building blocks for anion receptors

Bisamides based on the azulene moiety were investigated as building blocks for anion receptors. In the course of these studies, derivatives of azulene-1,3- and -5,7-dicarboxylic acid were synthesized and thoroughly characterized. The anion affinities of the derivatives based on functionalization in the five-membered ring and in the seven-membered ring were determined by (1)H NMR titration. The structural analysis of these building blocks was performed by X-ray diffractometry, molecular modelling and 2D NMR spectroscopy. The five-membered ring derivatives are easy to obtain, offer a binding site preorganized in the syn-syn conformation and bind anions with a strength similar to those of pyrrole-based analogues. There is also strong evidence for aromatic CH...anion interactions. The ligands substituted at the 5- and 7-positions offer a binding cleft with an uncommon geometry that originates from the seven-membered ring and seems to be complementary to the chloride anion.     

Derivatives of 2-benzazepine-1,3-dione

The reactions of the di(acid chloride) of 2-carboxy-3,4-dimethoxyphenylthiopyruvic acid with 1-aminoadamantane and with thiosemicarbazide take place with the closure of a seven-membered ring and the formation of 1,2-dihydro-(3H)-2-benzazepine-1,3-dione. On reaction with monochloroacetic acid, 4-mercapto-8, 9-dimethoxy-2-(N-thioureido)-1, 2-dihydro-(3H)-2-benzazepine-3-dione is converted into a derivative of thiazolidine-2,4-dione 2-hydrazone, which readily takes part in condensation reactions with oxo compounds forming 5-ylidene derivatives.Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 1, pp. 29–32, January, 1984.     

Expansion of the pentafluorobenzene ring and other skeletal transformations in the reaction of perfluoro(1,2-diethyl-1-phenyl-1,2-dihydrocyclobutabenzene) with antimony pentafluoride

The reaction of perfluoro(1-phenyl-1,2-diethyl-1,2-dihydrocuclobutabenzene) with SbF5 at 20°C, followed by treatment of the reaction mixture with water gave perfluoro {4-[1-(2-propylphenyl)propylidene]-2,5-cyclohexadien-1-one} together with perfluoro[4b,10-diethylbenzo[a]azulen-7(4bH)-one] resulting from unusual expansion of the pentafluorobenzene ring to seven-membered ring. Analogous reaction at 90°C, apart from the above compounds, afforded perfluorinated 10-ethyl- and 3,10-diethylbenzo[a]azulen-6(10H)-ones via elimination of C₂F₅ group from the seven-membered ring or its migration to the benzene ring.     

A concise synthesis of the functionalized [5-7-6] tricyclic skeleton of guanacastepene A

The six membered ring of guanacastepene A was constructed by a Diels-Alder reaction of 1,1,4-trisubstituted diene to set up the correct relative stereochemistry at the C8 quaternary center and the remote C5 stereocenter. In 10 efficient steps from the Diels-Alder adduct 9, the desired highly functionalized [5-7-6] tricyclic skeleton 2 was synthesized. Key steps involve trimethylsilyl chloride (TMSCl) assisted Michael addition to form enol ether and the usage of the enol ether in the following intramolecular Mukaiyama aldol reaction to form the middle seven membered ring of guanacastepene A.     

Studies toward the total synthesis of diterpene antibiotic guanacastepene A: construction of the hydroazulenic core

[reaction: see text] As a part of studies aimed toward the total synthesis of biologically important natural product guanacastepene A of contemporary interest, a new and concise route to a fully functionally endowed hydroazulenic core is delineated. The strategy involves the building of the requisite stereochemical features on a endo-tricyclo[5.2.1.0(2,6)]decane matrix and excision of the five-membered ring through a retro-Diels-Alder reaction. Generation of the seven-membered ring to access the hydroazulenic framework was achieved employing ring closure metathesis (RCM) reaction as the key step.     

New total synthesis of the marine antitumor alkaloid (-)-agelastatin A

[reaction: see text] A new total synthesis of (-)-agelastatin A (1) has been achieved from the chiral oxazolidinone (-)-3. Although enone transposition was problematic when the Michael ring closure of 2 was attempted with strong base, the desired cyclization could be effected with Hunig's base after the pyrrole nucleus was brominated. Subsequent reduction and monobromination afforded synthetic (-)-agelastatin A (1).     

An asymmetric synthesis of aza analogues of the tricyclic skeleton of daphnane and the ABC ring system of phorbol

An asymmetric synthesis of aza analogues of the ABC ring system of phorbol and related compounds containing the 5-7-6-fused framework of daphnane involved construction of the central seven-membered ring by a regioselective reduction of a chiral imide and cyclization with trifluoromethanesulfonic acid. Subsequent demethylation and oxidative dearomatization of ring C afforded an enantiopure dienone 20 with the same relative and absolute configuration at the 9- and 10-positions of the phorbol skeleton.     

Photodissociation and photoisomerization of alpha-fluorotoluene and 4-fluorotoluene in a molecular beam

The photodissociation of jet-cooled alpha-fluorotoluene and 4-fluorotoluene at 193 and 248 nm was studied using vacuum ultraviolet (vuv) photoionization/multimass ion imaging techniques as well as electron impact ionization/photofragment translational spectroscopy. Four dissociation channels were observed for alpha-fluorotoluene at both 193 and 248 nm, including two major channels C6H5CH2F-->C6H5CH2 (or C7H7)+F and C6H5CH2F-->C6H5CH (or C7H6)+HF and two minor channels C6H5CH2F-->C6H5CHF+H and C6H5CH2F-->C6H5+CH2F. The vuv wavelength dependence of the C7H7 fragment photoionization spectra indicates that at least part of the F atom elimination channel results from the isomerization of alpha-fluorotoluene to a seven-membered ring prior to dissociation. Dissociation channels of 4-fluorotoluene at 193 nm include two major channels C6H4FCH3-->C6H4FCH2+H and C6H4FCH3-->C6H4F+CH3 and two minor channels C6H4FCH3-->C6H5CH2 (or C7H7)+F and C6H4FCH3-->C6H5CH (or C7H6)+HF. The dissociation rates for alpha-fluorotoluene at 193 and 248 nm are 3.3 x 10(7) and 5.6 x 10(5) s(-1), respectively. The dissociation rate for 4-fluorotoluene at 193 nm is 1.0 x 10(6) s(-1). An ab initio calculation demonstrates that the barrier height for isomerization from alpha-fluorotoluene to a seven-membered ring isomer is much lower than that from 4-fluorotoluene to a seven-membered ring isomer. The experimental observed differences of dissociation rates and relative branching ratios between alpha-fluorotoluene and 4-fluorotoluene may be explained by the differences in the six-membered ring to seven-membered ring isomerization barrier heights, F atom elimination threshold, and HF elimination threshold between alpha-fluorotoluene and 4-fluorotoluene.     

Asymmetric total synthesis of (-)-scabronine G via intramolecular double Michael reaction and Prins cyclization

The enantioselective total synthesis of (-)-scabronine G is described. The key features of the present synthesis include the construction of a 5-6 ring system containing two quaternary carbon centers via a diastereoselective intramolecular double Michael reaction and the formation of a seven-membered ring using a Prins cyclization.     

A new scheme for determining the intramolecular seven-membered ring N-H...O=C hydrogen-bonding energies of glycine and alanine peptides

In this paper a new scheme was proposed to calculate the intramolecular hydrogen-bonding energies in peptides and was applied to calculate the intramolecular seven-membered ring N-H...O=C hydrogen-bonding energies of the glycine and alanine peptides. The density-functional theory B3LYP6-31G(d) and B3LYP6-311G(d,p) methods and the second-order Moller-Plesset perturbation theory MP26-31G(d) method were used to calculate the optimal geometries and frequencies of glycine and alanine peptides and related structures. MP26-311++G(d,p), MP26-311++G(3df,2p), and MP2/aug-cc-pVTZ methods were then used to evaluate the single-point energies. It was found that the B3LYP6-31G(d), MP26-31G(d), and B3LYP6-311G(d,p) methods yield almost similar structural parameters for the conformers of the glycine and alanine dipeptides. MP2/aug-cc-pVTZ predicts that the intramolecular seven-membered ring N-H...O=C hydrogen-bonding strength has a value of 5.54 kcal/mol in glycine dipeptide and 5.73 and 5.19 kcal/mol in alanine dipeptides, while the steric repulsive interactions of the seven-membered ring conformers are 4.13 kcal/mol in glycine dipeptide and 6.62 and 3.71 kcal/mol in alanine dipeptides. It was also found that MP26-311++G(3df,2p) gives as accurate intramolecular N-H...O=C hydrogen-bonding energies and steric repulsive interactions as the much more costly MP2/aug-cc-pVTZ does.     

Methanol facilitated synthesis of 7-methoxy-2-thioxo-2,3-dihydro-1H-1,3-diazepin-4(7H)-ones from nitroallylic acetates and thiourea

A novel efficient strategy for the synthesis of rare 7-methoxy-2-thioxo-2,3-dihydro-1H-1,3-diazepin-4(7H)-ones is described. Methanol, solvent for this one-step reaction, participated in this seven-membered ring closure reaction between nitroallylic acetates and thiourea. The thiourea itself also served as a base in this reaction. A possible mechanism for the reaction is proposed.     

Arbeiten über Phosphorsäure- und Thiophosphorsäureester mit einem heterocyclischen Substituenten. 7. Mitteilung. Thio- und Dithiophosphorsäureester von der Art des GS 13005 mit einem analogen oder homologen heterocyclischen Ring

To complete results presented in this and in previous papers of this series as well as published in patents of other authors a review is given on known and new variations of the heterocyclic moiety in GS 13005 type thio- and dithiophosphoric acid esters ( 1, 2 ) by modification of the 1,3,4-thiadiazol-2(3H)-one ring 5 and by its replacement by analogue five- and homologue six-membered rings. Among new esters of this type some containing the pyrazolinone ring 3 or a 2-alkoxy-4H, 6H-1,3,4-thiadiazin-5-one ring 10 (homologue of the original 5-methoxy-1,3,4-thiadiazol-2(3H)-one ring in GS 13005) show no remarkable pesticidal activity, some others containing a pyrazolering 7 or a 3(2H)-pyridazinonc ring 8 are moderately to highly active but toxic to inauinials in the same proportion. Attempts to prepare seven-membered 2-alkoxy- and 2-alkylthio-6,7-dihydro-l, 3,4-thiadiazepin-S(4H)-ones 11 , Z-rnethoxy-l,3,4-thiadiazepin-S(4H)-one 12 (ring vinylogue of the original 5-methoxy-l,3,4-thiadIazol-2(3H)-one ring in GS 13005) and its 7-methyl-derivative have been unsuccessful due to unexpected side reactions, such as: five-ring closure of 3-(3-chloropropionyl)-thio- and -dithiocarbazic acid esters 22 to pyrazolidinone derivatives 23 , pyrazolinone ring closure of a 3-(acetoacety1)-thiocarbazic acid O-methyl ester derivative 26 , bromine attack on sulfur in 3-(2-alkenoyl)-thiocarbazic O-methyl esters 29 instead of bromine addition at the double bond, and halogen splitting off without ring closure in 3-(2,3-dihalogeno-alkanoyl) -thiocarbazic O-methyl esters 30 prepared by acylation of thiocarbazic acid O-methyl ester with dihalogeno-alkanoyl-chlorides.     

DFT calculations on the protonation of two 1,3-butadiyne units fixed in medium-sized rings

The N-bis-protonated forms of 1-azacyclotetradeca-3,5,10,12-tetrayne (19) and 1,8-diazacyclotetradeca-3,5,10,12-tetrayne (20) were used as model systems to study the HCl addition to two 1,3-butadiyne units in close proximity using quantum chemical means. The model calculations were carried out mainly at the B3LYP/3-21G or 6-31G level. The basis set 6-311G was used for single-point calculations. The calculations reveal that 19 and 20 are preferably protonated at the C4 center accompanied by a transannular ring closure between C3 and C13 yielding the bicyclic systems 23 and 24, respectively. Further stabilization of these vinyl cations is achieved by a second transannular ring closure between C6 and C10 leading to the 5-8-5 tricyclic systems 27 and 28, which are further stabilized by the addition of a chloride anion. The different regiochemistry experimentally observed for 13b and 16b was rationalized by calculating local softness parameters. The observed product selectivities for the formation of 14b and 15b were traced back to the relative stabilities of the primary protonation products 23 and 24, respectively. Model calculations on 1-azacyclopentadeca-3,5,11,13-tetrayne (65) and 1-azacyclohexa-deca-3,5,12,14-tetrayne (66) as examples for medium-sized rings with nonparallel 1,3-butadiyne units revealed a concerted process of protonation and C3-C15 (65) or C3-C16 (66) ring closure. The second step is the formation of an aromatic central ring as a result of a ring closure between C6-C13 and C6-C14, respectively.     

Total syntheses of (+/-)-beta-erythroidine and (+/-)-8-oxo-beta-erythroidine by an intramolecular Diels-Alder cycloaddition of a 2-amidoacrolein

[reaction: see text] The total syntheses of (+/-)-beta-erythroidine and (+/-)-8-oxo-beta-erythroidine are described. The tetracyclic ring system of the natural products was quickly assembled by a strategy that features a retrocycloaddition/cycloaddition reaction of an amidodioxin, an intramolecular Heck reaction, and a 6pi-electrocyclic ring closure of a dienoic acid.     

Stereoselective formal [3 + 3] cycloaddition approach to cis-1-azadecalins and synthesis of (-)-4a,8a-diepi-pumiliotoxin C. evidence for the first highly stereoselective 6pi-electron electrocyclic ring closures of 1-azatrienes

Evidence is described here to support that a highly stereoselective 6pi-electron electrocyclic ring closure of 1-azatrienes is a key step in formal [3 + 3] cycloaddition or annulation reactions of chiral vinylogous amides with alpha,beta-unsaturated iminium salts. This would represent the first highly stereoselective 6pi-electron electrocyclic ring closure of 1-azatrienes. We have also unambiguously demonstrated that these specific ring closures are reversible, leading to the major diastereomer that is also thermodynamically more stable, and that a rotation preference likely also plays a role. A synthetic application is illustrated here to stereoselectively transform the resulting dihydropyridines to cis-1-azadecalins with unique anti relative stereochemistry at C2 and C2a, leading to synthesis of epi isomers of (-)-pumiliotoxin C.     

Stereoselective synthesis of (−)-α-conhydrine

(?)-α-Conhydrine was synthesized from propargyl alcohol in 20% overall yield in nine steps. The key intermediates were obtained via a regioselective epoxide opening, cross-metathesis, tandem hydrogenation and hydrogenolysis, and stereoselective dihydroxylaton. The side product from the epoxide ring opening was used to synthesize the seven-membered amino sugar DMJ analogue.