Total synthesis of apigenin 7,4′-di-O-β-glucopyranoside, a component of blue flower pigment of Salvia patens, and seven chiral analogues

We have succeeded in the first total synthesis of apigenin 7,4′-di-O-β-d-glucopyranoside (1a), a component of blue pigment, protodelphin, from naringenin (2). Glycosylation of 2 according to Koenigs-Knorr reaction provided a monoglucoside 4a in 80% yield, and this was followed by DDQ oxidation to give apigenin 7-O-glucoside (12a). Further glycosylation of 4′-OH of 12a with 2,3,4,6-tetra-O-acetyl-α-d-glucopyranosyl fluoride (5a) was achieved using a Lewis acid-and-base promotion system (BF₃·Et₂O, 2,6-di-tert-butyl-4-methylpyridine, and 1,1,3,3-tetramethylguanidine) in 70% yield, and subsequent deprotection produced 1a. Synthesis of three other chiral isomers of 1a, with replacement of d-glucose at 7 and/or 4′-OH by l-glucose (1b-d), and four chiral isomers of apigenin 7-O-β-glucosides (6a,b) and 4′-O-β-glucosides (7a,b) also proved possible.     

New cyclometalated palladium(II) complexes with iminophosphines: Crystal structures of [Pd(C^N)(o-Ph2PC6H4–CH=NR)][PF6] (C^N=azobenzene,R=Et; C^N=2-phenylpyridine,R=Me)

The synthesis of new cyclometalated compounds of palladium(II) with the mixed-donor bidentate ligands o-Ph₂PC₆H₄–CH=NR is described. Two series of complexes [Pd(C^N)(o-Ph₂PC₆H₄–CH=NR)][PF₆] have been prepared using either azobenzene or 2-phenylpyridine as cyclometalated ligands [C^N=azobenzene (azb); R=Me (1a), Et (2a), ⁿPr (3a), ⁱPr (4a), ^tBu (5a), Ph (6a), NH–Me (7a); C^N=2-phenylpyridine (phpy); R=Me (1b), Et (2b), ⁿPr (3b), ⁱPr (4b), ^tBu (5b), Ph (6b), NH–Me (7b)]. The new complexes were characterized by partial elemental analyses and spectroscopic methods (IR, FAB, ¹H and ³¹P NMR). The molecular structures of compounds 2a (monoclinic, P 2₁/n) and 1b (monoclinic, C 2/c) have been determined by a single-crystal diffraction study. In both cases this technique revealed the relative trans configuration between the phosphorus atom and the nitrogen atom of the ortho-metalated ligand.     

Functionalized enamines—XXII : Annelation of enamines of polycyclic α,β-unsaturated ketones; a facile partial synthesis of furano- indolo- and benzsteroids. Total synthesis of 3-oxa-A-norsteroid

Reaction of dienamine 4a with substituted phenacyl bromides gave steroidal[3,4-b] furans 5a–g. The same principle reaction was utilized for the total synthesis of (±) 2 - (p - chlorophenyl) - 3 - oxa - A - nor - estra - 1,5(10), 9(11) - triene - 17 - acetate 12a. Treatment of 4a, b with benzenediazonium salts, in DMF, followed by a Fischer-indole cyclization yielded steroidal[6, 7-b] indoles 8a–k. Dienamine 4b could be annelated to benz[4, 5, 6] steroids 9a and 9b by reaction with methyl vinyl ketone and crotonaldehyde, respectively.     

Structural diversity and versatility for organoaluminum complexes supported by mono- and di-anionic aminophenolate bidentate ligands

The present contribution describes the synthesis and structural characterization of structurally diverse organoaluminum species supported by variously substituted aminophenolate-type ligands: these Al complexes are all derived from the reaction of AlMe₃ with aminophenols 2-CH₂NH(R)-C₆H₃OH (1a, R = mesityl (Mes); 1b, R = 2,6-di-isopropylphenyl (Diip)) and 2-CH₂NH(R)-4,6-^tBu₂-C₆H₂OH (1c, R = Mes; 1d, R = Diip). The low temperature reaction of AlMe₃ with 1a–b readily affords the corresponding Al dimeric species [μ-η¹,η¹-N,O-{2-CH₂NH(R)-C₆H₄O}]₂Al₂Me₄ (2a–b), consisting of twelve-membered ring aluminacycles with two μ-η¹,η¹-N,O-aminophenolate units, as determined by X-ray crystallographic studies. Heating a toluene solution of 2a (80 °C, 3 h) affords the quantitative and direct formation of the dinuclear aluminium complex Al[η²-N; μ,η²-O-{2-CH₂N(Mes)-C₆H₄O}](AlMe₂) (4a) while species 2b, under the aforementioned conditions, affords the formation of the Al dimeric species [η²-N,O-{2-CH₂N(Dipp)-C₆H₄O}AlMe]₂ (3b), as deduced from X-ray crystallography for both 3b and 4a. In contrast, the reaction of bulky aminophenol pro-ligands 1c–d with AlMe₃ afford the corresponding monomeric Al aminophenolate chelate complexes η²-N,O-{2-CH₂NH(R)-4,6-^tBu₂-C₆H₂O}AlMe₂ (5c–d; R = Mes, Diip; Scheme 3) as confirmed by X-ray crystallographic analysis in the case of 5d. Subsequent heating of species 5c–d yields, via a methane elimination route, the corresponding Al-THF amido species η²-N,O-{2-CH₂N(R)-4,6-^tBu₂-C₆H₂O}Al(Me)(THF) (6c–d; R = Mes, Diip). Compounds 6c–6d, which are of the type {X₂}Al(R)(L) (L labile), may well be useful as novel well-defined Lewis acid species of potential use for various chemical transformations. Overall, the sterics of the aminophenol backbone and, to a lesser extent, the reaction conditions that are used for a given ligand/AlMe₃ set essentially govern the rather diverse “structural” outcome in these reactions, with a preference toward the formation of mononuclear Al species (i.e. species 5c–d and 6c–d) as the steric demand of the chelating N,O-ligand increases.     

Preparation of various enantiomerically pure (benzotriazol-1-yl)- and (benzotriazol-2-yl)-alkan-2-ols

(S)-(−)-(Benzotriazol-1-yl)- and (S)-(−)-(benzotriazol-2-yl)-alkan-2-ols 7a–9a, 7b–9b and their (R)-(+)-acetates 10a–12a and 10b–12b were prepared in high enantiomeric excess via lipase from Pseudomonas fluorescens (Amano AK) catalyzed enantioselective acetylation of racemic alcohols 4a–6a and 4b–6b with vinyl acetate in tert-butyl methyl ether or toluene at 23 °C. The enantioselectivity of this transformation was dependent on the length of the alkyl chain with E-values ranging from 30 to 57. Several benzotriazole substituted ketones 1a–3a and 1b–3b were synthesized from 1H-benzotriazole and corresponding haloketones. These compounds were stereoselectively reduced with Baker’s yeast in water or in organic solvent containing 5% v/v of water at 30 °C to give the (S)-(−)-alcohol. Better stereoselectivity was observed in the kinetic resolution of racemic alcohols 4a–6a and 4b–6b (ee = 69–92% at 44–52% conversion) compared to reduction of corresponding prochiral ketones 1a–3a and 1b–3b with Baker’s yeast (ee = 40–67% at 39–89% conversion). Enhanced enantioselectivities were observed at lower temperatures.     

Structural diversity and versatility for organoaluminum complexes supported by mono- and di-anionic aminophenolate bidentate ligands

The present contribution describes the synthesis and structural characterization of structurally diverse organoaluminum species supported by variously substituted aminophenolate-type ligands: these Al complexes are all derived from the reaction of AlMe₃ with aminophenols 2-CH₂NH(R)-C₆H₃OH (1a, R = mesityl (Mes); 1b, R = 2,6-di-isopropylphenyl (Diip)) and 2-CH₂NH(R)-4,6-^tBu₂-C₆H₂OH (1c, R = Mes; 1d, R = Diip). The low temperature reaction of AlMe₃ with 1a–b readily affords the corresponding Al dimeric species [μ-η¹,η¹-N,O-{2-CH₂NH(R)-C₆H₄O}]₂Al₂Me₄ (2a–b), consisting of twelve-membered ring aluminacycles with two μ-η¹,η¹-N,O-aminophenolate units, as determined by X-ray crystallographic studies. Heating a toluene solution of 2a (80 °C, 3 h) affords the quantitative and direct formation of the dinuclear aluminium complex Al[η²-N; μ,η²-O-{2-CH₂N(Mes)-C₆H₄O}](AlMe₂) (4a) while species 2b, under the aforementioned conditions, affords the formation of the Al dimeric species [η²-N,O-{2-CH₂N(Dipp)-C₆H₄O}AlMe]₂ (3b), as deduced from X-ray crystallography for both 3b and 4a. In contrast, the reaction of bulky aminophenol pro-ligands 1c–d with AlMe₃ afford the corresponding monomeric Al aminophenolate chelate complexes η²-N,O-{2-CH₂NH(R)-4,6-^tBu₂-C₆H₂O}AlMe₂ (5c–d; R = Mes, Diip; Scheme 3) as confirmed by X-ray crystallographic analysis in the case of 5d. Subsequent heating of species 5c–d yields, via a methane elimination route, the corresponding Al-THF amido species η²-N,O-{2-CH₂N(R)-4,6-^tBu₂-C₆H₂O}Al(Me)(THF) (6c–d; R = Mes, Diip). Compounds 6c–6d, which are of the type {X₂}Al(R)(L) (L labile), may well be useful as novel well-defined Lewis acid species of potential use for various chemical transformations. Overall, the sterics of the aminophenol backbone and, to a lesser extent, the reaction conditions that are used for a given ligand/AlMe₃ set essentially govern the rather diverse “structural” outcome in these reactions, with a preference toward the formation of mononuclear Al species (i.e. species 5c–d and 6c–d) as the steric demand of the chelating N,O-ligand increases.     

Synthesis of 5-endo-, 5-exo-, 6-endo- and 6-exo-hydroxylated analogues of epibatidine

A convenient, high-yield synthesis of N-Boc-7-azabicyclo[2.2.1]hept-5-en-2-one (7) was developed by SmI₂-mediated desulfonylation of 6. Thus, 5-endo-, 5-exo-, 6-endo-, and 6-exo-hydroxylated epibatidine analogues 2a,b and 3a,b were synthesized from 7 by using a Pd(PPh₃)₄-catalyzed reductive Heck coupling reaction and SmI₂-mediated reduction of the carbonyl group as the key steps. Other reaction conditions for the reductive Heck procedure and the reduction step were also investigated.     

Synthesis of novel β-amino alcohols and their application in the catalytic asymmetric sulfoxidation of sulfides

Novel chiral norephedrine-based β-amino alcohol ligands containing a thiophene ring were prepared from norephedrine and substituted furan carbaldehydes (methyl- or ethyl-substituted) and used in combination with VO(acac)₂ for the asymmetric oxidation of aryl methyl sulfides using H₂O₂ as an oxidant. Amino alcohol derived Schiff bases 4,5a–b gave higher enantiomeric excesses than amino alcohol-derived reduced Schiff based ligands 6,7a–b. Of these chiral ligands, (1S,2R)-5b and (1S,2R)-7b gave high yields (90%) with moderate to high enantioselectivities (78%, 96% ee, respectively). The oxidation of other aryl methyl sulfides with (1S,2R)-5b and (1S,2R)-7b as ligands afforded the corresponding sulfoxides in 60–89% yields and with 92–99% ee.     

Synthesis,characterization and biological evaluation of purine nucleoside analogues

We present a convenient route for the synthesis of C6-amino-C5′-N-cyclopropyl carboxamido-C2-alkynylated purine nucleoside analogues 11a–g via Sonogashira coupling reaction. The nine step synthesis is easy to perform, employing commercially available reagents. Compound 9 is used as key intermediate for the synthesis of analogues 11a–g. Synthetic intermediates and final products are appropriately characterized by IR, ¹H NMR, ¹³C NMR and Mass. The modified nucleoside analogues 11a–g is evaluated for in vitro anticancer activity against MDA-MB-231 and Caco-2 cell lines. Screening data reveals that compounds 11b and 11e displayed potent IC₅₀ value of 7.9, 6.8 µg/mL respectively against MDA-MB-231 and of 7.5, 8.3 µg/mL respectively against Caco-2 than the standard drug doxorubicin, thus establishing the potential anti-cancer properties of these newer derivatives.     

Novel thiosemicarbazone derivatives containing benzimidazole moiety: Green synthesis and anti-malarial activity

A series of (E)-2-[5-chloro-1-(1H-benzo[d]imidazol-2-yl)ethylidene] N-(substituted) hydrazine carbothioamide (7a–7t) and (E)-2-[1-(1H-benzo[d]imidazol-2-yl)ethylidene] N-(substituted) hydrazine carbothioamide (8a–8t) were prepared via the synthesis of 1-(substituted-1H-benzimidazol-2-yl) ethanol (3a–3b) which was synthesized by the condensation of substituted o-phenylenediamine (2a–2b) with dl-lactic acid (1) followed by oxidation with sodium hypochlorite in mild acidic condition to form the corresponding ketones 4a–4b. Final compounds were formed by condensation of 4a–4b with different thiosemicarbazides 6a–6t. A total of 40 compounds were synthesized and characterized by FT-IR, ¹H NMR, ¹³C NMR, Mass spectral technique and elemental analysis, in addition they were evaluated for anti-malarial properties. Among the compounds tested 7o, 7p, 7q, 7r, 7s, 8e and 8h exhibited good antimalarial activity in vitro.     

Regioselective synthesis of the 1-bromo-4-phenyl-tetrahydro-7-amino-benzocyclohepten-6-one,a subnanomolar aminopeptidase-N/CD13 inhibitor

A regioselective synthesis of the title 1-bromo-4-phenyl-tetrahydro-7-amino-benzocyclohepten-6-one 2 has been pursued and develop in order to allow a large scale synthesis of this highly potent and selective APN inhibitor (K_i 60 pM). The pivotal step in this approach was the desymmetrization of the ketones 6a,b through regioselective generation of the silyl enol ethers 5a,b. After obtention of the corresponding enones 13a,b and the ene-amides 4a,b–4′a,b, it was possible to separate the regioisomers at this step. Conversion to the desired phenylbromo-amide 17 was achieved from the both isolated major and minor regioisomers through chemical manipulations including Suzuki coupling and Sandmeyer reaction. The title compound 2·HCl was finally synthesized after a series of deprotections/protection.     

Synthesis and characterization of novel five-membered palladacycles

3-(2-Chloroquinolin-3-yl)-1,5-bis(3,4,5-trimethoxy-phenyl)-pentane-2,4-dione derivatives 3a–b were conveniently synthesized in excellent yields (82% each) by tandem Knoevenagel condensation reactions of 2-chloro-3-carbaldehyde-quinoline 1a–b with 3,4,5-trimethoxy acetophenone, followed by a base catalyzed Michael addition, such as DBU (1,8-diazabicyclo[5,4,0]undec-7-ene) with or without solvent. The reactions of 3a–b with Pd(dba)₂ in the presence of PPh₃ (1:2) in degassed acetone provided the dinuclear palladium complexes {Pd(C,N-2-C₉H₄N–CH–[–CH₂CO(3,4,5-(OMe-)₃–C₆H₂-]₂–3-R-6)Cl(PPh₃)}₂ [(R = H (4a), R = OMe (4b)] in moderate yields (38% and 43%), which in turn reacted with an excess of isonitrile XyNC (Xy = 2,6-Me₂C₆H₃) to give the corresponding palladacycles 5a–b in moderate yields (45% and 43%). The palladacycles 5a–b were also obtained in similar yields (32% and 33%) via a one-pot oxidative addition reaction of 3a-b with isonitrile XyNC:Pd(dba)₂ (4:1). The products were characterized by satisfactory elemental analysis and spectral studies (IR, ¹H, and ³¹P NMR). The crystal structure of 5a was determined by X-ray crystallography diffraction studies.     

An efficient route for the synthesis of 2-arylthiazino[5,6-b]indole derivatives

Substituted 2-thiobenzamidomethylindole derivatives (14a-e) were prepared by the reaction of 2-aminomethylindole (9) with substituted benzoyl chlorides, followed by sulfurization using Lawesson's reagent. Alternatively, these thioamides were obtained from the amine in one step in an efficient manner by using substituted benzaldehydes in the presence of sulfur, or at room temperature with the aid of substituted methyl dithiobenzoates. The Hugerschoff reactions of thiobenzamides (14a-e) with phenyltrimethylammonium tribromide provided the rare title 2-arylthiazino[5,6-b]indoles (15a-e) in good yields. A convenient one-pot approach for the synthesis of 2-phenyl-1,3-thiazino[5,6-b]indole (15a) from 2-aminomethylindole (9) is also described.     

Alkynylcarbyne complexes containing various tri- and bidentate ligands such as cyclopentadienide,tris(pyrazolyl)borate,bis(pyrazolyl)acetate and tmeda: synthesis and spectroscopic properties

The (alkynylcarbyne)tungsten complexes [L₃(CO)₂WCCCR] (3a,b–6a,b) [L₃=hydro[tris(3,5-dimethylpyrazol-1-yl)]borato (Tp′, 3), hydro[tris(pyrazol-1-yl)]borato (Tp, 4), cyclopentadienyl (Cp, 5), bis(3,5-dimethylpyrazol-1-yl)acetato (bdmpza, 6); R=SiMe₃ (a), Ph (b)] were prepared in a stepwise fashion from [W(CO)₆] and Li[CCR], (CF₃CO)₂O and M[L₃] (M=Na, K). The formation of 6a,b was highly selective, only complexes with a trans arrangement of the carboxylate group of bdmpza and the alkynylcarbyne ligand were detected. The reaction of [W(CO)₆] with Li[CCR], C₂O₂Cl₂ and tmeda afforded trans-[Cl(CO)₂(tmeda)WCCCR] (7a,b). The electron-donating potential of the different tripodal ligands L₃ was studied by IR- and ¹³C-NMR spectroscopy and compared to that of the ligand combination Cl/tmeda. The IR data suggest that in these complexes bdmpza is a weaker electron donor than Tp′ and Tp but displays stronger electron-donating abilities than Cp. The structures of 6b and 7b were established by X-ray structural analyses.     

Asymmetric catalysis. Part 153: Metal-catalysed enantioselective α-ketol rearrangement

Promoted by catalytic amounts of Ni complexes tertiary α-hydroxyketones 1a, 3a–5a undergo rearrangement, forming chiral isomers 1b, 3b–5b. The best enantioselection was obtained with the model system 1-benzoylcyclopentanol 4a/2-hydroxy-2-phenylcyclohexanone 4b. In a ligand screening 2-[4-(S)-tert-butyloxazolin-2-yl]pyridine gave the highest enantiomeric excess of 46% (S)-4b. The analogous isomerisation reactions of α-hydroxyimines 6a, 7a forming chiral α-aminoketones 6b, 7b were established.     

Further applications of endocyclic enamine-enone annulations : The total syntheses of rac-Sceletium alkaloid A4 and 3'-demethoxy sceletium alkaloid A4

The total synthesis of rac-sceletium alkaloid A₄1a and of its 3'-demethoxy analogue 1b via the annulation of endocyclic enamines 4a–b is presented. The Michael acceptor 5a is a useful synthon for the two-step synthesis of 2,3-disubstituted pyridines from Δ²-pyrrolines.     

Solvent-dependent reactivities of acyclic nitrones with β-diketones: catalyst-free syntheses of endiones and enones

Reactions of the nitrones ^?O⁺N(Me)C(H)Ar 1 (Ar=phenyl 1a, 4-methylphenyl 1b, 2,4,6-trimethylphenyl 1c, and anthracen-9-yl 1d) with the cyclic β-diketones 1,3-indandione 2 or barbituric acid 3 in CH₂Cl₂, afford the corresponding endiones 2′a–2′d or 3′a–3′d. In contrast, dimedone 4 reacts with 1a or 1b to give the endione 4′a or 4′b and the bis-adduct 4″a or 4″b. Nevertheless, reaction of 4 with 1c or 1d in CH₂Cl₂ furnishes only the endione adducts 4′c or 4′d. However, the reaction of 4 with 1a or 1b in methanol gives only 4″a or 4″b, respectively. Among acyclic β-diketones only malonic acid 7 reacts with 1a–1c. Reaction of 7 with 1a in CH₂Cl₂ forms cinnamic acid 7″a, whereas in the case of 1b, the endione 7′b and (E)-3-p-tolylacrylic acid 7″b are obtained. The nitrone 1c reacts with 7 in CH₂Cl₂ to afford the endione 7′c or with acetone yielding (E)-4-mesitylbut-3-en-2-one 8. X-ray analyses are reported for 4′c, 5, and 7″b. In addition, the calculated acidity of the hydrogen at the α-C atom is shown to correlate with the reactivity of the β-diketones with nitrones.     

Stereocontrolled synthesis of enantiomerically pure unsaturated analogues of 2,6-DAP. Part 5

An efficient new stereocontrolled synthesis of (2R,6R)-(+)- and (2S,6S)-(−)-2,6-diamino-4-methylene-1,7-heptanedioic acid 8a and 9a, respectively, has been accomplished starting from the glycine-derived chiral synthon 1. The enantiomerically pure α-alkyl derivatives 8b–d and 9b–d have also been synthesized. The absolute configuration of the new stereocenters was assigned on the basis of ¹H NMR spectra.     

Synthese von (5,10)-(7,8)-Bisepoxiden aus α- und β-4-Phenyl-1,2,4-triazolin-3,5-dion-Addukten von Vitamin D3 und Röntgenstrukturanalyse eines der Benzoylderivate

Oxidation of the α- and β-4-phenyl-1,2,4-triazolin-3,5-dione adducts of vitamin D₃ (2 and1) withMCPBA yields two diastereomeric mixtures of the (5,10)-(7,8)-dioxiranes3 a,3 b,3 c and4 a,4 b respectively. The corresponding benzoates5 a,5 b,6 a and6 b were prepared and the X-ray crystal structure of5 b was determined. This analysis proved5 b to be the (5R, 1 OS)-(7R, 8R)-dioxirane of the β-resp. (6S)-4-phenyl-1,2,4-triazolin-3,5-dione adduct1 of vitamin D₃.     

d- and l-Serine, useful synthons for the synthesis of 24-hydroxyvitamin D3 metabolites. A formal synthesis of 1α,24R,25-(OH)3-D3, 24R,25-(OH)2-D3 and 24S,25-(OH)2-D3

d- and l-Serine have been used for the enantioselective synthesis of tosylates 7a and 7b, useful building blocks for the synthesis of triols 5a and 5b which have already been obtained via a diastereoselective synthesis and used for the synthesis of 2a, 2b and 2c. We have thus performed a formal synthesis of 24S,25-(OH)₂-D₃, 24R,25-(OH)₂-D₃ and 1α,24R,25-(OH)₃-D₃.