Cyclotransformation in the series of fused 5-nitropyridin-2(1<Emphasis Type="Italic">H</Emphasis>)-ones

Reactions with excess hydrazine hydrate of 5-nitropyridin-2(1H)-ones fused with benzene, pyridine, and 1,2,3-triazole rings led to a cyclotransformation of the 5-nitro-2-oxopyridine fragment into the 6-methyl-3-oxopyridazine structure. This cyclotransformation is of general character; a probable mechanism of the process is suggested. Details of the assumed mechanism were experimentally confirmed on model compounds.     

Influence of excitation and solvation on the shift of tautomeric equilibrium. A quantum-mechanical study

Two quantum-mechanical models are proposed to described a shift of tautomeric equilibrium as a result of electronic excitation and change of environment. According to the first n PD MEP model which is used to estimate the relative solvation effect on the stability of tautomers in an excited state, the calculation of the interaction energy between a solvent (simulated by a set of n point dipoles, n PD) and an excited solute molecule is based on the molecular electrostatic potential (MEP) of the corresponding excited state. In the second n PDQ model, a solvent represented by a set of n point dipoles and quadrupoles (n PDQ) modifies the solute's hamiltonian via an electrostatic interaction contribution. Comparing the results of the calculation for isolated and solvated tautomers, the n PDQ model is used to estimate the influence of electronic excitation on the change of relative stability of tautomers existing in a solution. An application of both models to 2- and 4-oxopyridine predicts a shift of the tautomeric equilibria in their excited states in accordance with experimental evidence.     

Water environmental effect on tautomeric equilibria of 2- and 4-oxopyridines. A CNDO/2 study

The supermolecule approach is proposed to evaluate the shift of the tautomeric equilibrium of a molecule when going from the vapour phase to water solution. According to the model, a comparison of the stabilization (hydration) energies of different tautomers of a molecule surrounded by water molecules predicts changes in tautomeric equilibrium upon solvation. An application of the model (within the CNDO/2 method) to 2- and 4-oxopyridine shows that the lactam tautomers of the molecules are more stabilized by water molecules than the corresponding lactim forms by about 7–8 kcal/mole.     

Synthesis of certain 1-β-D-ribofuranosyl-1,2-dihydro-2-oxopyridines structurally related to nicotinamide ribonucleoside

Several substituted 1-β-D-ribofuranosyl-1,2-dihydro-2-oxopyridines have been prepared as congeners of nicotinamide ribonucleoside. Direct glycosylation of the silylated 3-ethylcarboxylate 5 or 3-carbamoyl 6 derivative of 1,2-dihydro-2-oxopyridine with 1,2,3,5-tetra-O-acetyl-β-D-ribofuranose ( 7 ) in the presence of trimethylsilyl triflate gave the corresponding blocked nucleosides 8 and 9 , respectively in good yield. Ammonolysis of 8 and 9 with methanolic ammonia furnished 1-β-D-ribofuranosyl-1,2-dihydro-2-oxopyridine-3-carboxa-mide ( 10 ), the structure of which was established by single-crystal X-ray diffraction analysis. Thiation of 9 with Lawesson's reagent and subsequent deacetylation of the thiated product 11 with methanolic ammonia furnished 1-β-D-ribofuranosyl-1,2-dihydro-2-oxopyridine-3-thiocarboxamide ( 12 ). Modification of the carbo-nitrile function of 1-(2,3,5-tri-O-acetyl-β-D-ribofuranosyl)-1,2-dihydro-2-oxopyridine-4-carbonitrile ( 13 ) gave a series of 4-substituted-1-β-D-ribofuranosyl-1,2-dihydro-2-oxopyridines, in which the 4-substituent is a thiocarboxamide 15 , carboxamide 16 , carboxamidoxime 17 , carboxamidine 18 and aminomethyl 19 group. None of these compounds exhibited any significant antitumor or antiviral effects in vitro.     

New modular and efficient approach to 6-substituted pyridin-2-yl C-nucleosides

A novel modular, efficient, and practical methodology of preparation of 6-substituted pyridin-2-yl C-nucleosides was developed. An addition of 2-lithio-6-bromopyridine 2b to TBDMS-protected 2-deoxyribonolactone 5 gave aduct 7 as an equilibrium mixture of anomeric hemiketals 1-(6-bromopyridin-2-yl)-1-hydroxynucleosides 7a,b and its open form 7c. Reduction of the adduct 7 with Et3SiH and BF3 x Et2O afforded the desired 6-bromonucleoside 8a as pure beta-anomer in a total yield of 32% over two steps from 5. Intermediate 8a was then subjected to a series of palladium catalyzed cross-coupling reactions and aminations to give a series of protected 1beta-(6-alkyl-, 6-aryl-, and 6-aminopyridin-2-yl)-2-deoxyribonucleosides 9. Catalytic hydrogenation of 8a gave an unsubstituted pyridine C-nucleoside, and diazotative oxodeamination of 6-aminopyridine nucleoside 9f by isopentyl nitrite in acetic acid gave 6-oxopyridine nucleoside 10i. Deprotection of silylated nucleosides 9 by Et3N.3HF gave a series of free C-nucleosides 10.     

Modular and practical synthesis of 6-substituted pyridin-3-yl C-nucleosides

A novel modular and practical methodology for preparation of 6-substituted pyridin-3-yl C-nucleosides was developed. The Heck reaction of 2-chloro-5-iodopyridine with a 3'-TBDMS-protected glycal gave a 6-chloropyridin-3-yl nucleoside analogue, which was then desilylated, selectively reduced, and reprotected to give the TBDMS-protected 6-chloropyridin-3-yl C-2'-deoxyribonucleoside as a pure beta-anomer in a total yield of 39% over four steps. This key intermediate was then subjected to a series of palladium-catalyzed cross-coupling reactions, aminations, and alkoxylations to give a series of protected 1beta-(6-alkyl-, 6-aryl-, 6-hetaryl, 6-amino-, and 6-tert-butoxypyridin-3-yl)-2'-deoxyribonucleosides. 6-Unsubstituted pyridin-3-yl C-nucleoside was prepared by catalytic hydrogenation of the chloro derivative and 6-oxopyridine C-nucleoside by treatment of the 6-tert-butoxy derivative with TFA. Deprotection of all the silylated nucleosides by Et3N.3HF gave a series of free C-nucleosides (10 examples).     

Conformationally rigid chelate rings in metal complexes of pyridyloxy-substituted 2,2'-dioxybiphenyl-cyclotetra- and cyclotriphosphazene platforms

Divalent metal halides react with pyridyloxy-substituted 2,2'-dioxybiphenyl-cyclotri- and cyclotetraphosphazene ligands to form the complexes, [MLX2] [M=Co or Cu; L=(2,2'-dioxybiphenyl)tetrakis(2-pyridyloxy)cyclotriphosphazene (L1) or (2,2'-dioxybiphenyl)tetrakis(4-methyl-2-pyridyloxy)cyclotriphosphazene (L2); X=Cl or Br], [ZnLCl2] [L=bis(2,2'-dioxybiphenyl)bis(2-pyridyloxy)cyclotriphosphazene (L3) or bis(2,2'-dioxybiphenyl)bis(4-methyl-2-pyridyloxy)cyclotriphosphazene (L4)], [MLCl2] [M=Cu or Hg; L=tris(2,2'-dioxybiphenyl)bis(2-pyridyloxy)cyclotetraphosphazene (L5)] and [Cu2LCl4] (L=trans-bis(2,2'-dioxybiphenyl)tetrakis(2-pyridyloxy)cyclotetraphosphazene (L6)]. Single-crystal X-ray structures show the L2 ligand complexes to have a N3Cl2 five-coordinate, trigonal-bipyramidal donor set with the phosphazene ring and pendant pyridyloxy nitrogens binding to the metal ions. The coordinated L2 ligand in the complex, [CoL2Cl2], slowly hydrolyses in acetonitrile with the loss of a pyridine pendant arm to form a dimetallic species, which has been characterized by crystallography as [{CoL2aCl}]2.4MeCN (L2a=[N3P3(biph)(OPy)3(O)]-, biph=2,2'-dioxybiphenyl, OPy=2-oxopyridine). The ligands, L3, L4, L5, and L6, bind to the metal halides via gem-substituted pyridyloxy nitrogens only. The resulting rigid eight-membered chelate rings all have distorted boat conformations, which force distorted-tetrahedral N2Cl2 coordination environments onto the metal ions. The spectroscopic (ESR and electronic) and magnetic properties of the complexes are reported.     

A macrocyclic ligand able to bind gallium(III) by preorganized pendant arms; coordination and kinetic studies

The equilibria and kinetics of the binding of gallium(III) to 4-(N),10-(N)-bis[2-(3-hydroxo-2-oxo-2-H-pyridine-1-y1)acetamido]-1,7-dimethyl-1,4,7,10-tetraazacyclododecane (L) were investigated in acidic medium at ionic strength 1 M (NaClO4). Spectrophotometric titrations in the UV region revealed that L is able to bind Ga3+ also at high H+ concentration. The kinetic (stopped-flow) experiments are interpreted on the basis of three parallel reaction paths (i) M3+ + H2L2+ = M(H2L)5+ where M(H2L)5+ is in a steady state, (ii) M(OH)2+ + H2L2+ = M(HL)4+ + H2O and (iii) M(OH)2+ + HL+ = ML3+ + H2O. The first-order rate constants for conversion of the outer-sphere into the inner-sphere complexes are similar to those of the Ga(III)/tropolone system which is known to react according to the dissociative Id mechanism and to the relevant rate constants for water exchange at the metal ion. The effects of pH on the UV-Vis absorption, fluorescence emission properties and NMR spectral features on the Ga(III)/L system were also investigated. Spectrophotometric titrations in the UV region reveal that, in acid medium the prevailing species is M(HL)4+ whereas the chelate ML3+ prevails for [H+] < 0.01 M. The results indicate metal coordination at the oxygen atoms of the 3-hydroxo-2-oxopyridine residues.     

Studies towards the synthesis of (1R,2S)- and (1S,2S)-1,2-epoxy-3-hydroxypropylphosphonates and (1S,2S)- and (1R,2S)-2,3-epoxy-1-hydroxypropylphosphonates

The trans-configured fosfomycin analogue, diethyl (1S,2S)-1,2-epoxy-3-hydroxypropylphosphonate, was synthesised by the intramolecular Williamson reaction of diethyl (1S,2R)-1,3-dihydroxy-2-mesyloxypropylphosphonate. The cis-analogue was obtained as O-ethyl or O,O-diethyl (1R,2S)-1,2-epoxy-3-hydroxypropylphosphonates, when (1R,2R)-1,3-dihydroxy-2-mesyloxypropylphosphonate or its 3-O-trityl derivative were used as starting materials, respectively. The intramolecular Williamson cyclisations of diethyl (1S,2R)- and (1R,2S)-1-benzyloxy-3-hydroxy-2-mesyloxypropylphosphonates led to diethyl (1S,2S)- and (1R,2S)-2,3-epoxy-1-benzyloxypropylphosphonates, respectively, with the concomitant formation of diethyl (E)-1-benzyloxy-3-hydroxyprop-1-en-1-phosphonate. From diethyl (1S,2S)- and (1R,2S)-2,3-epoxy-1-benzyloxypropylphosphonates, enantiomerically pure diethyl (1S,2S)- and (1R,2S)-1,2-dihydroxypropylphosphonates were obtained by catalytic hydrogenation, while diethyl (1S,2S)- and (1R,2S)-3-acetamido-1,2-dihydroxypropylphosphonates were produced after epoxide ring opening with dibenzylamine, acetylation and hydrogenolysis.     

A mild and efficient cyanosilylation of ketones catalyzed by a Lewis acid-Lewis base bifunctional catalyst

A new family of bifunctional catalysts (N-oxides-Ti(OⁱPr)₄ (2:1)) containing a Lewis acid and a Lewis base was developed and applied to the catalytic cyanosilylation of ketones. Utilizing rac((1R,2S) and (1S,2R))-1-(2′-pyridylmethyl)-2-diphenylhydroxymethylpyrrolidine N-oxide-titanium (2:1) complex and N-benzyl-diethanolamine N-oxide-titanium (2:1) complex as catalysts, the cyanosilylation products were obtained in 42-97% yield. Based on experimental phenomena and kinetic studies, a catalytic cycle was proposed to explain the remarkable activities of these catalysts. Investigations indicated that rac((1R,2S) and (1S,2R))-1-(2′-pyridylmethyl)-2-diphenylhydroxymethylpyrrolidine N-oxide-titanium (2:1) complex and N-benzyl-diethanolamine N-oxide-titanium (2:1) complex should promote the reaction via a dual activation of the ketone by the titanium and TMSCN by the N-oxide.     

Regioselective biocatalytic hydrolysis of (E,Z)-2-methyl-2-butenenitrile for production of (E)-2-methyl-2-butenoic acid

Acidovorax facilis 72W nitrilase catalyzed the regioselective hydrolysis of (E,Z)-2-methyl-2-butenenitrile, producing only (E)-2-methyl-2-butenoic acid with no detectable conversion of (Z)-2-methyl-2-butenenitrile. (E)-2-Methyl-2-butenoic acid, produced in aqueous solution as the ammonium salt, was readily separated from (Z)-2-methyl-2-butenenitrile, and isolated in high yield and purity. The combination of nitrile hydratase and amidase activities of several Comamonas testosteroni strains were also highly regioselective for the production of (E)-2-methyl-2-butenoic acid from (E,Z)-2-methyl-2-butenenitrile.     

Solid-state structure determination and solution-state NMR characterization of the (2R,4R)/(2S,4S)- and (2R,4S)/(2S,4R)-diastereomers of the agricultural fungicide propiconazole,the (2R,4S)/(2S,4R)-symmetrical triazole constitutional isomer,and a ditriazole analogue

Single-crystal X-ray diffraction analysis was used to determine the structure of a racemic diastereomer of the agricultural fungicide propiconazole [1-(2-(2,4-dichlorophenyl)-4-n-propyl-1,3-dioxolane-2-yl-methyl)-1-H-1,2,4-triazole] and of two by-products (a symmetrical 1,3,4-triazole racemic-constitutional isomer and a propiconazole ditriazole analogue). All three crystalline racemic-diastereomers had (2R,4S)/(2S,4R)-stereochemistry in which then-propyl group was observed in atrans-to-phenyl disposition. Propiconazole (2R,4S)/(2S,4R)-diastereomer gives crystals belonging to the monoclinic space group P2₁,/a, and, at 293 K,a=8.1192(3),b=18.9769(6),c=10.7137(4) å,Β=99.765(3)?,V=1626.8(1) å³, Z=4,R(F)=0.060, andR _w(F)=0.058. The constitutional isomer by-product (2R,4S)/(2S,4R)-1-(2-(2,4-dichlorophenyl)-4-n-pro-pyl-1,3-dioxolane-2-yl-methyl)-1-H-1,3,4-triazole gives crystals belonging to the monoclinic space group P2₁/n, and, at 293 K,a=11.1763(6),b=10.7716(4),c=14.5804(8) å,Β=107.445(4)?,V=1674.6(1) å³, Z=4,R(F)=0.043, andR _w(F)=0.043. The ditriazole byproduct (2R,4S)/(2S,4R)-1-(2-(2-chloro-4-(1,2,4-triazole-1-yl)phenyl)-4-n-propyl-1,3-dioxolane-2-yl-methyl)-1-H-1,2,4-triazole gives crystals belonging to the triclinic space groupP¯ 1, and, at 193 K,a=5.3329(8),b=8.3738(7),c=20.240(2) å, α=84.213(6)?,Β=87.20(1)?,γ=86.23(1)?,V=896.5(2) å³, Z=2,R(F)=0.046, andR _w(F)=0.051. The presence of both propiconazole (2R.4S)- and (2S,4R)-enantiomers enables the formation of a crystalline racemic modification, while the diastereomeric propiconazole (2R,4R)- and (2S,4S)-enantiomers are viscous oils. In the absence of its enantiomorphic partner, the propiconazole (2R,4S)- or (2S,4R)-enantiomers remain as viscous oils rather than form chiral crystals.     

Superconducting LaRu2P2 and other alkaline earth and rare earth metal ruthenium and osmium phosphides and arsenides with ThCr2Si2 structure

The ThCr₂Si₂-type compounds MRu₂P₂ (M = Ca, Sr, Ba, Y, La, Ce, Pr, Nd, Sm, Eu, Gd, Tb, Dy, Ho, Er, Yb), MOs₂P₂ (M = Sr, Ba, Eu), and MRu₂As₂ (M = Ca, Sr, Ba, La, Eu) were prepared by sintering techniques and/or by reaction of the elemental components in a tin flux. The crystal structures of SrRu₂P₂ and LaRu₂P₂ were refined from single-crystal diffractometer data to residuals of R = 0.019 (224 structure factors, 11 variable parameters) and R = 0.028 (510 F's, 11 variables), respectively. LaRu₂P₂ is diamagnetic and becomes superconducting at 4.1 K. No transition to a superconducting state was observed down to 1.8 K for the compounds MFe₂P₂ (M = Ca, Sr, Ba, La), MRu₂P₂ (M = Ca, Sr, Ba, Y), and MOs₂P₂ (M = Sr, Ba).     

Autoionization resonances in atomic Ga,In, and Pb

Autoionization resonances of the type (n?1)d→np, wheren pertains to the outermost shell of Ga, In and Pb, were studied with the use of electron spectrometry in combination with synchrotron radiation. The relative strengths of the exit channels for the various resonance states were measured. In the case of Ga and In, a complete partitioning of the total absorption cross section into thes ^{2 1} S,sp ¹ P, andsp ³ P components (exit channels) was achieved, and in the case of Pb the decay of the resonance states into the major exit channels 6s ² 6p ² P _1/2, 6s ² 6p ² P _3/2, 6s 6p ^{2 4} P _1/2, 6s 6p ^{2 2} D _3/2 and 6s 6p ^{2 2} P _1/2 was determined. In Ga, strong coupling was observed for those states of the 4p ² manifold that have the same symmetries as the final ionic states, e.g. 4p ^{2 3} P→4s 4p ³ P and 4p ^{2 1} S→4s ^{2 1} S. In In, there is a similar, but weaker correlation, which also includes two-electron excitation channels. Comparison between Ga and In shows that thesp ³ P channel is much stronger in In (52% vs 40% in Ga) while thesp ¹ P channel is correspondingly weaker (28% vs 37%), with thes ^{2 1} S channel remaining practically unchanged (20 vs 23%). In Pb, the 6s ² 6P ² P _1/2 channel displays interference patterns due to a strong, competing direct transition, whereas the other channels do not, indicating population predominantly via the resonance states.     

2-Chloro and 2-fluoro ketones derived from the chiral-pool

Both (2R,5R)- and (2S,5R)-isomers of 2-chloro-2-isopropyl-5-methyl-, 2-chloro-2-methyl-5-isopropyl- and 2-fluoro-2-methyl-5-isopropylcyclohexanones have been synthesized and fully characterized. It is shown that a rapid overview of the ¹H NMR spectrum allows an unambiguous assignment of the axial or equatorial position of the halogen atom and that the IR ν_CO absorption does not differ from one isomer to the other.     

2-Acetylpyridine- and 2-benzoylpyridine-derived thiosemicarbazones and their antimony(III) complexes exhibit high anti-trypanosomal activity

Complexes [Sb(2Ac4oClPh)Cl₂] (1), [Sb(2Ac4oFPh)Cl₂] (2), [Sb(2Ac4oNO₂Ph)Cl₂] (3), [Sb(2Bz4oClPh)Cl₂] (4), [Sb(2Bz4oFPh)Cl₂] (5) and [Sb(2Bz4oNO₂Ph)Cl₂] (6) were obtained with 2-acetylpyridine-N(4)-ortho-chlorophenyl thiosemicarbazone (H2Ac4oClPh) and its N(4)-ortho-fluor (H2Ac4oFPh) and N(4)-ortho-nitro (H2Ac4oNO₂Ph) analogues, and with the corresponding 2-benzoylpyridine-derived thiosemicarbazones (H2Bz4oClPh, H2Bz4oFPh, H2Bz4oNO₂Ph). The studied compounds are excellent inhibitors of Trypanosoma cruzi growth. H2Bz4oClPh and complexes (4) and (1) were the most trypanosomicidal.Upon coordination of H2Ac4oClPh to antimony(III) in 1, the therapeutic index (TI) goes from 10.58 to 14.35. However, the best values of TI were found for H2Bz4oClPh (TI = 1240) and H2Ac4oNO₂Ph (TI = 773). Structure-activity relationship (SAR) studies did not allow the establishment of correlations between the anti-trypanosomal activity and physico-chemical parameters, but correlations were found between the cytotoxicities and physico-chemical properties.     

1,4-dicyanobutene-bridged binuclear rhodium(I) complexes and their catalytic activities

Reactions of Rh(ClO₄)(CO)(PPh₃)₂ with dicyano olefins, cis-NCCHCH-CH₂CH₂CN (c-DC1B), rans-NCCHCHCH₂CH₂CN (t-DC1B), trans-NCCH₂CHCHCH₂CN (t-DC2B), and NCCH₂CH₂CH₂CN (DCB) produce the binuclear dicationic rhodium(I) complexes, [(CO)(PPh₃)₂RhNCACNRh-(PPh₃)₂(CO)](ClO₄)₂ (NCACN = c-DC1B 1), t-DC1B (2), t-DC2B (3), DCB (4). Complexes 1 and 2 are catalytically active for the hydrognation of c-DC1B and t-DC1B, respectively, to give DCB, while complex 3 catalyze the isomerization of t-DC2B to give c-DC1B and t-DC1B, and the hydrogenation of t-DC2B to DCB at 100°C.     

Diastereoselective reduction of β-keto carbonyl compounds by cultured plant cells

The diastereoselective reduction of β-keto carbonyl compounds such as 2-benzamidomethyl-3-oxobutanoates and 2-methyl-2-(2-propenyl)cyclopentan-1,3-dione by cultured cells of higher plants was investigated. The reduction of the 2-benzamidomethyl-3-oxobutanoates by Parthenocissus tricuspidata diastereoselectively produced the (2R,3S)-2-benzamidomethyl-3-hydroxybutanoates, whereas the reduction by Gossypium hirsutum gave the (2S,3S)-2-benzamidomethyl-3-hydroxybutanoates. The (2R,3S)/(2S,3S) predominance in the reduction with Nicotiana tabacum, Glycine max, and Catharanthus roseus was reversed by the change in the structure of the alkoxyl group in the substrate. On the other hand, the reduction of 2-methyl-2-(2-propenyl)cyclopentan-1,3-dione by P. tricuspidata produced (2R,3S)-3-hydroxy-2-methyl-2-(2-propenyl)cyclopentan-1-one, whereas the reaction by N. tabacum, G. max, C. roseus, and G. hirsutum gave (2S,3S)-3-hydroxy-2-methyl-2-(2-propenyl)cyclopentan-1-one.     

Detailed electron spectrometric study of the ionization of H2 by He* (21 S, 23 S)

The energy spectra of electrons released in thermal energy (≈ 50 meV) ionizing collisions of He*(2¹ S, 2³ S) with H₂ have been measured with high resolution and low background. Based on a detailed data analysis, we report accurate H ₂ ⁺ (v′) vibrational populationsP(v′) for both He*(2¹ S)+H₂(v′=0–10) and He*(2³ S)+H₂(v′=0–15) and the spectral shapeS(ε) for the individual vibrational peaks. The vibrational populationsP(v′) are quite similar to the Franck-Condon factorsf _v ′0 for unperturbed H₂(v″=0)→H ₂ ⁺ (v′) transitions, but, more in detail, the ratiosP(v′)/f _v ′0 show a characteristically differentv′-dependence for He*(2³ S), He*(2¹ S), and HeI_α(58.4 nm) ionization. The vibrational level separations in the He*(2¹ S, 2³ S)+H₂ spectra agree with those in the HeI photoelectron spectrum to within 1–2 meV. The spectral shapesS(ε) are characteristically different for He*(2¹ S)+H₂ and He*(2³ S)+H₂, reflecting the respective differences in the entrance channel potentials, as determined previously in ab initio calculations and from scattering experiments.