Recognition of carboxylate and dicarboxylates by azophenol–thiourea derivatives: a theoretical host–guest investigation

Geometries of azophenol–thiourea derivative complexes with acetate, oxalate, malonate, succinate, glutarate, adipate, pimelate, suberate and azelate were carried out using the integrated MO:MO method. The binding and complexation energies of these complexes were derived from the ONIOM(B3LYP/6-31G(d):AM1) calculations. The relative stabilities of the complexes of azophenol–thiourea derivatives with carboxylate guests are reported. The binding interactions of the azophenol–thiourea receptor 1, 2 and carboxylate guests are described as multipoints hydrogen bonding, where the amine and phenolic hydrogen atoms of receptors act as hydrogen bond donors in complex with acetate and all amine-hydrogen and phenolic hydrogen atoms act as hydrogen bond donors in complex with dicarboxylate guests. Thermodynamic properties of binding interactions between receptors 1, 2 and their preorganizations and complexations are also reported.     

Armed-disarmed effect of remote protecting groups on the glycosylation reaction of 2,3-dideoxyglycosyl donors

The armed-disarmed effect of remote protecting groups at the C-4 and/or C-6 position(s) on the glycosylation reactions of 2,3-dideoxyglycosyl donors was investigated. It was found that under various glycosylation conditions, 4- or 6-O-Bn 2,3-dideoxyglycosyl donors were much more reactive than the corresponding 4,6-di-O-Bz 2,3-dideoxyglycosyl donors. Based on these results, an effective and chemoselective glycosylation reaction using 4,6-di-O-Bn glycosyl acetate and 4-OH-6-O-Bz glycosyl acetate was realized, producing a 2,3-dideoxydisaccharide in good yield with high α-stereoselectivity.     

New chiral organosulfur donors related to bis(ethylenedithio)tetrathiafulvalene

Six new enantiopure chiral organosulfur donors, with structures related to BEDT-TTF, have been synthesised for use in the preparation of organic metals, starting either by double nucleophilic substitutions on the bis-mesylate of 2R,4R-pentane-2,4-diol or by a cycloaddition with subsequent elimination of acetic acid on the enol acetate of (+)-nopinone. Crystal structures of some of their radical cation triiodides salts and TCNQ complexes are reported.     

Binary Mixtures of Aprotic and Protic Ionic Liquids Demonstrate Synergistic Polarity Effect: An Unusual Observation

In this communication, we demonstrate the solute–solvent and solvent–solvent interactions in the binary mixtures of two aprotic ionic liquids, namely 1-butyl-3-methylimidazolium bis(trifluoromethylsulfonyl)imide and 1-butyl-1-methylpyrrolidinium bis(trifluoromethylsulfonyl)imide, with the protic ionic liquid 1-methylimidazolium acetate. The synergistic effects as expressed by the solvatochromic parameter are noted. This observation is in contrast to the mixing of protic ionic liquids 1-methylpyrrolidium acetate and 4-methylmorpholine acetate with 1-methylimidazolium acetate, respectively. It appears that the synergistic effects in the binary mixtures of aprotic and protic ionic liquids are caused by the formation of hydrogen bonds, since cations are dominant H-bond donors while anions are dominant H-bond acceptors. Preferential solvation models are used to describe the solute–solvent interactions in the binary ionic liquid mixtures.     

Molecular modeling for Cu(II)‐aminopolycarboxylate complexes: Structures,conformational energies,and ligand binding affinities

A ligand field molecular mechanics (LFMM) force field (FF) has been developed for d⁹ copper(II) complexes of aminopolycarboxylate ligands. Training data were derived from density functional theory (DFT) geometry optimizations of 14 complexes comprising potentially hexadentate N₂O₄, tetrasubstituted ethylenediamine (ed), and propylenediamine cores with various combinations of acetate and propionate side arms. The FF was validated against 13 experimental structures from X‐ray crystallography including hexadentate N₂O₄ donors where the nitrogens donors are forced to be cis and bis‐tridentate ONO ligands which generate complexes with trans nitrogen donors. Stochastic conformational searches for [Cu{ed(acetate)_n (propionate)_4‐n}]^2?, n = 0–4, were carried out and the lowest conformers for each system reoptimized with DFT. In each case, both DFT and LFMM predict the same lowest‐energy conformer and the structures and energies of the higher‐energy conformers are also in satisfactory agreement. The relative interaction energies for n = 0, 2, and 4 computed by molecular mechanics correlate with the experimental log β binding affinities. Adding in the predicted log β values for n = 1 and 3 suggest for this set of complexes a monotonic decrease in log β as the number of propionate arms increases. © 2013 Wiley Periodicals, Inc.     

Efficient synthesis of Man2, Man3, and Man5 oligosaccharides, using mannosyl iodide donors

[reaction: see text] A highly efficient protocol for making Man(3) and Man(5) oligosaccharides with use of orthogonally protected glycosyl iodide donors has been developed. Glycosylation of a C-2-O-acetyl mannosyl iodide donor in the presence of silver triflate at -40 degrees C initially gave a mixture of the desired alpha-linked mannoside and an orthoacetate resulting from attack at the C-2 acetate. However, upon warming to room temperature the orthoacetate quantitatively rearranged to the desired oligosaccharide. Employing a 3,6-dihydroxy acceptor and subjecting it to double glycosidation quickly afforded high mannose sugars in nearly quantitative yields. Glycosyl iodide donors offer advantages over previously reported chloride donors as the reactions are faster, proceed in higher yields, and are not diminished in higher order constructs. These studies continue to dispel the notion that glycosyl iodides are too reactive to be of synthetic utility.     

2',7'-Difluorofluorescein excited-state proton reactions: correlation between time-resolved emission and steady-state fluorescence intensity

The presence of excited-state buffer-mediated proton exchange reactions influences the steady-state fluorescence signals from dyes in solution. Since biomolecules in general have some chemical groups that can act as proton acceptors/donors and are usually dissolved in buffer solutions which can also behave as appropriate proton acceptors/donors, the excited-state proton exchange reactions may result in distorted steady-state fluorescence signals. In a previous paper (J. Phys. Chem. A 2005, 109, 734-747), we evaluated kinetic and other pertinent parameters for the excited-state proton reactions of the prototropic forms of 2',7'-difluorofluorescein (Oregon Green 488, OG488), recording a fluorescence decay surface at different pH values and acetate buffer concentrations, analyzed by means of global compartmental analysis. In this article we use the rate constants and the corrected pre-exponential factors from the previously recorded fluorescence decay traces to simulate the decay times and associated pre-exponentials at different acetate buffer concentrations and constant pH and compare these theoretically calculated values with new experimental data. We also calculate the steady-state fluorescence intensity vs pH and vs acetate buffer concentration (at constant pH) and compare these calculated emission values with the experimental data previously published. The agreement between the experimental and simulated data is excellent.     

A new glycosylation method part 3: study of microwave effects at low temperatures to control reaction pathways and reduce byproducts

The efficiency of microwave irradiation at low temperature for glycosylations is described. Although oligosaccharide synthesis usually requires reactive donors for glycosylations, which have leaving groups on the anomer positions, i.e., trichloroacetoimidates, halogenates, thioalkyl glycosides, etc., the suitable donors in our microwave supported synthesis of Lewis X oligosaccharide were very stable acetate derivatives. Regarding glycosylation with a fucosyl acetate donor and a glucosamine acceptor, microwave irradiation with simultaneous cooling improved yields. Moreover, further synthesis to Lewis X derivatives was achieved only with microwave irradiation at low temperatures. Without microwave irradiation, we could only obtain byproducts and none of the designed product at any reaction temperature.     

Consumption of 2-Chlorophenol Using Anaerobic Sludge: Physiological and Kinetic Analysis

Chlorophenols are toxic and recalcitrant compounds produced by many industrial. Different strategies have been used to improve their biological consumption, but there is insufficient information to understand how the process is carried out. The objective of this study was to evaluate in batch tests the effect of the addition of phenol, acetate, or glucose as electron donors at different concentrations on the efficiencies, yields, and specific rates of 2-chlorophenol (2-CP) consumption. The addition of phenol (177.6 mg C/L), acetate (127.6 mg C/L), or glucose (77.6 mg C/L) increased the 2-CP consumption efficiency up to 54.6, 98.6, and 97.8 %, respectively. With respect to the control assay without electron donor, the specific rate of 2-CP consumption was up to 2.5 times higher with phenol (177.6 mg C/L), 8.4 times higher with acetate (127.6 mg C/L), and 3 times higher with glucose (127.6 mg C/L). The results showed that the type and concentration of electron donor determine the physiological behavior of the anaerobic sludge, modifying efficiency, yield, and specific rate values of the 2-CP consumption process. The addition of readily oxidable cosubstrates seems to be a good alternative and might be used for the biological treatment of industrial wastewater polluted with chlorinated phenols.     

Polyaniline-Anchored Metal Salts for Michael Reaction of α,β-Unsaturated Ketones

A catalyst consisting of polyaniline-anchored metal salts is used as a Lewis acid to promote the Michael reaction of α,β-unsaturated ketones. The reaction is performed efficiently with imidazole, acetyl acetone, and ethyl acetate as Michel donors and chalcones as the acceptors under ultrasound irradiation.     

Synthesis of stigmasteryl (β1→4)-oligoglucosides

Stigmasteryl (β1→4)-oligoglucosides were prepared with cellobiose, cellotriose, and cellotetraose as glycan chains. For the preparation of the peracetylated oligoglucosyl donors anomeric acetate was deprotected and the respective hemiacetals were converted into trichloroacetimidates. Glycosylation with stigmasterol yielded both α- and β-anomers because during the treatment with Lewis acid the 2-OAc is cleaved to some extent; thus, with the emerging hydroxyl group neighboring group participation does not take place. Due to their different number of hydroxyl groups (0 vs. 1) separation of the two products proved to be facile. Saponification led to the desired stigmasteryl glucosides.     

Evaluation of triproline and tri-α-methylproline chiral stationary phases: Retention and enantioseparation associated with hydrogen bonding

In this study, to demonstrate preparation strategy and improve understanding of chiral recognition mechanisms, triproline chiral stationary phases (CSPs) were evaluated with a series of analytes classified as having none, one, two or three H-bond donors. The average retention factors and mobile phase strength generally followed none < one < two < three hydrogen bond donors. The average solvent volume ratio (H_r stands for average hexane volume ratio in the mobile phase, Hp_r for heptane, ACN_r for acetonitrile, or H₂O_r for water) normalized chromatographic parameters calculated for di-, tri-, tetra-, penta-, hexa-, and decaproline CSPs facilitated the characterization of properties associated to the H-bond donor categorization. The H_r of triproline CSP were 1.0, 0.96 and 0.88 for analyte of none, one and two hydrogen bond donors with hexane/2-propanol mobile phase, respectively. The number of hydrogen bond donors in an analyte was found to be a primary factor in influencing the retention and enantioseparation in the normal-phase and polar organic modes. Two H-bond acceptor solvents methyl tert-butyl ether and ethyl acetate increased chiral separation on oligoproline CSPs for some compounds. The role of carbon-donor hydrogen bonding at the H atom of proline asymmetric center was implied through testing a tri-α-methylproline stationary phase. On oligoproline CSPs, three factors including adjacent hydrogen bond acceptor and carbon-donor, and a rigid proline residue chain were recognized as important for contributing to the broad enantioselectivity. The α hydrogen atom on chiral center of stationary phase was found to play a crucial role in enantiomeric discrimination.     

Palladium-catalyzed and samarium-promoted coupling of stereochemically-biased allylic acetates with carbonyl compounds

Stereochemically-biased bicyclic allylic acetates endo- and exo-1 were shown as being allyl donors for Pd-catalyzed carbonyl allylation using stoichiometric quantities of samarium diodide. Cyclopentenyl acetate and bicyclic derivatives 1 react with cyclic ketones in the presence of SmI₂ without requirement of palladium catalysis. Use of enantiomerically enriched substrate suggests that the reaction goes through a π-allyl samarium complex. However, this reactivity appears to be restricted to strained cyclopentenyl acetates since other linear and cyclic allylic acetates do not give the carbonyl allylation product.     

Lipase catalysis in the preparation of 3-(1-amino-3-butenyl)pyridine enantiomers

The kinetic resolution of 1-(3-pyridyl)buten-3-ylamine with activated and non-activated acyl donors and Burkholderia cepacia lipase (lipase PS-D) under dry conditions has been studied. The N-acylation in isopropyl acetate (E >100) and the acidic hydrolysis of the (R)-amide produced gave the corresponding enantiomerically enriched amines.     

A practical palladium catalyzed dehalogenation of aryl halides and α-haloketones

A practical and high-yielding protocol for the dehalogenation of aromatic halides is presented. In the presence of palladium acetate, triphenylphosphine, and potassium carbonate, a number of highly functionalized aromatic halides as well as α-haloketones were dehalogenated with alcohols as hydrogen donors.     

A highly efficient d-fructofuranosylation catalyzed by scandium(III) triflate

This Letter describes a highly efficient d-fructofuranosylation catalyzed by scandium(III) triflate. The benzylated and benzoylated d-fructofuranosyl acetate derivatives worked as good reactive donors in the presence of only 5 mol % scandium(III) triflate at 0 °C in toluene to afford the d-fructofuranosides in excellent yields. The fructofuranosylation also produced several non-reducing disaccharides of sucrose mimics using several aldopyranose derivatives as the acceptors.     

The scope of ambiphilic acetate-assisted cyclometallation with half-sandwich complexes of iridium, rhodium and ruthenium

C? H activation by acetate‐assisted cyclometallation of a phenyl group with half‐sandwich complexes [{MCl₂Cp*}₂] (M=Ir, Rh) and [{RuCl₂(p‐cymene)}₂] can be directed by a wide range of nitrogen donor ligands including pyrazole, oxazoline, oxime, imidazole and triazole, and X‐ray structures of a number of complexes are reported. All the ligands tested cyclometallated at iridium, however ruthenium and rhodium fail to cause cyclometallation in some cases. As a result, the nitrogen donors have been categorised based on their reactivity with the three metals used. The relevance of these cyclometallation reactions to catalytic synthesis of carbocycles and heterocycles is discussed.     

4,4′‐Methylenediphenol–4,4′‐bipyridine (2/3): decarboxylation of 5,5′‐methylenedisalicylic acid under hydrothermal conditions

Reaction of 5,5′‐methylenedisalicylic acid (5,5′‐H₄mdsa) with 4,4′‐bipyridine (4,4′‐bipy) and manganese(II) acetate under hydrothermal conditions led to the unexpected 2:3 binary cocrystal 4,4′‐methylenediphenol–4,4′‐bipyridine (2/3), C₁₃H₁₂O₂·1.5C₁₀H₈N₂ or (4,4′‐H₂dhdp)(4,4′‐bipy)_1.5, which is formed with a concomitant decarboxylation. The asymmetric unit contains one and a half 4,4′‐bipy molecules, one of which straddles a centre of inversion, and one 4,4′‐H₂dhdp molecule. O—H...N interactions between the hydroxy and pyridyl groups lead to a discrete ribbon motif with an unusual 2:3 stoichiometric ratio of strong hydrogen‐bonding donors and acceptors. One of the pyridyl N‐atom donors is not involved in hydrogen‐bond formation. Additional weak C—H...O interactions between 4,4′‐bipy and 4,4′‐H₂dhdp molecules complete a two‐dimensional bilayer supramolecular structure.     

Acetonitrile hydration and ethyl acetate hydrolysis by pyrazolate-bridged cobalt(II) dimers containing hydrogen-bond donors

The preparation of new CoII-mu-OH-CoII dimers with the binucleating ligands 3,5-bis{bis[(N'-R-ureaylato)-N-ethyl]aminomethyl}-1H-pyrazolate ([H4PRbuam]5-, R=tBu, iPr) is described. The molecular structure of the isopropyl derivative reveals that each CoII center has a trigonal-bipyramidial coordination geometry, with a Co...Co separation of 3.5857(5) A. Structural and spectroscopic studies show that there are four hydrogen-bond (H-bond) donors near the CoII-micro-OH-CoII moiety; however, they are too far away to be form intramolecular H-bonds with the bridging hydroxo ligand. Treating [CoII2H4PRbuam(micro-OH)]2- with acetonitrile led to the formation of bridging acetamidato complexes, [CoII2H4PRbuam(micro-1,3-OC(NH)CH3)]2-; in addition, these CoII-micro-OH-CoII dimers hydrolyze ethyl acetate to form CoII complexes with bridging acetato ligands. The CoII-1,3-micro-X'-CoII complexes (X'=OAc-, [OC(NH)CH3]-) were prepared independently by reacting [CoII2H3PRbuam]2- with acetamide or [CoII2H4PRbuam]- with acetate. X-ray diffraction studies show that the orientation of the acetate ligand within the H-bonding cavity depends on the size of the R substituent appended from the urea groups. The tetradentate ligand 3-{bis[(N'-tert-butylureaylato)-N-ethyl]aminomethyl}-5-tert-butyl-1H-pyrazolato ([H2PtBuuam]3-) was also developed and its CoII-OH complex prepared. In the crystalline state, [CoIIH2PtBuuam(OH)]2- contains two intramolecular H-bonds between the urea groups of [H2PtBuuam]3- and the terminal hydroxo ligand. [nPr4N]2[CoIIH2PtBuuam(OH)] does not hydrate acetonitrile or hydrolyze ethyl acetate. In contrast, K2[CoIIH2PtBuuam(OH)] does react with ethyl acetate to produce KOAc; this enhanced reactivity is attributed to the presence of the K+ ions, which can possibly interact with the CoII-OH unit and ester substrate to assist in hydrolysis. However, K2[CoIIH2PtBuuam(OH)] was still unable to hydrate acetonitrile.     

Practical ruthenium/lipase-catalyzed asymmetric transformations of ketones and enol acetates to chiral acetates

Ketones were asymmetrically transformed to chiral acetates by one-pot processes using a lipase and an achiral ruthenium complex under 1 atm of hydrogen gas in ethyl acetate. Molecular hydrogen was also effective for the transformation of enol acetates to chiral acetates without additional acyl donors with the same catalyst system.