1H and 13C NMR assignments of all three isomeric o‐fluoronaphthaldehydes and three o‐fluorophenanthrene aldehydes

Three isomeric o‐fluoronaphthaldehydes, 9‐fluorophenanthrene, and three previously unreported o‐fluorophenanthrene aldehydes were analyzed in detail by multiple NMR techniques to provide unambiguous assignment of structures and resonances. The six aldehydes serve as the key starting materials for novel chiral ligands used in highly enantioselective rhodium‐catalyzed asymmetric hydrogenation reactions. Copyright © 2009 John Wiley & Sons, Ltd.     

A one-pot synthesis and mild cleavage of 2-[2- or 5-(alkylsulfanyl)pyrrol-1-yl]ethyl vinyl ethers by t-BuOK/DMSO: a novel and facile approach to N-vinylpyrroles

Substituted N-[2-(vinyloxy)ethyl]pyrroles, prepared in good yield through an allenic or acetylenic carbanion/isothiocyanate one-pot methodology from 2-(vinyloxy)ethyl isothiocyanate and allyloxyallene, methoxyallene, N,N-dimethyl-2-propyn-1-amine, and 3-methoxy-1-(methylsulfanyl)-1-propyne, are smoothly converted into the corresponding N-vinylpyrroles using t-BuOK/DMSO (room temperature). The reaction proceeds via elimination of vinyl alcohol from the N-[2-(vinyloxy)ethyl] substituent and represents a novel approach to N-vinylpyrroles.     

Study on electronic density topology of various cluster models of Mg/Al hydrotalcite by density functional theory

The geometry and electronic topology properties of Mg/Al hydrotalcite cluster models were comparatively investigated by means of density functional theory at GGA/DND levels. The results suggested that cluster model containing seven octahedral cations was the smallest size to be employed to simulate other properties. The fact that the n+ charge of cluster models containing n aluminum atoms can reflect electronic properties of anionic clay layer sheet. The bond lengths of clusters can be modified by terminating with or without OH~-/H_2O groups in terms of principle of bond order conservation.     

Feasibility of SU-8-based capillary electrophoresis-electrospray ionization mass spectrometry microfluidic chips for the analysis of human cell lysates

Monolithically integrated, polymer (SU-8) microchips comprising an electrophoretic separation unit, a sheath flow interface and an ESI emitter were developed to improve the speed and throughput of proteomics analyses. Validation of the microchip method was performed based on peptide mass fingerprinting and single peptide sequencing of selected protein standards. Rapid, yet reliable identification of four biologically important proteins (cytochrome C, β-lactoglobulin, ovalbumin and BSA) confirmed the applicability of the SU-8 microchips to ambitious proteomic applications and allowed their use in the analysis of human muscle cell lysates. The characteristic tryptic peptides were easily separated with plate numbers approaching 10(6), and with peak widths at half height as low as 0.6 s. The on-chip sheath flow interface was also exploited to the introduction of an internal mass calibrant along with the sheath liquid which enabled accurate mass measurements by high-resolution Q-TOF MS. Additionally, peptide structural characterization and protein identification based on MS/MS fragmentation data of a single tryptic peptide was obtained using an ion trap instrument. Protein sequence coverages exceeding 50% were routinely obtained without any pretreatment of the proteolytic samples and a typical total analysis time from sampling to detection was well below ten minutes. In conclusion, monolithically integrated, dead-volume-free, SU-8 microchips proved to be a promising platform for fast and reliable analysis of complex proteomic samples. Good analytical performance of the microchips was shown by performing both peptide mass fingerprinting of complex cell lysates and protein identification based on single peptide sequencing.     

Triethylantimony(V) complexes with bidentate O,N-, O,O- and tridentate O,N,O′-coordinating o-iminoquinonato/o-quinonato ligands: Synthesis, structure and some properties

The novel triethylantimony(v) o-amidophenolato (AP-R)SbEt₃ (R = i-Pr, 1; R = Me, 2) and catecholato (3,6-DBCat)SbEt₃ (3) complexes have been synthesized and characterized by IR, NMR spectroscopy (AP-R is 4,6-di-tert-butyl-N-(2,6-dialkylphenyl)-o-amidophenolate, alkyl = isopropyl (1) or methyl (2); 3,6-DBCat is 3,6-di-tert-butyl-catecholate). Complexes 1–3 have been obtained by the oxidative addition of corresponding o-iminobenzoquinones or o-benzoquinones to Et₃Sb. The addition of 4,6-di-tert-butyl-N-(3,5-di-tert-butyl-2-hydroxyphenyl)-o-iminobenzoquinone to Et₃Sb at low temperature gives hexacoordinate [(AP-AP)H]SbEt₃ (4) which decomposes slowly in vacuum with the liberation of ethane yielding pentacoordinate complex [(AP-AP)]SbEt₂ (5). [(AP-AP)H]²⁻ is O,N,O′-tridentate amino-bis-(3,5-di-tert-butyl-phenolate-2-yl) dianion and [(AP-AP)]³⁻ is amido-bis-(3,5-di-tert-butyl-phenolate-2-yl) trianion. The decomposition of 4–5 accelerates in the presence of air. o-Amidophenolates 1 and 2 bind molecular oxygen to give spiroendoperoxides Et₃Sb[L-iPr]O₂ (6) or Et₃Sb[L-Me]O₂ (7) containing trioxastibolane rings. This reaction proceeds slowly and reaches the equilibrium at 15–20% conversion five times more than for (AP-R)SbPh₃ analogues. Molecular structures of 1 and 5 were determined by X-ray analysis.     

Synthesis and characterization of new heterocyclic Schiff base palladacycles: Ring activation through N-oxide formation

Reaction of the Schiff base ligand derived from 4-pyridinecarboxaldehyde NC₅H₄C(H)N[2′,4′,6′-(CH₃)C₆H₂], (1), with palladium(II) acetate in toluene at 60 °C for 24 h gave [Pd{NC₅H₄C(H)N[2′,4′,6′-(CH₃)C₆H₂]}₂(OCOCH₃)₂], (2), with two ligands coordinated through the pyridine nitrogen. Treatment of the Schiff base ligand derived from 4-pyridinecarboxaldehyde N-oxide, 4-(O)NC₅H₄C(H)N[2′,4′,6′-(CH₃)C₆H₂], (4), with palladium(II) acetate in toluene at 75 °C gave the dinuclear acetato-bridged complex [Pd{4-(O)NC₅H₃C(H)N[2′,4′,6′-(CH₃)C₆H₂]}(OCOCH₃)]₂, (5) with metallation of an aromatic phenyl carbon. Reaction of complex 5 with sodium chloride or lithium bromide gave the dinuclear halogen-bridged complexes [Pd{4-(O)NC₅H₃C(H)N[2′,4′,6′-(CH₃)C₆H₂]}(Cl)]₂, (6) and [Pd{4-(O)NC₅H₃C(H)N[2′,4′,6′-(CH₃)C₆H₂]}(Br)]₂, (7), after the metathesis reaction. Reaction of 6 and 7 with triphenylphosphine gave the mononuclear species [Pd{4-(O)NC₅H₃C(H)N[2′,4′,6′-(CH₃)C₆H₂]}(Cl)(PPh₃)], (8) and [Pd{4-(O)NC₅H₃C(H)N[2′,4′,6′-(CH₃)C₆H₂]}-(Br)(PPh₃)], (9), as air stable solids. Treatment of 6 and 7 with Ph₂P(CH₂)₂PPh₂ (dppe) in a complex/diphosphine 1:2 molar ratio gave the mononuclear complexes [Pd{4-(O)NC₅H₃C(H)N[2′,4′,6′-(CH₃)C₆H₂]}(PPh₂(CH₂)₂PPh₂)][Cl], (10), and [Pd{4-(O)NC₅H₃C(H)N[2′,4′,6′-(CH₃)C₆H₂]}(PPh₂(CH₂)₂PPh₂)][PF₆], (11), with a chelating diphosphine. The molecular structure of complex 9 was determined by X-ray single crystal diffraction analysis.     

Secreted proteome of the murine multipotent hematopoietic progenitor cell line DKmix

Administration of the multipotent hematopoietic progenitor cell (HPC) line DKmix improved cardiac function after myocardial infarction and accelerated dermal wound healing due to paracrine mechanisms. The aim of this study was to analyse the secreted proteins of DKmix cells in order to identify the responsible paracrine factors and assess their relevance to the wide spectrum of therapeutic effects. A mass spectrometry (MS)‐based approach was used to identify secreted proteins of DKmix cells. Serum free culture supernatants of DKmix‐conditioned medium were collected and the proteins present were separated, digested by trypsin and the resulting peptides were then analyzed by matrix‐assisted laser desorption/ionization tandem time‐of‐flight (MALDI‐TOF/TOF) MS. Overall 95 different proteins were identified. Among them, secretory proteins galectin‐3 and gelsolin were identified. These proteins are known to stimulate cell migration and influence wound healing and cardiac remodelling. The remaining proteins originate from intracellular compartments like cytoplasm (69%), nucleus (12%), mitochondria (4%), and cytoplasmic membrane (3%) indicating permeable or leaky DKmix cells in the conditioned medium. Additionally, a sandwich immunoassay was used to detect and quantify cytokines and chemokines. Interleukin‐6 (IL‐6), interleukin‐13 (IL‐13), monocyte‐chemoattractant protein‐1 (MCP‐1), monocyte‐chemoattractant protein‐3 (MCP‐3), monocyte‐chemoattractant protein‐1α (MIP‐1α) and monocyte‐chemoattractant protein‐1β (MIP‐1β) were detected in low concentrations. This study identified a subset of proteins present in the DKmix‐conditioned medium that act as paracrine modulators of tissue repair. Moreover, it suggests that DKmix‐derived conditioned medium might have therapeutic potency by promoting tissue regeneration. Copyright © 2010 John Wiley & Sons, Ltd.     

Quantum chemical metabolism‐based simulation of carcinogenic potency of benzene derivatives

Using an oxenoid model, we investigated dependences of carcinogenic potency of the benzenes C₆H₅‐X on a nature of substituents X. According to the model, a P450 enzyme breaks a dioxygen molecule and generates the oxens, which readily react with substrates. We suggest that a stability of the intermediate OC₆H₆‐X with tetrahedrally coordinated C atom relative to the molecule C₆H₅‐X determines a rate of substrate biotransformation. Using MO LCAO MNDO approach, we calculated the total energies of molecules C₆H₆‐X and arene oxides OC₆H₆‐X. A difference ΔE_min of these values determines activation energy of oxidation reaction. The compounds with the low ΔE_min values are noncarcinogenic. Benzene derivatives with high ΔE_min values belong to carcinogenic compounds series. The carcinogenicity of amino‐ and nitro‐substituted benzenes is also determined by N‐oxidation of amino and reduction of the nitro group. As the phenylhydroxylamines XC₆H₄NHOH and nitrenium ions XC₆OH₄NH⁺ are the common metabolites of the nitro‐ and amino‐substituted benzenes and nitrenium ions XC₆H₄NH⁺ are the ultimate carcinogens, we use the differences ΔE_N = E(XC₆H₄NH⁺) ? E(XC₆H₄NHOH) as the second parameter characterizing the carcinogenic activity of amino‐ and nitro‐substituted benzenes. © 2009 Wiley Periodicals, Inc. Int J Quantum Chem, 2010