Über die kationische Wirksamkeit von Salzen organischer Basen

Zusammenfassung Die kationische Wirksamkeit von Salzen aromatischer, aliphatisch-aromatischer und rein aliphatischer Amine bei der Phenolätherspaltung wird verglichen. Neben der Diskussion des Reaktionsmechanismusses werden die ermittelten Gesetzmäßigkeiten mit den Haftfestigkeiten der SO₂–N-Bindungen von Tosylderivaten der entsprechenden Amine gegenüber kationisch wirkenden Agenzien in bezug gebracht und Zusammenhänge zwischen der kationischen Wirkung der Salze bzw. der Basizität der zugrunde liegenden Amine und der genannten Bindungsfestigkeit aufgezeigt.     

Fettuntersuchung

Ohne Zusammenfassung     

C–H⋅<Emphasis Type="Italic">s</Emphasis>O hydrogen bond networks in <Emphasis Type="Italic">E</Emphasis>- and Z-unsaturated esters of C-glycosides

Methyl E(Z)-4,7 anhydro-5-benzamido-6,8-di-O-benzoyl-2,3,5-trideoxy-d-allo-oct-2-enoate have been synthesized like intermediates and isolated as single crystals during the synthesis of pyrazole-related C nucleosides as synthetic product with cytotoxic activity.¹ Crystal structures of E(Z) isomers were determined by X-ray analysis. E isomer crystallizes in the triclinic crystal system, space group P1, a = 5.319(1) Å, b = 10.758(2) Å, c = 12.229(2) Å, α = 72.38(2)^∘, β = 89.97(2)^∘, γ = 87.07(2)^∘, D_x = 1.320 Mgm⁻³ and Z isomer in the orthorhombic crystal system, space group P2₁2₁2₁, a = 5.1297(13) Å, b = 19.667(5) Å, c = 25.871(6) Å, D_x = 1.348 Mgm⁻³. The molecular structure was solved by direct method on the basis of 2609 and 2727 unique reflections recorded at the temperature 293 K (E-isomer) and 173 K (Z-isomer) up to the final R-factor 0.0378 and 0.0435, respectively. C–H⋅sO contact networks were analyzed and the correlation established between the existence of the weak C–H⋅sO hydrogen bonds and the melting point of the single crystals.     

Asymmetric intermolecular Stetter reactions catalyzed by a novel triazolium derived N-heterocyclic carbene

The asymmetric intermolecular Stetter reaction is catalyzed by a novel triazolium salt derived N-heterocyclic carbene leading to 1,4-diketones in moderate to excellent yields (49-98%) and moderate to good enantioselectivities (56-78% ee), which could be enhanced by one recrystallization to excellent levels (90-99% ee).     

Internal structure of a thin film of mixed polymeric micelles on a solid/liquid interface

The adsorption of mixed micelles of poly(4-(2-amino hydrochloride-ethylthio)-butylene)- block-poly(ethylene oxide), PAETB 49- b-PEO 212 and poly(4-(2-sodium carboxylate-ethylthio)-butylene)- block-poly(ethylene oxide), PCETB 47- b-PEO 212 on solid/liquid interfaces has been studied with light, X-ray, and neutron reflectometry. The structure of the adsorbed layer can be described with a two-layer model consisting of an inner layer formed by the coacervate of the polyelectrolyte blocks PAETB 49 and PCETB 47 ( approximately 1 nm) and an outer layer of PEO 212 blocks ( approximately 6 nm). The micelles unfold upon adsorption forming a rather homogeneous flat layer that exposes its polyethylene oxide chains into the solution, thus rendering the surface antifouling after modification with the micelles.     

Quantitative multiresidue method for about 100 veterinary drugs in different meat matrices by sub 2-microm particulate high-performance liquid chromatography coupled to time of flight mass spectrometry

A quantitative multiresidue method covering more than 100 veterinary drugs, belonging to different drug families, has been developed. The proposed approach uses an liquid-liquid-solid extraction technique (bi-polarity extraction) which is capable in recovering polar, medium polar and apolar compounds. A thorough generic reversed phase solid-phase extraction (SPE) clean-up removes interfering proteins and provides clean and stable extracts. Dedicated rinsing steps are proposed to reduce analyte adsorption on glass walls and on precipitating proteins. The resulting extract is analyzed by ultra-performance liquid chromatography (UPLC) coupled to time of flight mass spectrometry (TOF). The method was validated according to the Commission Decision 2002/657/EEC. Validation coved the relevant meat matrices (muscle, kidney and liver).     

Stable ion and electrophilic chemistry of the sterically crowded stilbene 1,1'-Bi(benzocyclobutenylidene) and its derivatives

Generation and NMR studies of novel carbocations and carboxonium ions are reported from sterically hindered stilbene 1,1'-bi(benzocyclobutenylidene) 1, its dimethoxy derivative 5, and from their skeletally rearranged derivatives, namely, the spirocyclic ketone 6, diastereomeric alcohols 7 and isomeric diols 8. Quenching experiments on the carbocations under various conditions resulted in the formation/isolation of several novel covalent adducts. Acid-catalyzed isomerization of the diols 8 produced a remarkable dimeric molecule, whose structure was confirmed by X-ray analysis. Reactions of hindered stilbenes 1 and 5 with Br 2/CDCl 3 were examined via NMR experiments. The experimentally observed carbocations were also studied computationally by GIAO-DFT and by NICS.     

Enantiotopos-differentiating (-)-sparteine-mediated gamma-deprotonation of 1-alkenyl carbamates: DFT calculations verify the observed stereoselectivity

The enantioselective lithiation/gamma-deprotonation of three 1-alkenyl N,N-diisopropylcarbamates 6 by alkyllithium/(-)-sparteine has been modeled by the DFT method B3LYP/6-31G(d). The results of these calculations predict the preferential removal of the gamma-pro-R proton from the precomplexes 7 to give the (S)-lithio derivates 8. The calculations also indicate the necessity of an anion-stabilizing substituent (Ph, -CC-Ph) in the alpha-position of the substrate. These data are in excellent concordance with the experimental results. It is demonstrated that the formation and the properties of lithium carbanions are predictable with high accuracy by standard quantum chemical calculations if these species are monomeric and rigidified to some extent by chelation.     

Synthesis and Characterization of Diorganocobalt Chlorides by Aliphatic Vinylic C–Cl Bond Activation

Three diorganocobalt chlorides [CoClMe(PMe₃)₂–{(C₅H₆)–CH=O}] ( 4 ), [CoClMe(PMe₃)₂–{(C₆H₈)–CH=O}] ( 5 ), and [CoClMe(PMe₃)₂–{(C₆H₇Memeta)–CH=O}] ( 6 ) were synthesized through cyclometalation reactions with aldehyde as an anchoring group involving aliphatic vinylic C–Cl bond activation. Complexes 4 – 6 were characterized by IR and NMR spectroscopy. The crystal and molecular structures of complexes 4 and 5 were determined by single‐crystal X‐ray diffraction. Complexes 4 – 6 are stable in solution at room temperature, but they decompose at above 30 °C affording C,C‐couplings products with the formation of [Co(PMe₃)₃Cl]. The results of this work will be important for people to deepen the understanding of the C–Cl bond activation mechanism.     

Ca2+‐complex stability of GAPAGPLIVPY peptide in gas and aqueous phase,investigated by affinity capillary electrophoresis and molecular dynamics simulations and compared to mass spectrometric results

Strong, sequence‐specific gas‐phase bindings between proline‐rich peptides and alkaline earth metal ions in nanoESI‐MS experiments were reported by Lehmann et al. (Rapid Commun. Mass Spectrom. 2006, 20, 2404–2410), however its relevance for physiological‐like aqueous phase is uncertain. Therefore, the complexes should also be studied in aqueous solution and the relevance of the MS method for binding studies be evaluated. A mobility shift ACE method was used for determining the binding between the small peptide GAPAGPLIVPY and various metal ions in aqueous solution. The findings were compared to the MS results and further explained using computational methods. While the MS data showed a strong alkaline earth ion binding, the ACE results showed nonsignificant binding. The proposed vacuum state complex also decomposed during a molecular dynamic simulation in aqueous solution. This study shows that the formed stable peptide–metal ion adducts in the gas phase by ESI‐MS does not imply the existence of analogous adducts in the aqueous phase. Comparing peptide–metal ion interaction under the gaseous MS and aqueous ACE conditions showed huge difference in binding behavior.