Synthesis and evaluation of the catalytic properties of semicarbazides derived from N-triphenylmethyl-aziridine-2-carbohydrazides

A straightforward synthesis of a series of new catalysts derived from N-triphenylmethyl-aziridine-2-carbohydrazides is described. The new compounds have been tested for the enantioselective addition of diethyl- and phenylethynylzinc to aryl and alkyl aldehydes, which afforded the corresponding chiral alcohols in high chemical yields (up to 92%) and with excellent ee’s of approximately 90%.     

Profiling primaquine metabolites in primary human hepatocytes using UHPLC‐QTOF‐MS with 13C stable isotope labeling

Therapeutic efficiency and hemolytic toxicity of primaquine (PQ), the only drug available for radical cure of relapsing vivax malaria are believed to be mediated by its metabolites. However, identification of these metabolites has remained a major challenge apparently due to low quantities and their reactive nature. Drug candidates labeled with stable isotopes afford convenient tools for tracking drug‐derived metabolites in complex matrices by liquid chromatography‐tandem mass spectrometry (LC‐MS‐MS) and filtering for masses with twin peaks attributable to the label. This study was undertaken to identify metabolites of PQ from an in vitro incubation of a 1:1 w/w mixture of ¹³C₆‐PQ/PQ with primary human hepatocytes. Acquity ultra‐performance LC (UHPLC) was integrated with QTOF‐MS to combine the efficiency of separation with high sensitivity, selectivity of detection and accurate mass determination. UHPLC retention time, twin mass peaks with difference of 6 (originating from ¹³C₆‐PQ/PQ), and MS‐MS fragmentation pattern were used for phenotyping. Besides carboxy‐PQ (cPQ), formed by oxidative deamination of PQ to an aldehyde and subsequent oxidation, several other metabolites were identified: including PQ alcohol, predictably generated by oxidative deamination of PQ to an aldehyde and subsequent reduction, its acetate and the alcohol's glucuronide conjugate. Trace amounts of quinone‐imine metabolites of PQ and cPQ were also detected which may be generated by hydroxylation of the PQ/cPQ quinoline ring at the 5‐position and subsequent oxidation. These findings shed additional light on the human hepatic metabolism of PQ, and the method can be applied for identification of reactive PQ metabolites generated in vivo in preclinical and clinical studies. Copyright © 2013 John Wiley & Sons, Ltd.     

Phase transformation in shape memory alloys: a numerical approach for thermomechanical modeling via peridynamics

Meccanica - The work is devoted to the numerical aspects of the modeling tool elaborated to simulate the phenomenon of solid phase transformation in shape memory alloys. Particularly, a nonlocal...     

Synthesis and structural, spectroscopic, and electrochemical characterization of benzo[c]quinolizinium and its 5-aza-, 6-aza, and 5,6-diaza analogues

Four heterocyclic salts 1a-d were prepared by Ca²⁺-assisted cyclization of fluoro derivatives 3, and investigated by spectroscopic (NMR and UV), electrochemical, and computational (DFT and MP2) methods. The mechanism for the formation of the cations was investigated at the DFT level of theory. 2-D NMR spectroscopy for 1[ClO₄] in DMSO­d₆ aided with DFT results permitted the assignment of ¹H and ¹³C NMR signals in cations 1. The molecular and crystal structures for 1a[ClO₄] [C₁₃H₁₀ClNO₄ triclinic, P−1, a=9.6517(12) Å, b=11.0470(13) Å, c=12.2373(15) Å, α=67.615(1)°, β=78.845(2)°, γ=87.559(2)°; V=1183.0(2) Å³, Z=4] and 1d[ClO₄] [C₁₂H₉ClN₂O₄ triclinic, P−1, a=5.9525(6) Å, b=8.3141(9) Å, c=12.2591(13) Å, α=73.487(1)°, β=83.814(1)°, γ=83.456(1)°; V=576.07(10) Å³, Z=2] were determined by X-ray crystallography and compared with results of DFT and MP2 calculations. Electrochemical analysis gave the reduction potential order (1b>1c∼1d>1a), which is consistent with computational results.     

Chiral imines prepared from 1-(2-aminoalkyl)aziridines as novel chiral shifts reagents for efficient recognition of acids

Optically pure, chiral imines synthesized from the corresponding aldehydes and 1-(2-aminoalkyl)aziridines in good chemical yields, have been assessed as an NMR chiral shift reagents for effective discrimination of the signals of some acids (mandelic acid and its derivatives and N-protected amino acid). The title compounds have proven to be very useful for the determination of enantiomeric purity and absolute configuration of the aforementioned acid derivatives.     

Further studies on the stereochemistry of sparteine, its isomers and derivatives : Part. I. Synthesis, structure and properties of 16,17-endo-methylene-lupaniumm perchlorate, 17-β-methyllupanine and 17-β-methylsparteine

The reduction of the product (V) obtained from the reaction of δ^16,17-dehydro- lupaninium perchlorate with diazomethane leads to 17-β-methyllupanine (III) (NaBH₄- reduction) or to 17-β-methylsparteine (X) (LiAlH₄-reduction). The structures of III and X were determined by spectroscopic methods (NMR and IR) and further proved by chemical methods. The β-methyl group at C-17 has a pronounced effect on the basicity of III and X. The basicity of in is higher than that of its parent lupanine by about 1.5 pK^*_MCSunits which can be explained by additional stabilization of the C/D boat-chair conformation in III and better solvation conditions than in lupanine. The same effect leads to a decrease of the δpK^*_MCS-value of the diamine X with reference to that of sparteine by ca. 2.6 units. The methyl group in X stabilizes the C/D boat-chair conformation and hinders the formation of an intramolecular hydrogen bond in monoprotonated X, consequently the addition of a second proton is favoured and it is assumed that the diprotonated cations of X and sparteine have different conformations. The reaction intermediate 16,17-endo-methylenelupaninium perchlorate (V) was isolated and its structure was determined.     

Further studies on the chemistry and structure of n-oxides of sparteine and its derivatives—V: Synthesis and structure of 2-phenylsparteine-n16-oxide,a new case of “sponge” proton

The synthesis of 2-phenylsparteine-N₁₆-oxide (7) and its perchlorate salt (7-H⁺) was carried out. On the basis of spectral data, and by comparison with appropriate sparteine-N-oxides, the mechanism of formation and the structures of the two new compounds were proposed. It was found, the basicity of the new N-oxide is unexpectedly high and comparable to the basicity of quaternary ammonium hydroxides. The structure and the strength of intramolecular H-bond in 7-H⁺ makes 7 an excellent “catcher” proton or specific ”sponge” proton.     

Single molecule analysis by surfaced-enhanced Raman scattering

Our main objective in this tutorial review is to provide insight into some of the questions surrounding single molecule detection (SMD) using surface-enhanced Raman scattering (SERS) and surface-enhanced resonance Raman scattering (SERRS). Discovered thirty years ago, SERS is now a powerful analytical tool, strongly tied to plasmonics, a field that encompasses and profits from the optical enhancement found in nanostructures that support localized plasmon excitations. The spectrum of the single molecule carries the quantum fingerprints of the system modulated by the molecule-nanostructure interactions and the electronic resonances that may result under laser excitation. This information is embedded in vibrational band parameters. The dynamics and the molecular environment will affect the bandwidth of the observed Raman bands. In addition, the localized surface plasmon resonances (LSPR) empower the nanostructure with a number of optical properties that will also leave their mark on the observed inelastic scattering process. Therefore, controlling size, shape and the formation of the aggregation state (or fractality) of certain metallic nanostructures becomes a main task for experimental SERS/SERRS. This molecule-nanostructure coupling may, inevitably, lead to spectral fluctuations, increase photobleaching or photochemistry. An attempt is made here to guide the interpretation of this wealth of information when approaching the single molecule regime.     

Chemically selective sensing through layer-by-layer incorporation of biorecognition into thin film substrates for surface-enhanced resonance Raman scattering

In this work, the fabrication, characterization, and application of avidin/Ag nanoparticle layer-by-layer (LbL) films as chemically selective substrates for surface-enhanced resonance Raman scattering (SERRS) is demonstrated. The biospecific interaction between avidin and the small molecule biotin, one of the strongest known to exist in nature, is exploited to preferentially capture biotinylated species from solution. This highly favored adsorption is shown to yield SERRS concentration enhancements and improved detection sensitivities of ca. 102 for commercially available and in situ prepared biotinylated species over their nontagged counterparts.