Phosphorylated 2-Chloroethynes in the Reactions with Malonic Acid Derivatives: Azirine or Oxazole?

Russian Journal of General Chemistry - The reactions of (2-chloroethynyl)diphenylphosphine oxide with diethyl 2-aminomalonate and of dimethyl (2-chloroethynyl)phosphonate with...     

Bioanalysis of drugs and their metabolites by chiral electromigration techniques (2010–2020)

The further development and application of capillary electromigration techniques for the enantioselective determination of drugs and their metabolites in body fluids, tissues, and in vitro preparations during the 2010 to 2020 time period continued to proof their usefulness and attractiveness in bioanalysis. This review discusses the principles and important aspects of capillary electrophoresis- based chiral drug bioassays, provides a survey of the assays reported during the past 10 years and presents an overview of the key achievements encountered in that time period. For systems with charged chiral selectors, special attention is paid on assays that feature field-amplified sample injection to enable the determination of ppb levels of analytes and optimized online incubation procedures for the rapid assessment of a metabolic pathway. Applications discussed encompass the pharmacokinetics of drug enantiomers in vivo and in vitro, the impact of inhibitors on metabolic steps, the elucidation of the stereoselectivity of drug metabolism in vivo and in vitro, and drug enantiomers in toxicological, forensic, and doping analysis.     

Diazido Mixed‐Amine Platinum(IV) Anticancer Complexes Activatable by Visible‐Light Form Novel DNA Adducts

Platinum diam(m)ine complexes, such as cisplatin, are successful anticancer drugs, but suffer from problems of resistance and side‐effects. Photoactivatable Pt^IV prodrugs offer the potential of targeted drug release and new mechanisms of action. We report the synthesis, X‐ray crystallographic and spectroscopic properties of photoactivatable diazido complexes trans,trans,trans‐[Pt(N₃)₂(OH)₂(MA)(Py)] ( 1 ; MA=methylamine, Py=pyridine) and trans,trans,trans‐[Pt(N₃)₂(OH)₂(MA)(Tz)] ( 2 ; Tz=thiazole), and interpret their photophysical properties by TD‐DFT modelling. The orientation of the azido groups is highly dependent on H bonding and crystal packing, as shown by polymorphs 1 p and 1 q . Complexes 1 and 2 are stable in the dark towards hydrolysis and glutathione reduction, but undergo rapid photoreduction with UVA or blue light with minimal amine photodissociation. They are over an order of magnitude more potent towards HaCaT keratinocytes, A2780 ovarian, and OE19 oesophageal carcinoma cells than cisplatin and show particular potency towards cisplatin‐resistant human ovarian cancer cells (A2780cis). Analysis of binding to calf‐thymus (CT), plasmids, oligonucleotide DNA and individual nucleotides reveals that photoactivated 1 and 2 form both mono‐ and bifunctional DNA lesions, with preference for G and C, similar to transplatin, but with significantly larger unwinding angles and a higher percentage of interstrand cross‐links, with evidence for DNA strand cross‐linking further supported by a comet assay. DNA lesions of 1 and 2 on a 50 bp duplex were not recognised by HMGB1 protein, in contrast to cisplatin‐type lesions. The photo‐induced platination reactions of DNA by 1 and 2 show similarities with the products of the dark reactions of the Pt^II compounds trans‐[PtCl₂(MA)(Py)] ( 5 ) and trans‐[PtCl₂(MA)(Tz)] ( 6 ). Following photoactivation, complex 2 reacted most rapidly with CT DNA, followed by 1 , whereas the dark reactions of 5 and 6 with DNA were comparatively slow. Complexes 1 and 2 can therefore give rapid potent photocytotoxicity and novel DNA lesions in cancer cells, with no activity in the absence of irradiation.     

Reactions of 2-Phosphonylethynylated 2-(Arylamino)malonates with Some Bases

Russian Journal of General Chemistry - The reaction of dialkyl 2-[(dialkoxyphosphoryl)ethynyl]-2-(arylamino)malonates with bases (CH3COOK, t-BuOK) can serve as a method for preparing original...     

Effect of oxidant on electronic transport in polypyrrole nanotubes synthesized in the presence of methyl orange

Polypyrrole nanotubes with diameter 60–400 nm are synthesized with methyl orange as template and various oxidants, iron(III) chloride hexahydrate, iron(III) sulfate hydrate, and ammonium peroxydisulfate. The highest electrical conductivity of compressed pellets, 66 S cm^?1, is found for iron(III) chloride. Regions with 3D variable range hopping in series with ordered regions near metal–insulator transition govern the charge transport. Other oxidants and globular morphology provide less conducting samples, <10 S cm^?1. The transport mechanism is identified with the heterogeneous model of tunneling between (bi)polaronic clusters with parallel contribution of Arrhenius‐like activated conductivity. The results of conductivity are correlated with the protonation level reflected in the infrared spectra and with the ratio of bipolaron/polaron bands revealed by Raman spectroscopy. © 2015 Wiley Periodicals, Inc. J. Polym. Sci., Part B: Polym. Phys. 2015 , 53, 1147–1159     

Ion source with electron ionization for a portable mass spectrometer

An ion source with electron ionization is considered. The charged-particle flow at the exit from this source has a cross section of ∼0.1 × 0.1 mm, an angle spread of 2° × 2°, a relative energy spread of <0.5%, and an energy range of 0.5–3.0 keV. This ion source is intended for systems where an ion beam is focused in two mutually perpendicular directions. The ion source design makes it possible to ionize a sample locally (in a volume of ∼10 mm³), where the concentration of the particles under study exceeds the concentration averaged over the volume of the vacuum chamber of the mass spectrometer by two to three orders of magnitude. The ion-optical properties of the source are numerically simulated, and the optimum parameters of the source are chosen. Examples of the application of the ion source are given for the mass-spectrometric determination of metal salts in aqueous solutions and of gases and volatile compounds in samples in various phase states.     

Dynamic high-resolution computer simulation of electrophoretic enantiomer separations with neutral cyclodextrins as chiral selectors

GENTRANS, a comprehensive one-dimensional dynamic simulator for electrophoretic separations and transport, was extended for handling electrokinetic chiral separations with a neutral ligand. The code can be employed to study the 1:1 interaction of monovalent weak and strong acids and bases with a single monovalent weak or strong acid or base additive, including a neutral cyclodextrin, under real experimental conditions. It is a tool to investigate the dynamics of chiral separations and to provide insight into the buffer systems used in chiral capillary zone electrophoresis (CZE) and chiral isotachophoresis. Analyte stacking across conductivity and buffer additive gradients, changes of additive concentration, buffer component concentration, pH, and conductivity across migrating sample zones and peaks, and the formation and migration of system peaks can thereby be investigated in a hitherto inaccessible way. For model systems with charged weak bases and neutral modified β-cyclodextrins at acidic pH, for which complexation constants, ionic mobilities, and mobilities of selector-analyte complexes have been determined by CZE, simulated and experimentally determined electropherograms and isotachopherograms are shown to be in good agreement. Simulation data reveal that CZE separations of cationic enantiomers performed in phosphate buffers at low pH occur behind a fast cationic migrating system peak that has a small impact on the buffer composition under which enantiomeric separation takes place.     

Knockout of deuterons and tritons with large transverse momenta in <Emphasis Type="Italic">pA</Emphasis> collisions involving 50-GeV protons

Formation of the d and t cumulative light nuclear fragments emitted from the nucleus with large transverse momenta at an angle of 35° in the laboratory frame is investigated. The data on collisions of 50-GeV protons with the C, Al, Cu, and W nuclei are collected using the extracted proton beam of the IHEP accelerator and the SPIN detector. The results indicate that the dominant contribution to formation of nuclear fragments comes from the local process of direct knockout from the nucleus.