Conformational and thermodynamic properties of gaseous levulinic acid

Molecular modeling is used to determine low-energy conformational structures and thermodynamic properties of levulinic acid in the gas phase. Structure and IR vibrational frequencies are obtained using density functional and M?ller-Plesset perturbation theories. Electronic energies are computed using G3//B3LYP and CBS-QB3 model chemistries. Computed anharmonic frequencies are consistent with reported experimental data. Population analysis shows a boat- and a chainlike structure to be most abundant at 298 K, with increasing proportions of two other conformers at higher temperatures. Population mean distribution values for thermodynamic quantities are derived. At 298 K and 1 atm, the enthalpy of formation, entropy, and heat capacity are -613.1 ± 1.0 kJ·mol(-1), 407.4 J·mol(-1)·K(-1), and 132.3 J·mol(-1)·K(-1), respectively.     

Selective turn-on fluorescent probes for imaging hydrogen sulfide in living cells

Hydrogen sulfide (H(2)S) is an important biological messenger but few biologically-compatible methods are available for its detection. Here we report two bright fluorescent probes that are selective for H(2)S over cysteine, glutathione and other reactive sulfur, nitrogen, and oxygen species. Both probes are demonstrated to detect H(2)S in live cells.     

Determination of valproic acid by high-performance liquid chromatography with photodiode-array and fluorescence detection.

The derivatization of valproic acid and undecylenic acid with 4-bromomethyl-7-methoxycoumarin is described. The derivatives were detected by photodiode-array and fluorescence detectors. The optimum monitoring conditions and the stability of the suspension solution and derivatives were investigated. A high-performance liquid chromatographic (HPLC) method with isocratic or gradient elution has been established for the analysis. This method has been used for the determination of total and free valproic acid in serum. There is a satisfactory correlation between the results obtained by this HPLC method and those measured by the enzyme immunoassay. Some other common anti-epileptic drugs did not interfere with the analysis. The method is simple and fast and has better sensitivity and linearity than enzyme immunoassay. It is suited for routine therapeutic drug monitoring.     

On the Adsorption and Reduction of the Herbicide Picloram on Mercury and Carbon Electrodes

At concentrations higher than 2?10^?4 M , and below pH 3, the cyclic voltammograms of picloram (=4‐amino‐3,5,6‐trichloropyridine‐2‐carboxylic acid) on Hg electrodes show two prepeak systems (named I and II attending to the proximity to the main reductions peak), which can be attributed to the weak adsorption of reactant and the strong adsorption of the product at the electrode surface. The system II is due to the uncharged form of picloram, and system I to the picloram protonated at the pyridine N‐atom. Small amounts of the surfactant Triton X‐100 (=α‐[4‐(1,1,3,3‐tetramethylbutyl)phenyl]‐ω‐hydroxypoly(oxyethane‐1,2‐diyl)) cause the disappearance of system I, the shift of system II, and also affect the intensities and widths of anodic and cathodic peaks but not the charge passed in each peak. Thus, the adsorption process responsible for the appearance of system I is inhibited by the presence of Triton; by contrast, the process corresponding to system II is only modified by the surfactant, becoming an electrochemical process occurring at the potentials corresponding to system II, which is more reversible than that observed in the absence of Triton. The addition of Triton permitted the analysis of the main reduction process. Convolution voltammetry of the main reduction peak is consistent with the loss of a Cl‐atom in equilibrium which occurs after a reversible electron transfer and is followed by the reductions of both species present in the equilibrium (Scheme 2). This is also the reduction mechanism on a glassy carbon electrode but the electron transfer on the carbon electrode increases with respect to the mercury electrodes; in addition, the loss of the Cl‐atom does not take place on the electrode surface. From the recording of differential capacity–potential curves, it was concluded that picloram is adsorbed on the carbon electrode; but this adsorption is too weak to induce the appearance of prepeak systems.     

Spin pumping at the magnetic insulator (YIG)/normal metal (Au) interfaces

Spin injection across the ferrimagnetic insulator (YIG)/normal metal (Au) interface was studied by ferromagnetic resonance. The spin mixing conductance was determined by comparing the Gilbert damping in bare YIG films with those covered by a Au/Fe/Au structure. The Fe layer in Au/Fe/Au acted as a spin sink as displayed by an increased Gilbert damping parameter α compared to that in the bare YIG. In particular, for the 9.0 nm YIG/2.0 nm Au/4.3 nm Fe/6.1 nm Au structure, the YIG and Fe films were coupled by an interlayer exchange coupling, and the exchange coupled YIG exhibited an increased Gilbert damping compared to the bare YIG. This relationship between static and dynamic coupling provides direct evidence for spin pumping. The transfer of spin momentum across the YIG interface is surprisingly efficient with the spin mixing conductance g(↑↓) ? 1.2 × 10(14) cm(-2).     

On-line determination of 3,5,6-trichloro-2-pyridinol in human urine samples by surface plasmon resonance immunosensing

An immunochemical method for the analysis of 3,5,6-trichloro-2-pyridinol (TCP), a major urinary metabolite of chlorpyrifos, is developed using a surface plasmon resonance (SPR)-based biosensor. The stability of the assay was assessed by covalently linking the analyte derivative to a thin, gold-modified sensor surface. For optimization of analyte derivative immobilization, sensor chips were activated via alkanethiol monolayers with terminal amine or carboxyl groups. Binding inhibition tests were performed in untreated urine samples and compared to those obtained in distilled water and PBS was used as control. In all cases, similar detection limits, at the micrograms per litre level (0.1–0.24 μg L⁻¹), were attained for TCP assays independently of the dilution buffer. Reproducibility of measurements was studied throughout more than 130 regeneration cycles, which allowed the repeated use of the same immunosensor surface without significant variation of the SPR signal. All measurements were developed in real-time in only 10 min, using a SPR portable system. The device could be applied as a valuable analytical method to both environmental screening and clinic diagnostics.     

Structural stability and electrochemical properties of Gd-doped ZrO2 nanoparticles prepared by sol–gel

Cubic, tetragonal and monoclinic Gd-doped zirconia nanoparticles with nominal composition Gd_xZr_1?xO₂ in the range 0 ≤ x ≤ 0.2, were prepared by annealing dried gels of Gd-containing zirconia at temperatures over the range between 450 and 1,300 °C. The synthesized zirconia-based nanoparticles with increased gadolinium load were characterized by X-ray powder diffraction, infrared and Raman spectroscopies, and transmission electron microscopy. The stabilization of the crystalline forms of Gd-doped ZrO₂ solid solutions depends on the amount of Gd dopant and the annealing temperature. For low Gd loads in Gd_xZr_1?xO₂ being x < 0.05, the tetragonal form is the single phase up to 1,100 °C, whereas the monoclinic is the crystalline form detected up to 1,300 °C. Within the range of compositions 0.05 ≤ x < 0.1, is the tetragonal the only stabilized zirconia crystalline structure over the whole range of temperature up to 1,300 °C. For higher Gd-contents, in the range 0.1 ≤ x ≤ 0.2, is the cubic zirconia form the only stable phase for the whole range of annealing temperatures. Solid-state electrochemistry of the gadolinium-doped zirconia performed by the voltammetry of microparticles approach allowed distinguishing different electrochemical answers of Gd cation associated with slightly different local coordination surrounding of cations. Enantioselective electrocatalytic effect of monoclinic Gd-doped ZrO₂ on the oxidation of l-(+)-tartaric acid and d-(?)-tartaric was also studied.