Ceria-promoted oxygen reduction reaction in Pd-based electrocatalysts

PdCo-ceria electrocatalyst is synthesized on carbon support in a size of a few nm by colloid method. Enhanced oxygen reduction reaction (ORR) kinetics of PdCo is observed in the presence of ceria similarly as confirmed for PtCo-ceria in a half cell experiment. In addition, there appears a positive shift of the ORR onset potential of PdCo-ceria compared to PdCo while PtCo-ceria shows no such an apparent shift of onset potential. These effects of ceria on the ORR onset potential and the ORR kinetics are more remarkable as temperature increases. To get the most of oxygen storage and supply capacity of ceria, a high temperature proton exchange membrane fuel cell (PEMFC) is fabricated using PdCo-ceria as a catalyst at the cathode. Ceria effects on the ORR of PdCo-ceria catalyst are realized in the form of higher OCV and lower Tafel slope compared to PdCo catalyst in the PEMFC single cell performance. Enhancements in both ORR kinetics and ORR onset potential are very attractive features of ceria as a co-catalyst in the development of a non-Pt ORR electrocatalyst.     

Oxidation of I- and S2- Anions by Oxygen in Aqueous Suspensions of Silica Gel

Oxidation of I^- and S^{2 -} anions on the silica gel surface by atmospheric oxygen was studied at room temperature. The possibility and rate of oxidation processes are determined by the content of silica gel and oxygen in the systems. Tentative interpretation of the results is based on the assumption that a highly reactive singlet ¹O₂ species is formed in the oxygen ensemble on the silica surface.     

N(epsilon) functionalization of metal and organic protected L-histidine for a highly efficient,direct labeling of biomolecules with [Tc(OH2)3(CO)3]+

Two different pathways for the introduction of an acetyl group at N(epsilon ) in a N(alpha), N(delta), and -COO protected histidine to afford N(epsilon)-(CH(2)COOH)-histidine derivative 7 b are presented. The purpose of this study is the coupling of 7 b to amino groups in bioactive molecules such as peptides. After full deprotection of such a bioconjugate, histidine provides three coordination sites which efficiently coordinate to [(99m)Tc(OH(2))(3)(CO)(3)](+) or [Re(OH(2))(3)(CO)(3)](+) in a facial geometry. This allows the development of novel radiopharmaceuticals. Selective derivatization at the N(epsilon) position has conveniently been achieved by concomitant protection of N(alpha) and N(delta) with a carbonyl group forming a six-membered urea. Cyclic urea ring opening with Fm-OH, coupling of phenylalanine as a model to 7 b through its primary amine and removing of all protecting groups in one step gave a histidine derivative of phenylalanine which could be labeled at 10(-5) M with (99m)Tc in very high yield and even in about 50 % yield at 10(-6) M. The Xray structure of a complex with [Re(CO)(3)](+) in which anilin is coupled to 7 b confirms the facial arrangement of histidine. A second pathway applies directly the [Re(CO)(3)](+) moiety as a protecting group. This is one of the rare examples in which a metal fragment is used as a protecting group for organic functionalities. The coordination to histidine protects the N(alpha), N(delta) and COO group in one single step, subsequent alkylation with BrCH(2)COOH(R) at N(epsilon), coupling to phenylalanine and oxidative deprotection of [Re(CO)(3)](+) to [ReO(4)](-) gave the corresponding bioconjugate in which histidine is coupled to phenylalanine through an acetylamide at N(epsilon). Both methods offer convenient pathways to introduce histidine in a biomolecule under retention of its three coordination sites. The procedures are adaptable to any biomolecule with pendant amines and allow the development of novel radiopharmaceuticals or inversed peptides.     

Conjugation of a novel histidine derivative to biomolecules and labelling with [99mTc(OH2)3(CO)3]+

The new histidine derivative 3-[1-[3-(9H-fluoren-9-ylmethoxycarbonylamino)-propyl]-1H-imidazol-4-yl]-2-(3-trimethylsilanyl-ethylcarboxyamino)-propionic acid methyl ester (7) has been prepared via alkylation of the histidine urea derivative (7S)-5,6,7,8-tetrahydro-7-(methoxycarbonyl)-5-oxoimidazo-[1,5-c]-pyrimidine (2) with Fmoc-protected 3-iodopropyl-amine, followed by ring opening with 2-trimethylsilylethanol. After Fmoc cleavage by HNEt2, the histidine amine derivative was coupled to biotin, to the pentapeptide leucine-enkephalin and to Vitamin B12-b-acid by amide formation, employing TBTU as the coupling reagent. In order to make the histidine accessible for labelling, the teoc protecting group was removed by either NBu4F (for the biotin conjugate) or by TFA (for the enkephalin and B12 conjugates). Reaction of a 10(-4) M solution of the bioconjugates with [99mTc(H2O)3(CO)3]+ at 50 degrees C for 30 min led to the formation of one single new peak in the HPLC radiochromatogram in each case, confirming quantitative labelling of the respective biomolecules. To assess the nature of the labelled compounds, the rhenium analogues with Re(CO)3 were also synthesised and similar retention times confirmed the identity with the 99mTc labelled conjugates.     

Stereoselective hydrogenation of 11-hexadecyne-l-ol on supported copper catalysts

Hydrogenation of 11-hexadecyne-l-ol on 5–30 % copper catalysts supported on -A1₂O₃ and MgCO₃ results incis-11-hexadecyne-1-ol in 100 % yield. Hydrogenation does not occur on 5–30 % Cu/ZnO catalysts. The difference in behavior of the catalysts is connected with the valent state of copper on the surface and different hydrogen chemisorption.Positive conclusion on the application No. 930071.1 of 16.06.93 for the Kazakhstan preliminary Patent (A. M. Pak, O. 1. Kartonozhkina, and G. T. lzdebskaya).Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 5, pp. 1147–1150, May, 1996.     

Electric field effects on water clusters (n = 3-5): systematic ab initio study of structures, energetics, and transition states

The structures, energetics, and transition states of water clusters (trimer to pentamer, n = 3-5) are investigated as a function of electric field by using ab initio calculations. With an increasing strength of the field, the most stable cyclic structures of trimer, tetramer, and pentamer open up to align their dipole moments along the direction of the field. For the lower strength (below 0.3 V/angstroms) of the electric field, the dipole moment of each water monomer is along the same direction with the field, while it retains the cyclic structure. For the higher strength of the field, to have a higher dipole moment for the cluster along the field direction, each cyclic structure opens up to form a linear chain or "water wire." We have investigated the transition state structures between the cyclic and linear forms for the field strengths of 0.3-0.4 V/angstroms where both cyclic and linear forms are energetically comparable.     

The strong coupling constants of excited positive parity heavy mesons in light-cone QCD

We calculate the strong coupling constants g_p^**p^*π, where P^** (D^**, B^**) is the 1⁺ p-wave state, in the framework of the light-cone QCD sum rules, and using these values ofg_p^**p^*π , we compute the hadronic decay widths forD^** → D^* π and B^** → B^* π.     

Growth dynamics of Bragg gratings in multimode optical fibre

The spectrum of a Bragg grating in a multimode optical fiber can be controlled by the number of irradiation pulses during the writing procedure. Hence, a single mode grating can be fabrication readily within a multimode fiber. The width of the stop band of the grating can also be controlled by means of the number of irradiation pulses. A tilted grating leads to the coupling of core mode to cladding mode, and when the tilt is sufficiently large, eventually to radiation mode. In the case of small tilt, the grating spectrum is the sum of the core-core mode spectrum and the core-cladding mode spectrum.