Selective electrocatalysis of acetaldehyde oxime reduction on (111) sites of platinum single crystal electrodes and nanoparticles surfaces

The reduction of acetaldehyde oxime (AO) in acid medium on platinum surfaces is a structure sensitive reaction that takes place almost exclusively on (111) sites of Pt electrodes, and it is strongly inhibited on Pt(100) and Pt(110) surfaces. A study using stepped electrodes with (111) terraces and monoatomic steps either with (100) and (110) orientation shows that the activity of the electrode is also dependent on the terrace width, i.e., the wider the terrace is, the higher current density is recorded and the more positive the peak potential for AO reduction appears. Moreover, in the electrodes with (100) step sites, the reduction process appears at more negative potential than the electrodes with (111) step sites. Nanoparticles with some preferential orientations were also tested for the AO reduction reaction to check the presence of (111) ordered domains on the nanoparticles surface. Dedicated to Teresa Iwasita on the occasion of her retirement and for her contributions to Electrochemistry.     

Shape-dependent electrocatalysis: methanol and formic acid electrooxidation on preferentially oriented Pt nanoparticles

Reactivity towards methanol and formic acid electrooxidation on Pt nanoparticles with well characterised surfaces were studied and compared with the behaviour of single crystal electrodes with basal orientations. Polyoriented and preferential (100), (111) and (100)-(111) Pt nanoparticles were synthesised, cleaned preserving its surface structure, characterised and employed to evaluate the influence of the surface structure/shape of the Pt nanoparticles on these two relevant electrochemical reactions. The results pointed out that, in agreement with fundamental studies with Pt single crystal electrodes, the surface structure of the electrodes plays an important role on the reactivity of both oxidation processes, and thus the electrocatalytic properties strongly depend on the surface structure/shape of the nanoparticles, in particular on the presence of sites with (111) symmetry. These findings open the possibility of designing new and better electrocatalytic materials using decorated shape-controlled Pt nanoparticles as previously described with Pt single crystal electrodes.     

The role of adsorbates in electrocatalytic systems: An analysis of model systems with single crystals

The use of single crystal electrodes as model catalysts has been widely applied for the study of several reactions. The known structure of the surface provides a system with controlled electronic properties that helps in the understanding of the mechanism of reactions. In this model system, any modification, including the adsorption of anions, organic molecules or foreign atoms, generate changes in the electronic properties of the surface and, thus, in the adsorption energy of the species involved in the studied reaction. The adsorbate can hinder the surface and diminish the activity or prevent the oxidation of the surface and improve the catalysis. The changes in electronic properties can modify the adsorption energy and enhance or worsen the catalytic activity. The effect of any adsorbed species will depend on the structure of the surface, the nature of the species and the studied reaction.     

On-line synthesis of pseudopeptide library incorporating a benzodiazepinone turn mimic: biological evaluation on MC1 receptors

Alpha melanocyte stimulating hormone (alpha-MSH) is a widely distributed hormone. This tridecapeptide exhibits various biological activities mediated through different receptors. alpha-MSH binds to the melanocortin-1 receptor (MC1-R), mainly expressed in keratinocytes and melanocytes, inducing melanogenesis and anti-inflammatory processes. The central His-Phe-Arg-Trp tetrapeptide sequence of alpha-MSH is known to form a turn in the bioactive conformation. To find new potent analogs of alpha-MSH, we decided to introduce non-peptide building blocks in the alpha-MSH sequence. Molecular modeling studies showed that two amino acids of the central core sequence could be replaced by the benzodiazepinone building block without loosing the beta-turn conformation. Benzodiazepines are well-known pharmacophores exhibiting a wide scope of biological activities and are described as constrained dipeptide mimics templates. Although numerous synthetic pathways leading to benzodiazepinones have been described in literature, no methodology has 1,4-benzodiazepine-2,5-diones building blocks bearing a free carboxylic acid function and a protected amino function suitable for incorporation into peptide sequences. In this study, we report the synthesis of peptides with a benzodiazepinone moiety obtained directly during the course of solid-phase peptide synthesis (SPPS). This "on-line" strategy leads to the generation of a 54-member pseudo-peptide library of alpha-MSH analogs. After LC/MS purification, binding assays were performed on the MC1 receptor leading to the discovery of several micromolar ligands.     

Mechanistic and computational studies of the atom transfer radical addition of CCl4 to styrene catalyzed by copper homoscorpionate complexes

Experimental as well as theoretical studies have been carried out with the aim of elucidating the mechanism of the atom transfer radical addition (ATRA) of styrene and carbon tetrachloride with a Tp(x)Cu(NCMe) complex as the catalyst precursor (Tp(x) = hydrotrispyrazolyl-borate ligand). The studies shown herein demonstrate the effect of different variables in the kinetic behavior. A mechanistic proposal consistent with theoretical and experimental data is presented.     

Voltammetry of basal plane platinum electrodes in acetonitrile electrolytes: effect of the presence of water

The first part of this report studies the electrochemical properties of single-crystal platinum electrodes in acetonitrile electrolytes by means of cyclic voltammetry. Potential difference infrared spectroscopy in conjunction with linear voltammetry was used to obtain a molecular-level picture of this interface. The second part of this report studies the hydrogen evolution and the hydrogen oxidation reactions on the three low-index faces of Pt electrodes in acetonitrile electrolytes. The data (CVs and IR spectra) strongly suggest that acetonitrile and CN(-) molecules are adsorbed on single-crystal platinum electrodes in the range of -1.5 to 0.3 V versus Ag/AgCl. Those species block part of the adsorption sites for hydrogen adatoms, and they decompose on the surface in the presence of water. The nature of the cation and the presence of water strongly affect the onset of acetonitrile electrolysis and the kinetics and stability of the adsorbed species on the electrode. Finally, the hydrogen evolution and the hydrogen oxidation reactions on platinum single-crystal surfaces in acetonitrile electrolytes are strongly affected by the surface-energy state of Pt electrodes.     

Substitution reactions in dinuclear Ru-Hbpp complexes: an evaluation of through-space interactions

The synthesis of new dinuclear complexes of the general formula in,in-{[Ru(II)(trpy)(L)](μ-bpp)[Ru(II)(trpy)(L')]}(3+) [bpp(-) is the bis(2-pyridyl)-3,5-pyrazolate anionic ligand; trpy is the 2,2':6',2″-terpyridine neutral meridional ligand, and L and L' are monodentate ligands; L = L' = MeCN, 3a(3+); L = L' = 3,5-lutidine (Me(2)-py), 3c(3+); L = MeCN, L' = pyridine (py), 4(3+)], have been prepared and thoroughly characterized. Further, the preparation and isolation of dinuclear complexes containing dinitrile bridging ligands of the general formula in,in-{[Ru(II)(trpy)](2)(μ-bpp)(μ-L-L)}(3+) [μ-L-L = 1,4-dicyanobutane (adiponitrile, adip), 6a(3+); 1,3-dicyanopropane (glutaronitrile, glut), 6b(3+); 1,2-dicyanoethane (succinonitrile; succ), 6c(3+)] have also been carried out. In addition, a number of homologous dinuclear complexes previously described, containing the anionic bis(pyridyl)indazolate (bid(-)) tridentate meridional ligand in lieu of trpy, have also been prepared for comparative purposes. In the solid state, six complexes have been characterized by X-ray crystallography, and in solution, all of them have been spectroscopically characterized by NMR and UV-vis spectroscopy. In addition, their redox properties have also been investigated by means of cyclic voltammetry and differential pulse voltammetry and show the existence of two one-electron waves assigned to the formation of the II,III and III,III species. Dinitrile complexes 6a(3+), 6b(3+), and 6c(3+) display a dynamic behavior involving their enantiomeric interconversion. The energy barrier for this interconversion can be controlled by the number of methylenic units between the dinitrile ligand. On the other hand, pyridyl complexes in,in-{[Ru(II)(T)(py)](2)(μ-bpp)}(n+) (T = trpy, n = 3, 3b(3+); T = bid(-), n = 1, 3b'(+)) and 3c(3+) undergo two consecutive substitution reactions of their monodentate ligands by MeCN.The substitution kinetics have been monitored by (1)H NMR and UV-vis spectroscopy and follow first-order behavior with regard to the initial ruthenium complex. For the case of 3b(3+), the first-order rate constant k(1) = (2.9 ± 0.3) × 10(-5) s(-1), whereas for the second substitution, the k obtained is k(2) = (1.7 ± 0.7) × 10(-6) s(-1), both measured at 313 K. Their energies of activation at 298 K are 114.7 and 144.3 kJ mol(-1), respectively. Density functional theory (DFT) calculations have been performed for two consecutive substitution reactions, giving insight into the nature of the intermediates. Furthermore, the energetics obtained by DFT calculations of the two consecutive substitution reactions agree with the experimental values obtained. The kinetic properties of the two consecutive substitution reactions are rationalized in terms of steric crowding and also in terms of through-space interactions.     

Brønsted Acid Catalyzed Morita–Baylis–Hillman Reaction: A New Mechanistic View for Thioureas Revealed by ESI‐MS(/MS) Monitoring and DFT Calculations

A Morita–Baylis–Hillman (MBH) reaction catalyzed by thiourea was monitored by ESI‐MS(/MS) and key intermediates were intercepted and characterized. These intermediates suggest that thiourea acts as an organocatalyst in all steps of the MBH reaction cycle, including the rate‐limiting proton‐transfer step. DFT calculations, performed for a model MBH reaction between formaldehyde and acrolein with trimethylamine as base and in the presence or the absence of thiourea, suggest that thiourea accelerates MBH reactions by decreasing the transition‐state (TS) energies through bidentate hydrogen bonding throughout the whole catalytic cycle. In the rate‐limiting proton‐transfer step, the thiourea acts not as a proton shuttle, but as a Brønsted acid stabilizing the basic oxygen center that is formed in the TS.     

Solid-phase synthesis of biaryl cyclic peptides containing a histidine-tyrosine linkage

A solid-phase strategy for the synthesis of biaryl cyclic peptides containing a side-chain to side-chain His-Tyr linkage was developed. The key step was the macrocyclization of a linear peptidyl resin incorporating a 5-bromohistidine and a 3-boronotyrosine via the formation of the biaryl bond by means of a microwave-assisted Suzuki-Miyaura reaction. This method allowed direct access to biaryl cyclic peptides containing a 3- or 5-amino acid ring and bearing the histidine residue at the N- or the C-terminus, being especially conducive for analogues in which this amino acid is located at the C-terminus. This study also served to establish a strategy for the synthesis of biaryl cyclic peptides derived from the two hemispheres of the natural biaryl bicyclic peptides aciculitins.