Molecular versus Silica-Supported Iridium Water Oxidation Catalysts

A stringent comparison between two pairs of molecular/immobilized water oxidation catalysts ([Cp^*Ir(Me-pica)Cl], 1 , versus 1_SiO₂ , Me-pica=κ²-N-methyl-picolinamide; [Cp^*Ir(pysa)NO₃], 2 , versus 2_SiO₂ , pysa=κ²-pyridine-2-sulfonamide]) reveals distinctive catalytic trends. While the molecular compound 1 exhibits a substantial higher activity than the analogous immobilized system 1_SiO₂ , under all the experimental conditions explored, the contrary is found with 2 that is far less active than its immobilized counterpart 2_SiO₂ . This is explained by the unique tendency of 2 to form dimeric complexes [Cp^*Ir-(κ²-μ₂-Hpysa)(κ²-μ₂-pysa)IrCp^*], 2 a , in phosphate buffered solution at pH 7, and [Cp^*Ir-(κ²-μ₂-Hpysa)₂IrCp^*], 2 b , in water. 2 a and 2 b have been completely characterized in solution by multinuclear and multidimensional NMR spectroscopy. They have been also isolated as single crystals and their structure in solid state determined by X-Ray diffractometry. 2 a and 2 b appear to be off-cycle species, whose formation is detrimental for water oxidation activity, as indicated by the observation of a long induction period when 2 a is used as catalytic precursor. In addition, TOF versus ΔE (E−E⁰=−RT/nF ln([IO₄⁻]/[IO₃⁻]) trends for the first two runs do not overlap for catalyst 2 and TOF_max is remarkably higher in the second run upon the addition of fresh NaIO₄. In the immobilized system 2_SiO₂ the detrimental associative processes are likely inhibited leading to an activity higher than that of 2 .     

Combining Imine Condensation Chemistry with [3,3] Diaza-Cope Rearrangement for One-Step Formation of Hydrolytically Stable Chiral Architectures

Dynamic covalent chemistry (DCC) has, in recent years, provided valuable tools to synthesize molecular architectures of increasing complexity. We have also taken advantage of imine DCC chemistry to prepare TPMA -based supramolecular cages for molecular recognition applications. However, the versatility of this approach has as a major drawback the intrinsic hydrolytic lability of imines, which hampers some applications. We present herein a synthetic strategy that combines the advantages of a thermodynamic-driven formation of a supramolecular structure using imine chemistry, together with the possibility to synthetize chiral hydrolytically stable structures through a [3,3]-sigmatropic rearrangement. A preliminary mechanistic analysis of this one-pot synthesis and the scope of the reaction are also discussed.     

Controlling the Surface Functionalization of Ultrasmall Gold Nanoparticles by Sequence-Defined Macromolecules

Ultrasmall gold nanoparticles (diameter about 2 nm) were surface-functionalized with cysteine-carrying precision macromolecules. These consisted of sequence-defined oligo(amidoamine)s (OAAs) with either two or six cysteine molecules for binding to the gold surface and either with or without a PEG chain (3400 Da). They were characterized by ¹H NMR spectroscopy, ¹H NMR diffusion-ordered spectroscopy (DOSY), small-angle X-ray scattering (SAXS), and high-resolution transmission electron microscopy. The number of precision macromolecules per nanoparticle was determined after fluorescent labeling by UV spectroscopy and also by quantitative ¹H NMR spectroscopy. Each nanoparticle carried between 40 and 100 OAA ligands, depending on the number of cysteine units per OAA. The footprint of each ligand was about 0.074 nm² per cysteine molecule. OAAs are well suited to stabilize ultrasmall gold nanoparticles by selective surface conjugation and can be used to selectively cover their surface. The presence of the PEG chain considerably increased the hydrodynamic diameter of both dissolved macromolecules and macromolecule-conjugated gold nanoparticles.     

The role of the counteranion in the cation-pi interaction

Chemical double mutant cycles have been used to quantify cation-pi interactions in chloroform as a function of the nature of the counteranion. The cation-pi interaction is -2.5 +/- 0.4 kJ mol(-1) and independent of the anion, even though the overall stability of the complexes varies by an order of magnitude due to competition of the anion for alternative binding sites.     

New development of synthesis and reactivity of seleno- and tellurophenes

Due to the many new and remarkable findings and applications that have been published in recent years in seleno- and tellurophene chemistry, this review revisits the different aspects of this chemistry, including synthesis, reactivity and applications in the field of heterocycles.     

Hydrophobicity within the three-dimensional Mercedes-Benz model: potential of mean force

We use the three-dimensional Mercedes-Benz model for water and Monte Carlo simulations to study the structure and thermodynamics of the hydrophobic interaction. Radial distribution functions are used to classify different cases of the interaction, namely, contact configurations, solvent separated configurations, and desolvation configurations. The temperature dependence of these cases is shown to be in qualitative agreement with atomistic models of water. In particular, while the energy for the formation of contact configurations is favored by entropy, its strengthening with increasing temperature is accounted for by enthalpy. This is consistent with our simulated heat capacity. An important feature of the model is that it can be used to account for well-converged thermodynamics quantities, e.g., the heat capacity of transfer. Microscopic mechanisms for the temperature dependence of the hydrophobic interaction are discussed at the molecular level based on the conceptual simplicity of the model.     

Natural glycoconjugates with antitumor activity

Cancer is one of the major causes of death worldwide. As a consequence, many different therapeutic approaches, including the use of glycosides as anticancer agents, have been developed. Various glycosylated natural products exhibit high activity against a variety of microbes and human tumors. In this review we classify glycosides according to the nature of their aglycone (non-saccharidic) part. Among them, we describe anthracyclines, aureolic acids, enediyne antibiotics, macrolide and glycopeptides presenting different strengths and mechanisms of action against human cancers. In some cases, the glycosidic residue is crucial for their activity, such as in anthracycline, aureolic acid and enediyne antibiotics; in other cases, Nature has exploited glycosylation to improve solubility or pharmacokinetic properties, as in the glycopeptides. In this review we focus our attention on natural glycoconjugates with anticancer properties. The structure of several of the carbohydrate moieties found in these conjugates and their role are described. The structure–activity relationship of some of these compounds, together with the structural features of their interaction with the biological targets, are also reported. Taken together, all this information is useful for the design of new potential anti-tumor drugs.     

Monte Carlo and event-driven dynamics of Brownian particles with orientational degrees of freedom

Recently, a simple scaling argument was introduced that allows us to map, with some precautions, Brownian and Monte Carlo dynamics for spherical particles. Here, we extend the scaling to study systems that have orientational degrees of freedom and carefully asses its validity over a wide region of temperature and density. Our work allows us to devise a Brownian Monte Carlo algorithm that produces, to a good approximation, physically meaningful trajectories with a minimum programming effort, although at the expense of some sampling efficiency.     

Microstructural features and domain formation in (Ba,Sr)2TiSi2O8 fresnoites

The formation and co-existence of crystallographically modulated and non-modulated regions in (Ba,Sr)₂TiSi₂O₈ fresnoites is reviewed, particularly the dependence on local composition. It is shown that perturbations of the average fresnoite structure, determined from appreciable single crystals, are in some cases better described as nanometric domain intergrowths where departures from ideal stoichiometry are characteristics of incommensuration, while modulation is absent from volumes that are less perturbed chemically. Evidence for this differentiation is obtained from selected area electron diffraction (SAED) patterns and high-resolution transmission electron microscopy (HRTEM) images. The domains are readily distinguished by their unique contrast in bright field electron micrographs. Fourier reconstructions of HRTEM images collected from areas with darker contrast show that modulation can change within relatively small volumes. Nearby areas with lighter contrast were found by SAED to be free of structural disorder and incommensurate reflections.     

Amorphous Aggregation of Amyloid Beta 1‐40 Peptide in Confined Space

The amorphous aggregation of Aβ1‐40 peptide is addressed by using micromolding in capillaries. Both the morphology and the size of the aggregates are modulated by changing the contact angle of the sub‐micrometric channel walls. Upon decreasing the hydrophilicity of the channels, the aggregates change their morphology from small aligned drops to discontinuous lines, thereby keeping their amorphous structure. Aβ1‐40 fibrils are observed at high contact angles.