About the barriers to reaction of CCl4 with HFeOH and FeCl2

The reactions of zerovalent iron with water and carbon tetrachloride are of interest for environmental remediation of contaminated water and soil. Atom-dropping experiments have shown that the reactions of iron atoms with water and CCl(4) may produce HFeOH and FeCl(2), respectively, but these compounds are themselves unreactive toward CCl(4) at the low temperatures under which the atom-dropping experiments were performed. We report a modeling study of these reactions using density functional theory, ab initio Hartree-Fock and couple-cluster theory, and principles of Marcus-Hush theory to characterize the underlying intrinsic barriers and rationalize the experimental results. Electron-correlated CCSD(T) calculations (at B3LYP/TZVP optimized structures) show that the transition state for Cl atom transfer from CCl(4) to HFeOH arises from crossing of electronic states in which the configuration of Fe changes from a quintet high spin state in the Fe(II) reactant to a sextet high spin state in the Fe(III) products. The crossing point is 23.8 kcal/mol above a long-range precursor complex that is 2.1 kcal/mol more stable than the separated reactants. The electronic structure changes in these Cl atom transfer reactions involve unpairing of d electrons in Fe(II) and their recoupling with Cl-C σ bond electrons. These processes can be conveniently described by invoking the self-exchange reactions HFeOH/HFeClOH, FeCl(2)/FeCl(3), and CCl(4)/(?)CCl(3) for which we determined the energy barriers to be 15.5, 13.1, 18.6 kcal/mol, respectively. For the cross reaction FeCl(2)/CCl(4), we estimated a barrier of 16.6 kcal/mol relative to the separated reactants and 21.1 kcal/mol from the precursor complex. The magnitudes of the reaction barriers are consistent with reports of the absence of products in the atom-dropping experiments.     

The Role of a Dipeptide Outer‐Coordination Sphere on H2‐Production Catalysts: Influence on Catalytic Rates and Electron Transfer

The outer‐coordination sphere of enzymes acts to fine‐tune the active site reactivity and control catalytic rates, suggesting that incorporation of analogous structural elements into molecular catalysts may be necessary to achieve rates comparable to those observed in enzyme systems at low overpotentials. In this work, we evaluate the effect of an amino acid and dipeptide outer‐coordination sphere on [Ni(P^Ph₂N^Ph‐R₂)₂]²⁺ hydrogen production catalysts. A series of 12 new complexes containing non‐natural amino acids or dipeptides was prepared to test the effects of positioning, size, polarity and aromaticity on catalytic activity. The non‐natural amino acid was either 3‐(meta‐ or para‐aminophenyl)propionic acid terminated as an acid, an ester or an amide. Dipeptides consisted of one of the non‐natural amino acids coupled to one of four amino acid esters: alanine, serine, phenylalanine or tyrosine. All of the catalysts are active for hydrogen production, with rates averaging ～1000 s^?1, 40 % faster than the unmodified catalyst. Structure and polarity of the aliphatic or aromatic side chains of the C‐terminal peptide do not strongly influence rates. However, the presence of an amide bond increases rates, suggesting a role for the amide in assisting catalysis. Overpotentials were lower with substituents at the N‐phenyl meta position. This is consistent with slower electron transfer in the less compact, para‐substituted complexes, as shown in digital simulations of catalyst cyclic voltammograms and computational modeling of the complexes. Combining the current results with insights from previous results, we propose a mechanism for the role of the amino acid and dipeptide based outer‐coordination sphere in molecular hydrogen production catalysts.     

Methionine Capped Nanoparticles as Acetylcholinesterase Inhibitors

The silver and gold L-methionine capped nanoparticles (Ag and Au @LM NPs) were analyzed as prospective acetylcholinesterase (AChE) inhibitors to test their potential in the treatment of cognitive impairment in depression and Alzheimer's disease. The stability of NPs, and their ability to inhibit AChE were studied by UV-Vis and FTIR spectrophotometry. At the same time, TEM and SEM measurements, DLS, and zeta potential measurements were employed in the structural characterization of NPs. Nearly spherical, negatively charged Ag and Au @LM NPs, with 17 nm and 31 nm in diameter, respectively, showed moderate inhibitory potential toward AChE in the given frame of investigated concentrations. For both NPs IC50 is not reached. Furthermore, the adsorption of enzyme molecules on the surface of Ag and Au @LM NPs was demonstrated. Hence, our assumption is that inhibition of AChE is caused by blockage of the enzyme‘s active site due to the steric hindrance of NPs.     

Heavy metal content of a medicinal moss tea for hypertension

The content of various heavy metals (arsenic, cadmium, chromium, copper, iron, lead, mercury, nickel, manganese and zinc) in the moss species Rhodobryum ontariense (Kindb.) Kindb. and its tea are presented in this study. Pursuant to the use of this tea in traditional Chinese medicine for hypertension, the aim of this study was to examine its safety in regard to the metals. All heavy metals were determined by adequate EPA methods. The concentrations of all metals for daily intake in its tea were below the safety levels for human consumption. These results indicate the importance of manganese in R. ontariense tea traditionally used for hypertension and other heart disorders.     

Acceleration of uncertainty updating in the description of transport processes in heterogeneous materials

The prediction of thermo-mechanical behaviour of heterogeneous materials such as heat and moisture transport is strongly influenced by the uncertainty in parameters. Such materials occur e.g., in historic buildings, and the durability assessment of these therefore needs a reliable and probabilistic simulation of transport processes, which is related to the suitable identification of material parameters. In order to include expert knowledge as well as experimental results, one can employ an updating procedure such as Bayesian inference. The classical probabilistic setting of the identification process in Bayes’ form requires the solution of a stochastic forward problem via computationally expensive sampling techniques, which makes the method almost impractical.     

Cell Uptake and Trafficking Behavior of Non‐covalent,Coiled‐coil Based Polymer–Drug Conjugates

This paper reports on the cell uptake and trafficking properties of a series of non‐covalent polymer–drug conjugates. These nanomedicines are composed of a poly(N‐(2‐hydroxypropyl)methacrylamide) backbone functionalized with multiple copies of a drug. The drug moieties are attached to the polymer via a non‐covalent, so called coiled coil motif, which is formed by heterodimerization of two complementary peptide strands, one of which is attached to the polymer carrier and the other to the drug. Cytotoxicity and FACS experiments, which were carried out with model anticancer drug or fluorophore conjugates, provided insight into the cell uptake and trafficking behavior of these conjugates.

     

A small-molecule probe for hepatitis C virus replication that blocks protein folding

The hepatitis C virus (HCV) is a growing global health problem. Small molecules that interfere with host-viral interactions can serve as powerful tools for elucidating the molecular mechanisms of pathogenesis and defining new strategies for therapeutic development. Using a cell-based screen involving subgenomic HCV replicons, we identified the ability of 18 different abscisic acid (ABA) analogs, originally developed as plant growth regulators, to inhibit HCV replication. Three of these were further studied. One compound, here named origamicin, showed antiviral activity through the inhibition of host proteins involved in protein folding. Origamicin could therefore be an important tool for studying the maturation of both host and viral proteins. Herein we demonstrate an application for molecular scaffolds based on ABA for mammalian cell targets involved in protein folding.     

Directed mutagenesis alters the stereochemistry of catalysis by isolated ketoreductase domains from the erythromycin polyketide synthase

The ketoreductase (KR) domains eryKR(1) and eryKR(2) from the erythromycin-producing polyketide synthase (PKS) reduce 3-ketoacyl-thioester intermediates with opposite stereospecificity. Modeling of eryKR(1) and eryKR(2) showed that conserved amino acids previously correlated with production of alternative alcohol configurations lie in the active site. eryKR(1) domains mutated at these positions showed an altered stereochemical outcome in reduction of (2R, S)-2-methyl-3-oxopentanoic acid N-acetylcysteamine thioester. The wild-type eryKR(1) domain exclusively gave the (2S, 3R)-3-hydroxy-2-methylpentanoic acid N-acetylcysteamine thioester, while the double mutant (F141W, P144G) gave only the (2S, 3S) isomer, a switch of the alcohol stereochemistry. Mutation of the eryKR(2) domain, in contrast, greatly increased the proportion of the wild-type (2R, 3S)-alcohol product. These data confirm the role of key residues in stereocontrol and suggest an additional way to make rational alterations in polyketide antibiotic structure.     

Galvanic displacement of Co with Rh boosts hydrogen and oxygen evolution reactions in alkaline media

Journal of Solid State Electrochemistry - The growing energy crisis put an emphasis on the development of novel efficient energy conversion and storage systems. Here we show that surface...