Polarization properties of phase gratings recorded in a Bi12SiO20 crystal

Due to the co-existence of optical activity and linear birefringence in a Bi₁₂SiO₂₀ crystal, a phase gratting induced in this medium has many interesting and unusual properties. We study the ellipticity and orientation of the directly transmitted and diffracted beams as a function of the read-beam vector orientation. In image processing experiments the signal to noise ratio can be increased significantly by appropriately choosing the read-beam orientation such that the strong direct beam is linearly polarized and can be eliminated with the help of a polarizer.     

Synthesis of Low-Valent Dinuclear Group 14 Compounds with Element–Element Bonds by Transylidation

Dinuclear low-valent compounds of the heavy main group elements are rare species owing to their intrinsic reactivity. However, they represent desirable target molecules due to their unusual bonding situations as well as applications in bond activations and materials synthesis. The isolation of such compounds usually requires the use of substituents that provide sufficient stability and synthetic access. Herein, we report on the use of strongly donating ylide-substituents to access low-valent dinuclear group 14 compounds. The ylides not only impart steric and electronic stabilization, but also allow facile synthesis via transfer of an ylide from tetrylene precursors of type ^RY₂E to ECl₂ (E=Ge, Sn; ^RY=TolSO₂(PR₃)C with R=Ph, Cy). This method allowed the isolation of dinuclear complexes amongst a germanium analogue of a vinyl cation, [(^PhY)₂GeGe(^PhY)]⁺ with an electronic structure best described as a germylene-stabilized Ge^II cation and a ylide(chloro)digermene [^CyY(Cl)GeGe(Cl)^CyY] with an unusually unsymmetrical structure.     

Nilpotent completely positive maps

We study the structure of nilpotent completely positive maps in terms of Choi-Kraus coefficients. We prove several inequalities, including certain majorization type inequalities for dimensions of kernels of powers of nilpotent completely positive maps.     

Survival of Classical and Quantum Particles in the Presence of Traps

We present a detailed comparison of the motion of a classical and of a quantum particle in the presence of trapping sites, within the framework of continuous-time classical and quantum random walk. The main emphasis is on the qualitative differences in the temporal behavior of the survival probabilities of both kinds of particles. As a general rule, static traps are far less efficient to absorb quantum particles than classical ones. Several lattice geometries are successively considered: an infinite chain with a single trap, a finite ring with a single trap, a finite ring with several traps, and an infinite chain and a higher-dimensional lattice with a random distribution of traps with a given density. For the latter disordered systems, the classical and the quantum survival probabilities obey a stretched exponential asymptotic decay, albeit with different exponents. These results confirm earlier predictions, and the corresponding amplitudes are evaluated. In the one-dimensional geometry of the infinite chain, we obtain a full analytical prediction for the amplitude of the quantum problem, including its dependence on the trap density and strength.     

Synthesis of sugar-derived spiroaminals via lactamization and metathesis reactions

A series of sugar-derived spiroaminals has been synthesized by utilizing cross metathesis, ring closing metathesis and lactamization reactions as key steps from 1-C-alkylated glycosyl azides and important correlations in the spectral data between spiroaminals and their respective anomers are reported.     

Platinum(II)-Catalyzed Novel Synthesis of 3,4-Fused Furans

A novel synthesis of 3,4-fused furans (both tricyclic and bicyclic) through platinum-catalyzed cyclization of 3-(2-formylcycloalkenyl)-acrylic amides 2 in methanol is described (up to 90% yield). Tricyclic 3,4-fused dihydrofuran derivatives were also obtained via reductive cyclization of 2. The substrates 2 were obtained from β- bromovinyl aldehydes by a Pd-catalyzed Heck reaction.     

Potential Therapeutic Target Protein Tyrosine Phosphatase-1B for Modulation of Insulin Resistance with Polyphenols and Its Quantitative Structure–Activity Relationship

The increase in the number of cases of type 2 diabetes mellitus (T2DM) and the complications associated with the side effects of chemical/synthetic drugs have raised concerns about the safety of the drugs. Hence, there is an urgent need to explore and identify natural bioactive compounds as alternative drugs. Protein tyrosine phosphatase 1B (PTP1B) functions as a negative regulator and is therefore considered as one of the key protein targets modulating insulin signaling and insulin resistance. This article deals with the screening of a database of polyphenols against PTP1B activity for the identification of a potential inhibitor. The research plan had two clear objectives. Under first objective, we conducted a quantitative structure–activity relationship analysis of flavonoids with PTP1B that revealed the strongest correlation (R² = 93.25%) between the number of aromatic bonds (naro) and inhibitory concentrations (IC₅₀) of PTP1B. The second objective emphasized the binding potential of the selected polyphenols against the activity of PTP1B using molecular docking, molecular dynamic (MD) simulation and free energy estimation. Among all the polyphenols, silydianin, a flavonolignan, was identified as a lead compound that possesses drug-likeness properties, has a higher negative binding energy of −7.235 kcal/mol and a pKd value of 5.2. The free energy-based binding affinity (ΔG) was estimated to be −7.02 kcal/mol. MD simulation revealed the stability of interacting residues (Gly183, Arg221, Thr263 and Asp265). The results demonstrated that the identified polyphenol, silydianin, could act as a promising natural PTP1B inhibitor that can modulate the insulin resistance.     

(1‐Butyl‐4‐methyl‐pyridinium)[Cu(SCN)2]: A Coordination Polymer and Ionic Liquid

The compound (C₄C₁py)[Cu(SCN)₂], (C₄C₁py=1‐Butyl‐4‐methyl‐pyridinium), which can be obtained from CuSCN and the ionic liquid (C₄C₁py)(SCN), turns out to be a new organic–inorganic hybrid material as it qualifies both, as a coordination polymer and an ionic liquid. It features linked [Cu(SCN)₂]^? units, in which the thiocyanates bridge the copper ions in a μ_1,3‐fashion. The resulting one‐dimensional chains run along the a axis, separated by the C₄C₁py counterions. Powder X‐ray diffraction not only confirms the single‐crystal X‐ray structure solution but proves the reformation of the coordination polymer from an isotropic melt. However, the materials shows a complex thermal behavior often encountered for ionic liquids such as a strong tendency to form a supercooled melt. At a relatively high cooling rate, glass formation is observed. When heating this melt in differential scanning calorimetry (DSC) and temperature‐dependent polarizing optical microscopy (POM), investigations reveal the existence of a less thermodynamically stable crystalline polymorph. Raman measurements conducted at 10 and 100 °C point towards the formation of polyanionic chain fragments in the melt. Solid‐state UV/Vis spectroscopy shows a broad absorption band around 18 870 cm^?1 (530 nm) and another strong one below 20 000 cm^?1 (<500 nm). The latter is attributed to the d(Cu^I)→π*(SCN)‐MLCT (metal‐to‐ligand charge transfer) transition within the coordination polymer yielding an energy gap of 2.4 eV. At room temperature and upon irradiation with UV light, the material shows a weak fluorescence band at 15 870 cm^?1 (630 nm) with a quantum efficiency of 0.90(2) % and a lifetime of 131(2) ns. Upon lowering the temperature, the luminescence intensity strongly increases. Simultaneously, the band around 450 nm in the excitation spectrum decreases.     

Spectroscopic investigation on the interaction of ICT probe 3-acetyl-4-oxo-6,7-dihydro-12H Indolo-[2,3-a] quinolizine with serum albumins

Interaction of 3-acetyl-4-oxo-6,7-dihydro-12H indolo-[2,3-a] quinolizine (AODIQ), a biologically active molecule, with model transport proteins, bovine serum albumin (BSA) and human serum albumin (HSA) have been studied using steady state and picosecond time-resolved fluorescence and fluorescence anisotropy. The polarity dependent intramolecular charge transfer (ICT) process is responsible for the remarkable sensitivity of this biological fluorophore to the protein environments. The CT fluorescence exhibits appreciable hypsochromic shift along with an enhancement in the fluorescence yield, fluorescence anisotropy (r) and fluorescence lifetime upon binding with the proteins. The reduction in the rate of ICT within the hydrophobic interior of albumins leads to an increase in the fluorescence yield and lifetime. Marked increase in the fluorescence anisotropy indicates that the probe molecule is located in a motionally constrained environment within the proteins. Micropolarities in the two proteinous environments have been determined following the polarity sensitivity of the CT emission. Addition of urea to the protein-bound systems leads to a reduction in the fluorescence anisotropy indicating the denaturation of the proteins. Polarity measurements and fluorescence resonance energy transfer (FRET) studies throw light in assessing the location of the fluorophore within the two proteinous media.