A single amino acid Gly-tag enables metal-free protein purification

Analytically pure proteins are indispensable for diverse applications, including therapeutics. Here, we report a methodology where a single amino acid, glycine, enables metal-free protein purification. This robust platform is enabled by a Gly-tag resin for site-specific capture, enrichment, and release through chemically triggered C–C bond dissociation by resonance-assisted electron density polarization.

Gly-tag resin precisely captures and releases a protein with one glycine at the N-terminus. The user-friendly protocol delivers analytically pure protein free of metal contaminants.     

Euphorbiasteroid Abrogates EGFR and Wnt/β-Catenin Signaling in Non-Small-Cell Lung Cancer Cells to Impart Anticancer Activity

EGFR and Wnt/β-catenin signaling pathways play a prominent role in tumor progression in various human cancers including non-small-cell lung carcinoma (NSCLC). Transactivation and crosstalk between the EGFR and Wnt/β-catenin pathways may contribute to the aggressiveness of cancers. Targeting these oncogenic pathways with small molecules is an attractive approach to counteract various types of cancers. In this study, we demonstrate the effect of euphorbiasteroid (EPBS) on the EGFR and Wnt/β-catenin pathways in NSCLC cells. EPBS induced preferential cytotoxicity toward A549 (wildtype EGFR-expressing) cells over PC-9 (mutant EGFR-expressing) cells. EPBS suppressed the expression of EGFR, Wnt3a, β-catenin, and FZD-1, and the reduction in β-catenin levels was found to be mediated through the activation of GSK-3β. EPBS reduced the phosphorylation of GSK-3β^S9 with a parallel increase in β-TrCP and phosphorylation of GSK-3β^Y216. Lithium chloride treatment increased the phosphorylation of GSK-3β^S9 and nuclear localization of β-catenin, whereas EPBS reverted these effects. Forced expression or depletion of EGFR in NSCLC cells increased or decreased the levels of Wnt3a, β-catenin, and FZD-1, respectively. Overall, EPBS abrogates EGFR and Wnt/β-catenin pathways to impart its anticancer activity in NSCLC cells.     

Crystallization of Pseudopolymorphs of Some Gamboge Pigments. Pyridine,Dimethylformamide and Dimethylsulfoxide Solvates of Morellic Acid,Gambogic Acid and Guttiferic Acid

Abstract

Morellic acid, gambogic acid and guttiferic acid are related naturally-occurring xanthone pigments that yield X-ray quality crystals only from solvents like pyridine, dimethylformamide (dmf) and dimethyl sulfoxide (dmso). The structures of four of these crystals have been determined and are found to contain solvents of crystallization. The solvents hydrogen bond to the carboxyl groups with O—H…O/N motifs previously seen in other carboxylic acids. Distinctive, however, is the presence of an extended though somewhat diffuse array of C—H…O hydrogen bonds that aggregates the entire solute-solvent assemblage in a multi-point manner. Pyridine and dmf are able to mimic each other with respect to their hydrogen bond donating and accepting characteristics and in this respect play equivalent roles in their solvates with morellic acid and gambogic acid. Dmso is seen to self-associate in its guttiferic acid solvate. It is possible that these solvents with multiple hydrogen bonding donor and acceptor capability can act as hydrogen bond nucleators, providing just enough rigidity to the solutes to ensure crystallization.     

Realization of vibronic entanglement in terms of tunneling current in an artificial molecule

Based on the concept of molecular nonadiabatic processes, namely, curve crossing and electronic interstate coupling, here we have introduced a model of an artificial molecule composed of three coupled quantum dots in terms of displaced harmonic oscillators of the confinement potential. We have shown that the static and dynamic features of vibronic entanglement can be realized in terms of the tunneling current in our model. An entanglement sudden-death can be shown to be equivalent to the suppression of tunneling current at the appropriate parameters of the magnetic field. We have also provided the nonclassicality of the vibration of the dot confinement potential which maximizes at the anticrossing zone.     

Box–Behnken Design-Based Development and Validation of a Reverse-Phase HPLC Analytical Method for the Estimation of Paclitaxel in Cationic Liposomes

Chromatographia - Stability-indicating reverse-phase HPLC analytical method for the quantification of Paclitaxel (PTX) in the bulk and cationic liposomes was developed. The optimized method was...     

Spatial dependency of the groundwater uranium in the alluvial soil region of Gunnaur,India

Journal of Radioanalytical and Nuclear Chemistry - GIS based groundwater uranium and other physico-chemical parameters pH, electrical conductivity, oxidation reduction potential, temperature,...     

Theoretical investigation of the molecular structure,vibrational spectra,and molecular docking of tramadol using density functional theory

The optimized molecular structures, harmonic vibrational wavenumbers, and the corresponding vibrational assignments of (1S,2S)-tramadol and (1R,2R)-tramadol are computationally examined using the B3LYP density functional theory method together with the standard 6–311++G(d,p) and def2-TVZP basis sets. The optimized structures show that phenolic rings of both 1R,2R and 1S,2S tramadol adopt planar geometry, which are slightly distorted due to the substitution at the meta-position; and the six-membered cyclohexane adopts a slightly distorted chair conformation. The 1S,2S enantiomer is energetically more favorable than 1R,2R with the energy differences of 1.32 and 1.03 kcal/mol obtained at B3LYP/6–311++G(d,p) and B3LYP/Def2-TVZP levels, respectively. The analysis of the binding pocket in the silico molecular docking with the m-opioid receptor shows that it originated two clusters with the 1S,2S enantiomer and one cluster with the 1R,2R enantiomer of tramadol. The results point to a more stable complex of the m-opioid receptor with the 1R,2R enantiomer of tramadol.     

Porous silicon layers prepared by electrochemical etching for application in silicon thin film solar cells

In this paper, multilayer structures of porous silicon were fabricated by using electrochemical etching and characterized for its optical properties and surface morphology. Samples of monolayer of porous silicon were grown to study the characteristics of porous layer formation with respect to applied current density, etching time and hydrofluoric acid concentrations. Photoluminescence peaks of red emission at wavelength 695 and 650 nm were observed from multilayer porous silicon structures. By atomic force microscopy measurement, hillocks like surface were clearly observed within the host material, which confirmed the formation of pores.     

Measurement and analysis of excitation functions for alpha-induced reactions in copper

Excitation functions for the production of⁶⁸Ga,⁶⁷Ga,⁶⁶Ga,⁶⁵Ga +⁶⁵Zn and⁶¹Cu fromα-induced reactions in natural copper have been measured in the energy range ≈ 10–40 MeV using the stacked foil technique. A stack of nine copper foils was irradiated by a 40 MeVα-beam. Theγ-rays emitted from the irradiated samples were recorded. Excitation functions have also been calculated theoretically using a statistical model with and without the inclusion of pre-equilibrium emission of particles. Pre-equilibrium component simulated by exciton model shows that the inclusion of pre-equilibrium emission gives better agreement between experimental and theoretical excitation functions. Pre-equilibrium fraction depends on the incident energy and the target mass number.