Hamanncook7299
The simulations show that the preference of Ca2+ to the LAS molecules is due to a strong specific attraction with the sulfonate head-group, besides the electrostatic one. This specific attraction involves significant reduction of the hydration shells of the interacting calcium cation and sulfonate group, which couple directly and form surface clusters of LAS molecules, coordinated around the adsorbed Ca2+ ions. In contrast, SLES molecules do not exhibit such specific interaction because the hydration shell around the sulfate anion is more stable, due to the extra oxygen atom in the sulfate group, thus precluding substantial dehydration and direct coupling with any of the cations studied.In this work, two hydrolysis reactions were used as a probe to investigate the properties of reverse micelles (RMs) formed by the ionic liquid-surfactant 1-butyl-3-methylimidazolium 1,4-bis-2-ethylhexylsulfosuccinate (bmim-AOT). The results were compared with those found for RMs generated with sodium 1,4-bis-2-ethylhexylsulfosuccinate (Na-AOT). As external nonpolar solvents, n-heptane (n-Hp), isopropyl myristate (IPM), and methyl laurate (ML) were used. Thus, the effect of changing the Na+ cation by bmim+ was analyzed, as well as the impact of the replacement of a conventional external nonpolar solvent by biocompatible solvents. The kinetics of the hydrolysis reactions of 4-methoxybenzoyl chloride (OMe) and 4-(trifluoromethyl)benzoyl chloride (CF3) were studied. The results indicate that the replacement of the Na+ counterion by bmim+ in AOT RMs alters the rates of reactions carried out in them and produces changes in the reaction mechanism. In bmim-AOT RMs, the bmim+ cation is located between the surfactant molecules; this has an important influence on the reaction intermediates' stability and, therefore, in the reaction rates and mechanisms. Also, the results indicate that when IPM is used as an external solvent instead of ML or n-Hp, interfacial water molecules have larger nucleophilicity due to the higher interface penetration of IPM.Imatinib, a drug used for the treatment of chronic myeloid leukemia and other cancers, works by blocking the catalytic site of pathological constitutively active Abl kinase. While the binding pose is known from X-ray crystallography, the different steps leading to the formation of the complex are not well understood. The results from extensive molecular dynamics simulations show that imatinib can primarily exit the known crystallographic binding pose through the cleft of the binding site or by sliding under the αC helix. Once displaced from the crystallographic binding pose, imatinib becomes trapped in intermediate states. These intermediates are characterized by a high diversity of ligand orientations and conformations, and relaxation timescales within this region may exceed 3-4 ms. Analysis indicates that the metastable intermediate states should be spectroscopically indistinguishable from the crystallographic binding pose, in agreement with tryptophan stopped-flow fluorescence experiments.By the emergence and worldwide spread of multi-drug-resistant Gram-negative bacteria, there have been growing demands for efficacious drugs to cure these resistant infections. The key mechanism for resistance to β-lactam antibiotics is the production of β-lactamases, which hydrolyze and deactivate β-lactams. Diazabicyclooctane (DBO) analogs play an important role as one of the new classes of β-lactamase inhibitors (BLIs), and several compounds such as avibactam (AVI) have been approved by the FDA, along with many derivatives under clinical or preclinical development. Although these compounds have a similar amide substituent at the C2 position, we have recently reported the synthesis of novel DBO analogs which possess a thio functional group. This structural modification enhances the ability to restore the antimicrobial activities of cefixime (CMF) against pathogens producing classes A, C, and D serine β-lactamases compared with AVI and expands the structural tolerance at the six position. Furthermore, some of these analogs showed intrinsic microbial activities based on multipenicillin binding protein (PBP) inhibition. This is the unique feature which has never been observed in DBOs. One of our DBOs had a pharmacokinetic profile comparable to that of other DBOs. These results indicate that the introduction of a thio functional group into DBO is a novel and effective modification to discover a clinically useful new BLI.Developing microstructure and multifunctional membranes toward switchable oil-water separation has been highly desired in oily wastewater treatment. Herein, a controllable Janus nozzle was employed to innovatively electrospin natural loofah/poly(vinylidene fluoride) (PVDF) nanofibers with a core-shell structure for gravity-driven water purification. By adjusting flow rates of the PVDF component, a core-shell structure of the composite fibers was obtained caused by the lower viscosity and surface tension of PVDF. In addition, a steady laminar motion of fluids was constructed based on the Reynolds number of flow fields being less than 2300. In order to investigate the formation mechanism of the microstructure, a series of Janus nozzles with different lengths were controlled to study the blending of the two immiscible components. The gravity difference between the two components might cause disturbance of the jet motion, and the PVDF component unidirectionally encapsulated the loofah to form the shell layer. Most importantly, the dry loofah/PVDF membranes could separate oil from an oil-water mixture, while the water-wetted membrane exhibited switchable separation that could separate water from the mixtures because of the hydroxyl groups of the hydrophilic loofah hydrogen-bonding with water molecules and forming a hydration layer. Selleck SY-5609 The composite fibers can be applied in water remediation in practice, and the method to produce core-shell structures seems attractive for technological applications involving macroscopic core-shell nano- or microfibers.An efficient and facile protocol for the synthesis of biologically and pharmaceutically important phthalimides is developed by l-proline-catalyzed reaction between two dienophiles of α,β-unsaturated aldehydes and maleimides. The reaction involves an efficient benzannulation that proceeds via a formal [4 + 2] cycloaddition of azadiene intermediates generated in situ from enals and N-substituted maleimides. This protocol provides a variety of functionalized phthalimide derivatives, including a potent COX-2 enzyme inhibitor.