Mixed-metal tellurites: synthesis, structure, and characterization of Na1.4Nb3Te4.9O18 and NaNb3Te4O16

Two new mixed-metal tellurites, Na1.4Nb3Te4.9O18 and NaNb3Te4O16, have been synthesized by standard solid-state techniques using Na2CO3, Nb2O5, and TeO2 as reagents. The structures of Na1.4Nb3Te4.9O18 and NaNb3Te4O16 were determined by single-crystal X-ray diffraction. Both of the materials exhibit three-dimensional structures composed of NbO6 octahedra, TeO4, and TeO3 polyhedra. The Nb5+ and Te4+ cations are in asymmetric coordination environments attributable to second-order Jahn-Teller (SOJT) effects. The Nb5+ cations undergo an intraoctahedral distortion toward a corner (local C4 direction), whereas the Te4+ cations are in distorted environments owing to their nonbonded electron pair. Infrared and Raman spectroscopy, UV-vis diffuse reflectance spectroscopy, thermogravimetric analysis, and dielectric measurements were also performed on the reported materials. Crystal data: Na1.4Nb3Te4.9O18, monoclinic, space group C2/m (No. 12), with a = 32.377(5) A, b = 7.4541(11) A, c = 6.5649(9) A, beta = 95.636(5) degrees, V = 1576.7(4) A3, and Z = 4; NaNb3Te4O16, monoclinic, space group P2(1)/m (No. 11), with a = 6.6126(13) A, b = 7.4738(15) A, c = 14.034(3) A, beta = 102.98(3) degrees, V = 675.9(3) A3, and Z = 2.     

Cancer cells undergoing epigenetic transition show short-term resistance and are transformed into cells with medium-term resistance by drug treatment

To elucidate the epigenetic mechanisms of drug resistance, epigenetically reprogrammed H460 cancer cells (R-H460) were established by the transient introduction of reprogramming factors. Then, the R-H460 cells were induced to differentiate by the withdrawal of stem cell media for various durations, which resulted in differentiated R-H460 cells (dR-H460). Notably, dR-H460 cells differentiated for 13 days (13dR-H460 cells) formed a significantly greater number of colonies showing drug resistance to both cisplatin and paclitaxel, whereas the dR-H460 cells differentiated for 40 days (40dR-H460 cells) lost drug resistance; this suggests that 13dR-cancer cells present short-term resistance (less than a month). Similarly, increased drug resistance to both cisplatin and paclitaxel was observed in another R-cancer cell model prepared from N87 cells. The resistant phenotype of the cisplatin-resistant (CR) colonies obtained through cisplatin treatment was maintained for 2–3 months after drug treatment, suggesting that drug treatment transforms cells with short-term resistance into cells with medium-term resistance. In single-cell analyses, heterogeneity was not found to increase in 13dR-H460 cells, suggesting that cancer cells with short-term resistance, rather than heterogeneous cells, may confer epigenetically driven drug resistance in our reprogrammed cancer model. The epigenetically driven short-term and medium-term drug resistance mechanisms could provide new cancer-fighting strategies involving the control of cancer cells during epigenetic transition.Subject terms: Tumour heterogeneity, Epigenetics     

Performance of hollow-fiber flow field-flow fractionation in protein separation

Since hollow-fiber flow field-flow fractionation (HF FIFFF) utilizes a cylindrical channel made of a hollow-fiber membrane, which is inexpensive and simple in channel assembly and thus disposable, interests are increasing as a potential separation device in cells, proteins, and macromolecules. In this study, performance of HF FIFFF of proteins is described by examining the influence of flow rate conditions and length of fiber (polyacrylonitrile or PAN in this work) on sample recovery as well as experimental plate heights. The interfiber reproducibility in terms of separation time and recovery was also studied. Experiments showed that sample recovery was consistent regardless of the length of fiber when the effective field strength (equivalent to the mean flow velocity at the fiber wall) and the channel void time were adjusted to be equivalent for channels of various fiber lengths. This supported that the majority of sample loss in HF FIFFF separation of apoferritin and their aggregates may occur before the migration process. It is finally demonstrated that HF FIFFF can be applied for characterizing the reduction in Stokes' size of low density lipoproteins from blood plasma samples obtained from patients having coronary artery disease and from healthy donors.     

Separation of carbon nanotubes by frit inlet asymmetrical flow field-flow fractionation

Flow field-flow fractionation (flow FFF), a separation technique for particles and macromolecules, has been used to separate carbon nanotubes (CNT). The carbon nanotube ropes that were purified from a raw carbon nanotube mixture by acidic reflux followed by cross-flow filtration using a hollow fiber module were cut into shorter lengths by sonication under a concentrated acid mixture. The cut carbon nanotubes were separated by using a modified flow FFF channel system, frit inlet asymmetrical flow FFF (FI AFIFFF) channel, which was useful in the continuous flow operation during injection and separation. Carbon nanotubes, before and after the cutting process, were clearly distinguished by their retention profiles. The narrow volume fractions of CNT collected during flow FFF runs were confirmed by field emission scanning electron microscopy and Raman spectroscopy. Experimentally, it was found that retention of carbon nanotubes in flow FFF was dependent on the use of surfactant for CNT dispersion and for the carrier solution in flow FFF. In this work, the use of flow FFF for the size differentiation of carbon nanotubes in the process of preparation or purification was demonstrated.     

Potentiodynamic deposition of Prussian blue from a solution containing single component of ferricyanide and its mechanism investigation

Potentiodynamic techniques were used for the direct electrodeposition of Prussian blue nano-clusters from an acidic solution of ferricyanide. Electrochemical, EQCM, IR, AFM, and UV/vis measurements were carried out to characterize deposited nano-sized Prussian blue and to explore the formation mechanism. Results showed that ferricyanide could partially dissociate to free ferric and cyanide ions. The driving force of this dissociation is the formation of PB and the evolution of HCN. The optimal potential window for the potentiodynamic formation of PB from an acidic solution (pH 1.6) is between –0.5 V and 0.4 V. In addition, the influence of surface adsorption of CN^- ions on the formation of PB was discussed.Dedicated to Professor W. Vielstich on the occasion of his 80th birthday.     

Absorption, first-pass metabolism, and disposition of itraconazole in rats

This study examined the pharmacokinetic disposition, oral absorption and hepatic extraction of itraconazole and its active metabolite, hydroxyitraconazole, in rats. After i.v. injection, serum itraconazole concentrations decreased biexponentially, with an average terminal elimination half-life, volume of distribution and systemic clearance of 4.9 h, 6.0 l/kg and 14.2 ml/min/kg, respectively. When given orally, its absorption was low, with a mean absolute bioavailability of 16.6%. The metabolite to parent drug area under the curve (AUC) ratio was higher after oral administration compared with i.v. injection (mean ratio, 2.7 vs. 0.9). The hepatic drug extraction ratio determined after femoral and portal vein administration averaged 18.5%. When hydroxyitraconazole was injected i.v., the elimination half-life, volume of distribution and systemic clearance of itraconazole averaged 10.0 h, 2.4 l/kg and 3.4 ml/min/kg, respectively. The fraction of the systemically available itraconazole that was metabolized to hydroxyitraconazole was 21.0% and 76.0% after i.v. and oral administration, respectively. In summary, this study is the first reporting the hepatic extraction of itraconazole and the i.v. disposition characteristics of hydroxyitraconazole in rats. Itraconazole is a drug with a low hepatic extraction ratio and its systemic clearance appears to be largely accounted for by hepatic metabolism.     

Electrically conducting electrospun silk membranes fabricated by adsorption of carbon nanotubes

We present a simple method of obtaining electrically conducting electrospun silk non-woven membranes consisting of nanofibers with multi-walled carbon nanotubes (MWCNTs) adsorbed on their surface. Nanofibrous membranes with fibroin diameters of 460 ± 40 nm were formed from aqueous Bombyx mori fibroin solution by electrospinning. The MWCNTs adhered well to the surface of the highly porous silk nanofibrous membranes when Triton X-100 was used as the surfactant for the dispersion of the MWCNTs in aqueous media. The electrical conductivity of the membranes was 2.4 × 10⁻⁴ S/cm due to the presence of the MWCNTs on their surface. In addition, the strong interaction between the MWCNTs and nanofibers keeps them from separating each other, even after ultrasonication. The combination of the high conductivity of the membranes and the simple process used to fabricate them could lead to significant advances in the development of new materials, such as electromagnetic interference shielding or electrostatic dissipation membranes.     

Hydrogenated polybutadiene–polymethyl methacrylate (HPB–PMMA) block copolymer. I. Synthesis of polybutadiene–polymethyl methacrylate (PB–PMMA) block copolymer

To get hydrogenated polybutadiene-polymethyl methacrylate (HPB-b-PMMA) block copolymer to be used as a compatibilizer for blends of polyolefin/polar polymer, PB-b-PMMA was synthesized by anionic-free radical mechanism transformation polymerization. Selective extraction, gradient elution thin layer chromatography, and oil-oil emulsion separation techniques were tried to attempt to separate the copolymerization products. Hydrogenation of the PB sequence in PB-b-PMMA yielded HPB-b-PMMA. The compatibilizing function of PB-b-PMMA was shown in blending experiments. © 1993 John Wiley & Sons, Inc.     

Molecular characteristics of the inhibition of human neutrophil elastase by nonsteroidal antiinflammatory drugs

Nonsteroidal antiinflammatory drugs(NSAIDs) are known as clinically effective agents for treatment of inflammatory diseases. Inhibition of cyclooxygenase has been thought to be a major facet of the pharmacological mechanism of NSAIDs. However, it is difficult to ascribe the antiinflammatory effects of NSAIDs solely to the inhibition of prostaglandin synthesis. Human neutrophil elastase (HNElastase; HNE, EC 3.4.21.37) has been known as a causative factor in inflammatory diseases. To investigate the specific relationship between HNElastase inhibition and specificity of molecular structure of several NSAIDs, HNElastase was purified by Ultrogel AcA54 gel filtration, CM-Sephadex ion exchange, and HPLC (with TSK 250 column) chromatography. HNElastase was inhibited by aspirin and salicylate in a competitive manner and by naproxen, ketoprofen, phenylbutazone, and oxyphenbutazone in a partial competative manner, but not by ibuprofen and tolmetin. HNElastase-phenylbutazone-complex showed strong Raman shifts at 200, 440, 1124, 1194, 1384, 1506, and 1768 cm(-1). The Raman bands 1194, 1384, and 1768 cm(-1) may represent evidences of the conformational change at -N=N-phi radical, pyrazol ring, and -C=O radical of the elastase-drug complex, respectively. Phenylbutazone might be bound to HNElastase by ionic and hydrophobic interaction, and masked the active site. Inhibition of HNElastase could be another mechanism of action of NSAIDs besides cyclooxygenase inhibition in the treatment of inflammatory diseases. Different inhibition characteristics of HNE-lastase by NSAIDs such as aspirin, phenylbutazone-like drugs and ineffective drugs could be important points for drawing the criteria for appropriate drugs in clinical application.     

Electroosmotic flow in a capillary annulus with high zeta potentials

The electroosmotic flow through an annulus is analyzed under the situation when the two cylindrical walls carry high zeta potentials. The analytical solutions for the electric potential profile and the electroosmotic flow field in the annulus are obtained by solving the Poisson-Boltzmann equation and the Stokes equation under an analytical scheme for the hyperbolic sine function. A mathematical expression for the average electroosmotic velocity is derived in a fashion similar to the Smoluchowski equation. Hence, a correction formula is introduced to modify the Smoluchowski equation, taking into account contributions due to the finite thickness of the electric double layer (EDL) and the geometry ratio-dependent correction. Specifically, under a circumstance when the two annular walls are oppositely charged, the flow direction can be determined from the sign of such correction formula, and there exists a zero-velocity plane inside the annulus. With the assumption of large electrokinetic diameters, the location of the zero-velocity plane can be estimated from the analytical expression for the velocity distribution. In addition, the characteristics of the electroosmotic flow through the annulus are discussed under the influences of the EDL parameters and geometric ratio of the inner radius to the outer radius of the annulus.