Submanifolds of complex space forms admitting an almost contact metric compound structure

Summary Real hypersurfaces of an almost Hermitian manifold naturally admit an almost contact metric structure and the (f, g, u, v, w, , , )-structure is defined on submanifolds of codimension 3 of an almost Hermitian manifold. We study the so-called semi-invariant submanifolds of a complex space form with almost contact metric compound structure which is a general notion of (f, g, u, v, w, , , )-structure.Dedicated to professor Eulyong Pak on his 60th birthdayThis research was partially supported by Korean Science and Engineering Foundation Grant.     

Loniceroside C,an antiinflammatory saponin from Lonicera japonica

A new triterpenoid saponin, loniceroside C was isolated from the aerial parts of Lonicera japonica. Its structure was established to be 3-O-beta-D-glucopyranosyl hederagenin 28-O-alpha-L-rhamnopyranosyl (1-->2)-[beta-D-xylopyranosyl(1-->6)]-beta-D-glucopyranosyl ester by spectroscopic techniques and chemical transformations. Loniceroside C showed in vivo antiinflammatory activity against mouse ear edema provoked by croton oil.     

Liquid–solid disk extraction followed by supercritical fluid elution and gas chromatography of phenols from water

A method combining the techniques of liquid – solid disk extraction (LSDE) and supercritical fluid elution (SFE) has been developed for the phenols regulated by the Clean Water Act. LSDE uses a disk or membrane made of polytetrafluoroethylene (PTFE) fibrils impregnated with small particles, e.g. styrene divinylbenzene (SDB) resin, to extract phenols from water. After disk extraction the retained analytes are eluted from the disk using SFE. SFE is used as an alternative to liquid solvent elution with an organic solvent. Analytes are separated, identified, and quantified using gas chromatography – ion trap detector mass spectrometry (GC-ITDMS). The method is capable of sub parts per billion detection limits, and precision of 5–28% RSD. Evaluation of various disks or membranes, such as C₁₈-silica disks, SDB disks, and ion exchange membranes, has also been performed for the extraction of phenols from water. The results obtained from the in-situ aqueous acetylation of phenols and extraction of their acetates are quantitative. The utilization of LSDE and SFE techniques has proven to be a more effective approach than liquid – liquid extraction in minimizing air pollution and solvent waste.     

CHIP-mediated hyperubiquitylation of tau promotes its self-assembly into the insoluble tau filaments

The tau protein is a highly soluble and natively unfolded protein. Under pathological conditions, tau undergoes multiple post-translational modifications (PTMs) and conformational changes to form insoluble filaments, which are the proteinaceous signatures of tauopathies. To dissect the crosstalk among tau PTMs during the aggregation process, we phosphorylated and ubiquitylated recombinant tau in vitro using GSK3β and CHIP, respectively. The resulting phospho–ub-tau contained conventional polyubiquitin chains with lysine 48 linkages, sufficient for proteasomal degradation, whereas unphosphorylated ub-tau species retained only one–three ubiquitin moieties. Mass-spectrometric analysis of in vitro reconstituted phospho–ub-tau revealed seven additional ubiquitylation sites, some of which are known to stabilize tau protofilament stacking in the human brain with tauopathy. When the ubiquitylation reaction was prolonged, phospho–ub-tau transformed into insoluble hyperubiquitylated tau species featuring fibrillar morphology and in vitro seeding activity. We developed a small-molecule inhibitor of CHIP through biophysical screening; this effectively suppressed tau ubiquitylation in vitro and delayed its aggregation in cultured cells including primary cultured neurons. Our biochemical findings point to a “multiple-hit model,” where sequential events of tau phosphorylation and hyperubiquitylation function as a key driver of the fibrillization process, thus indicating that targeting tau ubiquitylation may be an effective strategy to alleviate the course of tauopathies.

Multiple-hit model for tau aggregation, where sequential events of tau phosphorylation and hyperubiquitylation function as a key driver of the fibrillization process.     

A general strategy for the assignment of aliphatic side-chain resonances of uniformly 13C,15N-labeled large proteins

A general strategy is proposed to assign aliphatic side-chain resonances of large 13C,15N-labeled proteins without deuteration, using 4D 13C,15N-edited NOESY and MQ-(H)CCH-TOCSY experiments on the basis of prior assignments of backbone and 13Cbeta resonances. The strategy has been tested on a 214 residue protein (DdCAD-1) and applied to a chain-selectively 13C,15N-labeled hemoglobin (65 kDa). About 96 and 80% aliphatic side-chain spins in DdCAD-1 and hemoglobin have been assigned, respectively. The strategy proposed here will be very useful for the structure determination and dynamics characterization of large proteins by NMR.     

Effects of annealing treatment on the properties of MEH-PPV/titania hybrids prepared via in situ sol-gel reaction

A uniform poly[2-methoxy-5-(2′-ethylhexyloxy)-p-phenylenevinylene] (MEH-PPV)/titania hybrid film was successfully prepared by an in situ sol-gel reaction of titanium isopropoxide (TIP) in the presence of MEH-PPV/2-chlorophenol solution. The annealing treatment increased the conversion of TIP to titania as determined from evidence of the formation of Ti-O-Ti bonds in the Fourier transform infrared (FTIR) spectrum. Scanning electronic microscope (SEM) photographs showed that the morphology and distribution of titania in the hybrid film were strongly related to the amount of water in the in situ sol-gel reaction. The thermal stability of MEH-PPV/titania hybrids was enhanced by the annealing treatment. Small angle X-ray scattering (SAXS) and X-ray diffraction (XRD) analyses indicated that annealing treatment promoted the ordered aggregation of the MEH-PPV chains and crystallization of titania to a certain extent. The blue shift in Ultraviolet-visible (UV-vis) absorption of pure MEH-PPV after annealing was ascribed to the small extent of decomposition and coil conformation which occurred at high temperature. A more-obvious blue shift for the hybrids was observed, which resulted from irregular aggregation and coil conformation of the MEH-PPV chains induced by heterogeneous point, TIP (titania). The red shift in the photoluminescent (PL) emission for pure MEH-PPV resulted from a certain extent of ordered aggregation after annealing. However, only a slight red shift in the PL emission peak for the hybrids was found due to the hindrance of ordered aggregation of MEH-PPV chains in the presence of TIP (titania).     

Nucleophilic substitution by arenethiolates at the carbene carbon of pentacarbonyl(methoxymethylcarbene)-metal(o) complexes (metal = Cr,Mo, or W)

The phenylthiocarbene complexes, [(CO)₅MC(CH₃)(SPh)] (M = Cr, Mo, or W) have been prepared in good yield by the reaction of [(CO)₅MC(CH₃)(OCH₃)] (M = Cr, Mo, or W) with NaSPh in benzene/methanol in the presence of HCl. A series of para-substituted phenylthiocarbene complexes of tungsten. [(CO)₅WC(CH₃)SC₆H₄Y)], (Y = p-Br, p-F, p-H, p-CH₃, p-OCH₃ or p-OH) have also been prepared by the reaction of the appropriate arenethiolate ion with [(CO)₅WC(CH₃)(OCH₃)]. Poor nucleophiles such as p-nitrobenzenethiolate and pentafluorobenzenethiolate did not react with [(CO)₅WC(CH₃)(OCH₃) to form the corresponding phenylthiocarbene complex. A mechanism accounting for the formation of these phenylthiocarbene complexes is proposed. The complexes have been characterized by their infrared, electronic, mass, ¹H NMR, and ¹³C NMR spectra. These spectroscopic data have been used to establish the structure of these complexes in solution and indicate that the phenyl ring bonded to sulfur is probably not coplanar with the “carbene” plane.     

An evaluation of exogenous application of protoporphyrin IX and its dimethyl ester as a photodynamic diagnostic agent in poorly differentiated human nasopharyngeal carcinoma

5-Aminolevulinic acid and its esterified analogues have been under much investigation to enhance the endogenous production of protoporphyrin IX (PpIX) in tumor cells. However, in this work, we studied the in vitro and in vivo efficacy of exogenously administered PpIX and its esterified analogue, PpIX dimethyl ester (PME), in poorly differentiated human nasopharyngeal carcinoma (NPC/CNE-2) as a photodynamic diagnostic (PDD) agent. NPC/CNE-2 at its earliest time, 1 h after incubation with PME in in vitro studies, has exhibited 64% (P <0.01) higher tumor to normal cell (T/N) fluorescence ratio than with PpIX. In an in vivo mouse xenograft model, comparable photosensitizer concentration in tumor after intravenous administration was observed at 1-3 h time points, but at 9 h, PME had 31% (P=0.05) greater concentration in tumor compared with PpIX. In addition, by constituting PME and PpIX in different topical gel composites, of which, PME gel composition of 8:2 Plasdone and Gantrez resulted in the highest T/N ratio at 6 h after application (34%; P <0.05) in comparison with other gel composites. Evaluation of PME and PpIX constituted in the delivery vehicles investigated showed comparable selectivity for tumor at 1-3 h, thus neither photosensitizer is more efficient than the other for PDD at the early time points; however, beyond 6 h, PME had higher selectivity for tumor compared with PpIX. Thus, further investigation is warranted to improve the drug delivery vehicle for greater tumor selectivity at a shorter incubation time.