Kinetic and ESR studies on the radical polymerization of α‐n‐(α′‐methylbenzyl) β‐ethyl itaconamates derived from racemic and (s)‐α‐methylbenzylamines

The polymerization of α‐N‐(α′‐methylbenzyl) β‐ethyl itaconamate derived from racemic α‐methylbenzylamine (RS‐MBEI) by initiation with dimethyl 2,2′‐azobisisobutyrate (MAIB) was studied in methanol kinetically and with ESR spectroscopy. The overall activation energy of polymerization was calculated to be 47 kJ/mol, a very low value. The polymerization rate (R_p ) at 60 °C was expressed by R_p = k[MAIB]^0.5±0.05[RS‐MBEI]^2.9±0.1. The rate constants of propagation (k_p ) and termination (k_t ) were determined by ESR. k_p was very low, ranging from 0.3 to 0.8 L/mol s, and increased with the monomer concentration, whereas k_t (4–17 × l0⁴ L/mol s) decreased with the monomer concentration. Such behaviors of k_p and k_t were responsible for the high dependence of R_p on the monomer concentration. R_p depended considerably on the solvent used. S‐MBEI, derived from (S)‐α‐methylbenzylamine, showed somewhat lower homopolymerizability than RS‐MBEI. The k_p value of RS‐MBEI at 60 °C in benzene was 1.5 times that of S‐MBEI. This was explicable in terms of the different molecular associations of RS‐MBEI and S‐MBEI, as analyzed by ¹H NMR. © 2000 John Wiley & Sons, Inc. J Polym Sci A: Polym Chem 38: 4137–4146, 2000     

Synthesis of hydroxyl‐terminated poly(ether ether ketone) with pendent tert‐butyl groups and its use as a toughener for epoxy resins

Hydroxyl‐terminated poly(ether ether ketone) with pendent tert‐butyl groups (PEEKTOH) was synthesized by the nucleophilic substitution reaction of 4,4′‐difluorobenzophenone with tert‐butyl hydroquinone with potassium carbonate as a catalyst and N‐methyl‐2‐pyrrolidone as a solvent. Diglycidyl ether of bisphenol A epoxy resin was toughened with PEEKTOHs having different molecular weights. The melt‐mixed binary blends were homogeneous and showed a single composition‐dependent glass‐transition temperature (T_g). Kelley–Bueche and Gordon–Taylor equations gave good correlation with the experimental T_g. Scanning electron microscopy studies of the cured blends revealed a two‐phase morphology. A sea‐island morphology in which the thermoplastic was dispersed in a continuous matrix of epoxy resin was observed. Phase separation occurred by a nucleation and growth mechanism. The dynamic mechanical spectrum of the blends gave two peaks corresponding to epoxy‐rich and thermoplastic‐rich phases. The T_g of the epoxy‐rich phase was lower than that of the unmodified epoxy resin, indicating the presence of dissolved PEEKTOH in the epoxy matrix. There was an increase in the tensile strength with the addition of PEEKTOH. The fracture toughness increased by 135% with the addition of high‐molecular‐weight PEEKTOH. The improvement in the fracture toughness was dependent on the molecular weight and concentration of the oligomers present in the blend. Fracture mechanisms such as crack path deflection, ductile tearing of the thermoplastic, and local plastic deformation of the matrix occurred in the blends. The thermal stability of the blends was not affected by blending with PEEKTOH. © 2005 Wiley Periodicals, Inc. J Polym Sci Part B: Polym Phys 44: 541–556, 2006     

Isolation of salsolinol, a tetrahydroisoquinoline alkaloid, from the marine sponge Xestospongia cf. vansoesti as a proteasome inhibitor

Salsolinol (1), a tetrahydroisoquinoline alkaloid, was isolated from the marine sponge Xestospongia cf. vansoesti collected in Indonesia as a proteasome inhibitor, along with three salsolinol derivatives, norsalsolinol (2), cis-4-hydroxysalsolinol (3), and trans-4-hydroxysalsolinol (4). Compounds 1 and 2 inhibited the chymotrypsin-like activity of the proteasome with IC(50) values of 50 and 32 μg/ml, respectively, but 3 and 4 showed no inhibitory effect even at 100 μg/ml.     

Evaluation of a dichromatic color-appearance simulation by a visual search task

We used a visual search task to investigate the validity of the dichromatic simulation model proposed by Brettel et al. Although the dichromatic simulation could qualitatively predict reaction times for color-defective observers, the reaction times for color-defective observers tended to be longer than those of the trichromatic observers in Experiment 1. In Experiment 2, we showed that a reduction of purity excitation of simulated colors can provide a good prediction. Further, we propose an adaptive dichromatic simulation model based on the color differences between a simulated target color and simulated distractor colors in order to obtain a better quantitative prediction of reaction times in the visual search task for color defects.     

Omaezallene from Red Alga Laurencia sp.: Structure Elucidation,Total Synthesis,and Antifouling Activity

Natural antifouling products have been the subject of considerable attention. We screened marine algae for antifouling activity and discovered omaezallenes, the new bromoallene‐containing natural products isolated from the red alga Laurencia sp. Described is the isolation, structure elucidation, and total syntheses of omaezallenes. The relative and absolute configurations of natural omaezallenes were unambiguously established through total synthesis. The antifouling activities and ecotoxicity of omaezallenes were also evaluated.     

Allostery of the two-state model of hemoglobin studied by ECEPP energy minimization

Recently, a powerful parallel-vector processor became available for molecular science. A new FORTRUN program was coded to treat the whole hemoglobin molecule with twofold symmetry. Using the X-ray coordinates of deoxyhemoglobin and oxyhemoglobin, minimum energy conformations were obtained for both the T-state and the R-state on the two-state model of allostery. From them, further energy minimization was performed with simple perturbation to bring the proximal region close to the heme group instead of oxygen binding, and the structural changes and energy changes were investigated. The difference of calculated energy changes between T and R was semiquantitatively in agreement with the experimental value 2.7 kcal/mol for one oxygen binding. When the perturbation was exerted on the alpha-subunits, the energy change within the perturbed alpha-subunits in the T-state gave a main contribution, and in the R-state, the structural changes of the alpha-subunits were specifically large. When the perturbation was exerted on the beta-subunits, the intersubunit interaction energy between alpha1 and beta2 (alpha2 and beta1) was dominant in the difference of the energy changes between T and R.     

Controlled drug release through poly(L-leucine) and its copolymer

The release behavior of a water-soluble drug through membranes made of poly(L-leucine) and its copolymer with different hydrophilic properties was studied. The effect of casting methods on the release rate was also investigated. It was found that the membrane with a higher hydrophilic property resulted in a higher permeation rate. The capsule was prepared as a composite sheet from a poly(L-leucine)-prednisolone 21-sodium succinate sponge and a poly(L-leucine) membrane. Release of the water-soluble drug from the capsule was found to be effectively governed by the hydrophilic character and thickness of the outer membrane. Biocompatibility studies carried out by implanting the poly(L-leucine) sponge subcutaneously in the dorsal surface of the rat showed that the sponge had a good biocompatibility and slow biodegradation. It was concluded from these results that poly(L-leucine) should be a suitable material for preparing a controlledrelease drug device for long-term dosage.     

Determination of phenothiazines in human body fluids by solid-phase microextraction and liquid chromatography/tandem mass spectrometry

Eleven phenothiazine derivatives with heavy side-chains were found to be extractable from human whole blood and urine samples by solid-phase microextraction (SPME) with a polyacrylate-coated fiber. The fiber was then injected into the desorption chamber of an SPME-liquid chromatography (LC) interface for LC/tandem mass spectrometry (MS/MS) with positive ion electrospray (ES) ionization. All compounds formed base peaks due to [M + 1](+) ions by LC/ES-MS/MS. By use of LC/ES-MS/MS, the product ions produced from each [M + 1](+) ion showed base peaks due to side-chain liberation. Selected reaction monitoring (SRM) and selected ion monitoring (SIM) were compared for the detection of the 11 phenothiazine derivatives from human whole blood and urine. SRM showed much higher sensitivity than SIM for both types of sample. Therefore, a detailed procedure for the detection of drugs by SRM with SPME-LC/MS/MS was established and carefully validated. The extraction efficiencies of the 11 phenothiazine derivatives spiked into whole blood and urine were 0. 0002-0.12 and 2.6-39.8%, respectively. The regression equations for the 11 phenothiazine derivatives showed excellent linearity with detection limits of 0.2-200 ng ml(-1) for whole blood and 4-22 pg ml(-1) for urine. The intra- and inter-day precisions for whole blood and urine samples were not greater than 15.1%. The data obtained after oral administration of perazine or flupentixol to a male subject are presented.     

Comparison of SSI with APCI as an interface of HPLC-mass spectrometry for analysis of a drug and its metabolites

Sonic spray ionization (SSI) was compared with atmospheric pressure chemical ionization (APCI) as an interface of high-performance liquid chromatography (HPLC)-mass spectrometry (MS) for sensitive analyses of a neuroleptic drug, haloperidol and its two metabolites, such as reduced haloperidol and 4-(4-chlorophenyl)-4-hydroxypiperidine (CPHP), in biological samples. For both SSI and APCI interfaces, HPLC-MS-MS gave higher sensitivity than HPLC-MS. The sensitivities by HPLC-SSI-MS-MS for haloperidol and reduced haloperidol were 100 and 30 times higher, respectively, than those by HPLC-APCI-MS-MS; no spectrum with recognizable peaks was obtained for CPHP with the APCI interface. Therefore, detection limits and regression equations were examined by the HPLC-SSI-MS-MS for human plasma and urine samples spiked with the above drug and its metabolites. Haloperidol, reduced haloperidol, and CPHP showed good linearity in the ranges of 5-800, 10-800, and 100-800 ng/mL, respectively, for both human plasma and urine; their detection limits were 2.5, 5, and 75 ng/mL, respectively, using a new polymer HPLC column which enabled direct application of biological samples.