ELEMENTAL SELENIUM GENERATED BY THE PHOTOBLEACHING OF SELENOMEROCYANINE PHOTOSENSITIZERS FORMS CONJUGATES WITH SERUM MACROMOLECULES THAT ARE TOXIC TO TUMOR CELLS

Elemental selenium generated by the photobleaching of selenomerocyanine dyes forms conjugates with serum albumin and serum lipoproteins that are toxic to leukemia and selected solid tumor cells but well tolerated by normal CD34-positive hematopoietic stem and progenitor cells. Serum albumin and lipoproteins act as Trojan horses that deliver the cytotoxic entity (elemental selenium) to tumor cells as part of a physiological process. They exploit the fact that many tumors have an increased demand for albumin and/or low-density lipoprotein. Se(0)-protein conjugates are more toxic than selenium dioxide, sodium selenite, selenomethionine, or selenocystine. They are only minimally affected by drug resistance mechanism, and they potentiate the cytotoxic effect of ionizing radiation and several standard chemotherapeutic agents. The cytotoxic mechanism of Se(0)-protein conjugates is not yet fully understood. Currently available data are consistent with the notion that Se(0)-protein conjugates act as air oxidation catalysts that cause a rapid depletion of intracellular glutathione and induce apoptosis. Drugs modeled after our Se(0)-protein conjugates may prove useful for the local and/or systemic therapy of cancer.     

Heterodimerization of dye-modified cyclodextrins with native cyclodextrins

The heterodimerization behavior of dye-modified beta-cyclodextrins (1-6) with native cyclodextrins (CDs) was investigated by means of absorption and induced circular dichroism spectroscopy in an aqueous solution. Three types of azo dye-modified beta-CDs (1-3) show different association behaviors, depending on the positional difference and the electronic character of substituent connected to the CD unit in the dye moiety. p-Methyl red-modified beta-CD (1), which has a 4-(dimethylamino)azobenzene moiety connected to the CD unit at the 4' position by an amido linkage, forms an intramolecular self-complex, inserting the dye moiety in its beta-CD cavity. It also associates with the native alpha-CD by inserting the moiety of 1 into the alpha-CD cavity. The association constants for such heterodimerization are 198 M(-1) at pH 1.00 and 305 M(-1) at pH 6.59, which are larger than the association constant of 1 for beta-CD (43 M(-1) at pH 1.00). Methyl red-modified 2, which has the same dye moiety as that for 1 although its substituent position is different from that of 1, does not associate even with alpha-CD due to the stable self-intramolecular complex, in which the dye moiety is deeply included in its own cavity of beta-CD. Alizarin yellow-modified CD (3), which has an azo dye moiety different from that of 1 and 2, caused a slight spectral variation upon addition of alpha-CD, suggesting that the interaction between 3 and alpha-CD is weak. On the other hand, phenolphthalein-modified beta-CD (4), which forms an intermolecular association complex in its higher concentrations, binds with beta-CD with an association constant of 787 M(-1) at pH 10.80, where 4 exists as the dianion monomer in the absence of beta-CD. p-Nitorophenol-modified beta-CDs (5 and 6), each having p-nitorophenol moieties with a different connecting part with an amido and amidophenyl group, respectively, associated with alpha-CD with association constants of 66 and 16 M(-1) for 5 and 6, respectively. The phenyl unit in the connecting part of 6 may prevent the smooth binding with alpha-CD. All these results suggest that the dye-modified CDs, in which the dye part is not tightly included in its CD cavity, associate with the native CD to form heterodimer composed of two different CD units by inserting the dye moiety into the native CD unit. The resulting heterodimers have a cavity that can bind another appending moiety of host molecules. On this basis, more ordered molecular arrays or the supramolecular hereropolymers can be constructed.     

Preparation and properties of polysilsesquioxanes: Polysilsesquioxanes and flexible thin films by acid‐catalyzed controlled hydrolytic polycondensation of methyl‐ and vinyltrimethoxysilane

Polymethylsilsesquioxane (PMS) and polyvinylsilsesquioxane (PVS) were prepared by acid‐catalyzed controlled hydrolytic polycondensation of methyl‐ and vinyltrimethoxysilane (MTS and VTS), respectively. The spinnabilities and molecular weights of polysilsesquioxanes were easily controlled by the reaction conditions, such as the molar ratios of water, hydrochloric acid, and methanol to MTS or VTS; nitrogen flow rate; temperature; and stirring rate. PMS and PVS showed spinnability of more than 200 cm when their molecular weights were up to 42,000 (PMS) and 19,000 (PVS) M_w. Transparent, colorless, and flexible films of 0.02–0.10 mm thick were prepared by casting a 20 wt % acetone–methanol (V/V = 1) solution of PMS and PVS on a polymethylpentene shale, followed by heating at 80°C for 3 weeks. The tensile strength of the films, approximately 26 (PMS) and 17 (PVS) MPa, was found to be correlated with the structure of the polysilsesquioxanes. The surface contact angle and electroconductivity of films were also measured. © 1999 John Wiley & Sons, Inc. J Polym Sci A: Polym Chem 37: 1017–1026, 1999     

SugarDrawer: A Web-Based Database Search Tool with Editing Glycan Structures

In life science fields, database integration is progressing and contributing to collaboration between different research fields, including the glycosciences. The integration of glycan databases has greatly progressed collaboration worldwide with the development of the international glycan structure repository, GlyTouCan. This trend has increased the need for a tool by which researchers in various fields can easily search glycan structures from integrated databases. We have developed a web-based glycan structure search tool, SugarDrawer, which supports the depiction of glycans including ambiguity, such as glycan fragments which contain underdetermined linkages, and a database search for glycans drawn on the canvas. This tool provides an easy editing feature for various glycan structures in just a few steps using template structures and pop-up windows which allow users to select specific information for each structure element. This tool has a unique feature for selecting possible attachment sites, which is defined in the Symbol Nomenclature for Glycans (SNFG). In addition, this tool can input and output glycans in WURCS and GlycoCT formats, which are the most commonly-used text formats for glycan structures.     

Concept of Photorefractive Connection Module by Photorefractive Four-Wave Mixing with Extraordinary Writing Beams and an Ordinary Reading Beam

We propose a new optical network device photorefractive connection module (PRCM) which operates as optical switch, amplifier and signal distributor controlled by parallel optical signals. Simple optical control bus systems can be realized by cascade connection of PRCMs. PRCM branches off a desired channel from the spatial multiplexed optical bus line by appropriate setting of the control beam pattern. PRCM uses cross polarized four wave mixing (CPFWM) with extraordinary polarized writing beams and an ordinary polarized reading beam to achieve a high connection gain to the next PRCM stage. We analyze the phase matching angle of CPFWM in which the optical paths of two pump beams are slightly different. The phase conjugate reflectivity indicating a branching ratio of optical signal is derived and calculated in consideration of the phase mismatching Δk. The optimum pump ratio and the grating vector orientation for the largest phase conjugate reflectivity and signal amplification factor are discussed for optical design of PRCM. Since the measured signal beam power after passing through the BaTiO₃ crystal is three or four times higher than its incident power, PRCM has a sufficient connection gain for optical bus and interconnection systems.     

Studies of multilayers of Cu-Hf with a variable-energy positron beam

We report on the results of depth-profiling experiments of multilayers of Cu-Hf using a slow position beam. Experimental data reveal that the Hf layers contain many open-volume type defects and that there might be thin oxidized Hf that reduces theS parameter in the interfaces between Cu-Hf.     

An improved method for proteomics studies in C. elegans by fluorogenic derivatization, HPLC isolation, enzymatic digestion and liquid chromatography--tandem mass spectrometric identification

An improved method for proteomics studies, which includes the fluorogenic derivertization of protein mixtures with 7-chloro-4-(dimethylaminoethylaminosulfonyl)-2,1,3-benzoxadiazole (DAABD-Cl), followed by HPLC isolation, enzymatic digestion and identification of the derivatized proteins by HPLC-electrospray ionization (ESI)-MS/MS with the probability-based protein identification algorithm, identified 103 proteins in the soluble extract (10 microg protein) of Caenorhabditis elegans.     

Functional polymers. 6. Unusual catalysis of polymeric cinchona alkaloids in asymmetric reaction

Acrylonitrile-cinchona alkaloid copolymers catalyzed the asymmetric addition of benzyl mercaptan to 2-nitrostyrene to give always (+)-enantiomer in excess, indicating the participation of C(3)-chirality in the enantioface differentiating step.     

Functional polymers. II. Synthesis and properties of new polymeric cinchona alkaloids

New polymeric cinchona alkaloids having favorable structures and properties for asymmetric catalysts have been prepared by radical copolymerization of the alkaloids with acrylonitrile using azobisisobutyronitrile (AIBN) as an initiator. Of the many reaction solvents tried, dimethylformamide (DMF) was found to be the solvent of choice especially for a large-scale synthesis. Alkaloid monomers employed were free dalkaloids, such as quinine, quinidine, cinchonidine, and cinchonine, and modified ones including 9-O-ethoxycarbonylquinine and quinine salts. The copolymers were thermally stable powders, soluble in DMF and DMSO, and insoluble in common organic solvents. They were found to be converted into water-soluble polymeric alkaloids by hydrolysis with alkaline hydrogen peroxide.