A novel fluorescence method for the determination of the critical micelle concentration (cmc) is reported. The cmc values of nonionic and anionic surfactants were evaluated utilizing a photosensitive monoazacryptand-Ba2+ complex, whose fluorescence intensity is sensitively changed by environmental conditions based on the photoinduced electron transfer (PET) mechanism as a fluorescent probe (PET method). Based on a comparison of the cmc values obtained by the PET method versus those obtained by conventional fluorescence-based methods as well as the values reported in the literature, one can conclude that the PET method is useful for the cmc determination. In particular, the PET method was more effective for the cmc determination of nonionic surfactants with very low cmc values (< 10(-5) M) than any other fluorescence-based method. In the cases of anionic surfactants, the PET method revealed the formation of the premicellar aggregates comprised of surfactant molecules and fluorescent probes below the cmc. Moreover, the hydrophobicity around the monoazacryptand-Ba2+ complex incorporated into various nonionic surfactant micelles was evaluated by this PET method. 相似文献
[reaction: see text] Skeleton-modified cyclodextrin (CD) derivatives, in which an alpha-(1,4)-glucosidic bond is converted into a beta-(1,4)-glucosidic bond, were conveniently synthesized by cleavage of a single glucosidic bond in permethylated and 2,6-di-O-methylated alpha- and beta-CDs and subsequent recyclization via the trichloroacetoimidate intermediates. The selective cleavage of an alpha-(1,4)-glucosidic bond of permethylated alpha- and beta-CDs was accomplished by stirring in 30% aq HClO(4) at 25 degrees C to give the corresponding maltohexaose and maltoheptaose derivatives, respectively. The cleavage of a glucosidic bond of hexakis(3-O-benzyl-2,6-di-O-methyl)-alpha-CD was successfully carried out in a mixed 60% aq HClO(4) and 1,4-dioxane solution (1:20). In the case of heptakis(3-O-benzyl-2,6-di-O-methyl)-beta-CD, the solvent-free reaction with p-toluenesulfonic acid was found to be effective for selective cleavage of one glucosidic bond. The permethylated beta-CD derivative with a beta-(1,4)-glucosidic bond (4b) exhibited higher inclusion ability toward sodium m-nitrobenzoate than the parent permethylated beta-CD, while these hosts showed the same inclusion ability toward sodium p-nitrobenzoate. On the other hand, the beta-(1,4)-type permethylated alpha-CD derivative 4a exhibited lower inclusion ability toward sodium p- and m-nitrobenzoates than the parent permethylated alpha-CD. Interestingly, host molecules 4a and 4b showed inclusion selectivity for sodium m-nitrobenzoate as compared with the corresponding para-isomer, in contrast to permethylated CDs which possessed para-isomer selectivity. On the other hand, host molecules 4a and 4b showed para-isomer selectivity toward sodium nitrophenoxide guests, indicating that the inclusion selectivity was remarkably influenced by the guest hydrophilic groups. (1)H NMR studies on complexes of those beta-(1,4)-type CD derivatives with p- and m-nitrobenzoates and p- and m-nitrophenolates were carried out to estimate their structures. 相似文献
The reaction of [Mo(3)S(4)(H(2)O)(9)](4+) (1) with [(CpRhCl(2))(2)] afforded a novel rhodium-molybdenum cluster, [{Mo(3)RhCpS(4)(H(2)O)(7)(O)}(2)](8+) (2). X-ray structure analysis of [2](pts)(8).14H(2)O (pts(-) = CH(3)C(6)H(4)SO(3)(-)) has revealed the existence of a new oxo-bridged twin cubane-type core, (Mo(3)RhCpS(4))(2)(O)(2). The high affinity of the CpRh group for sulfur atoms in 1 seems to be the main driving force for this reaction. The strong Lewis acidity of the CpRh group in intermediate A, [Mo(3)RhCpS(4)(H(2)O)(9)](6+), caused a release of proton from one of the water molecules attached to the molybdenum atoms to give intermediate B, [Mo(3)RhCpS(4)(H(2)O)(8)(OH)](5+). The elimination of two water molecules from two intermediate B molecules, followed by the deprotonation reaction of hydroxo bridges, generated the twin cubane-type cluster 2. The formal oxidation states of rhodium and molybdenum atoms are the same before and after the reaction (i.e., Mo(IV)(3), Rh(III)). The Mo-O-Mo moieties in [2](pts)(8).14H(2)O are nearly linear with a bond angle of 164.3(3) degrees, and the basicity of the bridging oxygen atoms seems to be weak. For this reason, protonation at the bridging oxygen atoms does not occur even in a strongly acidic aqueous solution. The binding energy values of Mo 3d(5/2), Rh 3d(5/2), and C 1s obtained from X-ray photoelectron spectroscopy measurements for [2](pts)(8).14H(2)O are 229.8, 309.3, and 285 eV, respectively. The XPS measurements on the Rh 3d(5/2) binding energy indicate that the oxidation state of Rh is 3+. The binding energy of Mo 3d(5/2) (229.8 eV) compares with that observed for [1](pts)(4).7H(2)O (230.7 eV, Mo 3d(5/2)). A lower energy shift (0.9 eV) is observed in the binding energy of Mo 3d(5/2) for [2](pts)(8).14H(2)O. This energy shift may correspond to the coordination of an oxygen atom having a negative charge to the molybdenum atom. 相似文献
Using different type of initiators, the antibacterial moieties are introduced at the chain end of poly(L,L‐lactide) (PLLA) and poly(D,D‐lactide) (PDLA), and the thermal properties are simultaneously improved using the stereocomplex approach. The physical interaction of polymers and antibacterial compounds is investigated. The double bonds at the chain end are utilized for the interaction of silver ion; however, the silver ions are not detected after stereocomplexation of PLLA and PDLA. On the other hand, catechin (CT) is selected as an initiator precursor of lactide polymerization, protecting the phenolic hydroxyl groups. The linear PLLA and PDLA are obtained by the initiator, resulting in CT conjugated PLAs at the chain end groups after deprotection of phenolic hydroxyl groups. The antibacterial properties are determined by proliferation tests of staphylococcus aureus. The results suggest that the antibacterial properties of CT modified PLAs are derived from the original CT parts.
Novel types of layer-by-layer (LbL) assembly films were successfully fabricated onto a solid substrate through the inclusion complex formation between partially 2,3- O-methylated amyloses (MAs) and polytetrahydrofuran (PTHF). The formation of the LbL assembly films was confirmed by quartz crystal microbalance (QCM) analysis, atomic force microscopy (AFM) observation, and X-ray diffraction (XRD) measurement. The film formation was significantly affected by the methylation degree of amylose. When MAs with 8 and 20% methylation were used as hosts, the formation of LbL assembly films with PTHF was clearly observed. On the other hand, MAs with more than 33% methylation barely formed LbL assembly films with PTHF. 相似文献
Amphiphilic block or graft copolymers have been demonstrated to form a variety of self-assembled nano/microstructures in selective solvents. In this study, the self-association behavior of biodegradable graft copolymers composed of poly(γ-glutamic acid) (γ-PGA) as the hydrophilic segment and L-phenylalanine (Phe) as the hydrophobic segment in aqueous solution was investigated. The association behavior and unimer nanoparticle formation of these γ-PGA-graft-Phe (γ-PGA-Phe) copolymers in aqueous solution were characterized with a focus on the effect of the Phe grafting degree on the intra- and interpolymer association of γ-PGA-Phe. The particle size and number of polymer aggregates (N(agg)) in one particle of the γ-PGA-Phe depended on the Phe grafting degree. The size of γ-PGA-Phe with 12, 27, 35, or 42% Phe grafting (γ-PGA-Phe-12, -27, -35, or -42) was about 8-14 nm and the N(agg) was about 1, supporting the presence of a unimolecular graft copolymer in PBS. The pyrene fluorescence data indicated that γ-PGA-Phe-35 and -42 have hydrophobic domains formed by the intrapolymer association of Phe attached to γ-PGA. These results suggest that the Phe grafting degree is critical to the association behavior of γ-PGA-Phe and that γ-PGA-Phe-35 and -42 could form unimer nanoparticles. Moreover, when γ-PGA-Phe-42 dissolved in DMSO was added to various concentrations of NaCl solution, the particle size and N(agg) could be easily controlled by changing the NaCl concentration during the formation of the particles. These results suggest that biodegradable γ-PGA-Phe is useful for the fabrication of very small nanoparticles. It is expected that γ-PGA-Phe nanoparticles, including unimer particles, will have great potential as multifunctional carriers for pharmaceutical and biomedical applications, such as drug and vaccine delivery systems. 相似文献
Novel water‐insoluble, and reduction‐responsive nonwoven scaffolds were fabricated from γ‐PGA and tested in cell culture. An electrospinning method was developed to produce scaffolds of fibers with diameters of 0.05–0.5 µm. Crosslinking of the fibers with cystamine in the presence of EDC resulted in water‐insoluble γ‐PGA nonwovens with disulfide crosslinkages. These crosslinked fibers were easily decomposed under physiological conditions using L ‐cysteine, a biocompatible reductant. In vitro experiments with mouse L929 fibroblasts showed good adhesion onto γ‐PGA‐SS fiber matrices and excellent cell proliferation. These γ‐PGA‐SS nonwovens can be used as novel biocompatible and biodegradable scaffolds with reduction‐responsiveness for biomedical or tissue engineering applications.