Polymerization of methyl methacrylate in the presence of iron(II) complex with tetradentate nitrogen ligands under conditions of atom transfer radical polymerization

Four tetradentate nitrogen ligands, viz. dichloro{[N,N^′-diphenyl-N,N^′-di(quinoline-2-methyl)]-1,2-ethylene diamine} (1), {[N,N^′-dioctyl-N,N^′-di(quinoline-2-methyl)]-1,2-ethylene diamine} (2), {[N,N^′-dibenzyl-N,N^′-di(quinoline-2-methyl)]-1,2-ethylene diamine} (3), and (1R,2R)-(−)-N,N^′-di(quinoline-2-methyl) di-iminocyclohexane (4), were investigated as novel complexing ligands in iron-mediated atom transfer radical polymerization (ATRP) of methyl methacrylate where ethyl-2-bromoisobutyrate was the initiator in o-xylene at 90 °C. With ligands 1 and 2 the experimental molecular weights increased gradually with monomer conversion. High to moderate conversions (87%, 43%) were obtained in relatively short times (90 min for 1 and 30 min for 2), which indicates an efficient catalyst system, but after these times a dramatic increase in viscosity of the polymerization medium led to loss of control. It is noteworthy that polymerization proceeded in a controlled manner with ligand 1, which has two rather bulky substituents on the N-atom. Such bulky ligands did not work for a copper-based system, where they led to excessive terminations or other side reactions. When the bulkiness of the substituents was significantly increased, as in ligand 3, a decrease in polymerization rate and loss of control occurred. Ligand 4 was less efficient than the other ligands, probably because the ethylene bridge was replaced by cyclohexane bridge.     

INVESTIGATION OF THE ATRP OF n-BUTYL METHACRYLATE USING THE Cu（I）／N,N,N＇ N＂ N＂-PENTAMETHYLDIETHYLENETRIAMINE CATALYST SYSTEM

The polymerization of n-butyl methacrylate was investigated using the Atom Transfer Radical Polymerization technique with CuBr and CuCl/N,N,N‘,N“,N“-pentamethyldiethylenetriamine catalytic systems. Various combinations of catalyst systems and initiators were utilized in order to optimize the polymerization conditions and to obtain well-defined polymers (i.e. controlled molecular weights and low polydispersities). It has been found that the optimal initiator for this system is a chlorine-based initiator, when the catalyst used is a Cu(I) salt in conjunction with the N,N,N‘,N“,N“-pentamethyldiethylenetriamine ligand. Bromine-based initiators tend to result in large amounts of initial termination, leading to polymers with less than ideal chain end functionality, even if CuCI is used as the Cu(I) species to invoke the halogen exchange. Additionally, the effects of the polymerization temperature, copper(I) species and the initiator structure were determined.     

Controlled self-assembly of chiral gelator molecules into aligned fibers induced by nematic to smectic B phase transitions

Chiral bisoxalamide 1 shows remarkable gelling capacity of the nematic and smectic B liquid-crystalline phases of heptylcyclohexanecarboxylic acid (HCCA). Chiral nematic-containing left-handed helical fiber bundles are formed if the gelator is present in amounts higher than 0.55 wt %. With lower amounts of 1, no nematic gel forms, however, a nematic to smectic B phase transition triggers instantaneous self-assembly of gelator molecules into aligned fibers. The latter liquid crystalline gel system represents an example of controlled self-assembly induced by a liquid crystalline phase transition.     

In vitro degradation and release behavior of porous poly(lactic acid) scaffolds containing chitosan microspheres as a carrier for BMP-2-derived synthetic peptide

To develop a novel tissue engineering scaffold with the capability of controlled releasing BMP-2-derived synthetic peptide, porous poly(lactic acid)/chitosan microspheres (PLA/CMs) composites containing different quantities of chitosan microspheres were prepared by a thermally induced phase separation method. FTIR analysis revealed that there were strong hydrogen bond interactions between the PLA and chitosan component. Introduction of less than 30% CMs (on PLA weight basis) did not remarkably affect the morphology and porosity of the PLA/CMs scaffolds. The compressive strength of the composite scaffolds increased from 0.48 to 0.66 MPa, while the compressive modulus increased from 7.29 to 8.23 MPa as the microspheres' contents increased from 0% to 50%. In vitro degradability investigation indicated that the dissolution of chitosan component was preferential than PLA matrix and the inclusion of CMs could neutralize the acidity of PLA degradation products. Compared with the rapid release from CMs, the synthetic peptide was released from PLA/CMs scaffolds in a temporally controlled manner, mainly depending on the degradation of PLA matrix. The promising microspheres based scaffold release system can be used to deliver bioactive factors for a variety of non-loaded bone regeneration and tissue engineering application.     

Combination of “living” nitroxide-mediated and photoiniferter-induced “grafting from” free-radical polymerizations: From branched copolymers to unimolecular micelles and microgels

We report on solution properties of lightly grafted copolymers composed of polystyrene (PS) backbone (degree of polymerization of PS backbone, N_b=95) and variable length of poly(tert-butyl methacrylate) P(tBuMA) side chains (degree of polymerization of side chains, N_sc=14-222) at fixed number of grafting sites n = 11 and polydispersity index (M_w/M_n) ranging from 1.05 to 2.63. Synthesis of these graft copolymers is based on a novel synthetic route [Gromadzki D, Makuška R, Netopilík M, Holler P, Lokaj J, Janata M, et al. Eur Polym J 2008;44:59-71] involving two independent controlled/“living” polymerization mechanisms, namely nitroxide-mediated radical polymerization (NMP) for the synthesis of the backbone and photoinduced “grafting from” iniferter process for building of P(tBuMA) branches. The viscosity-related contraction factors g^′<1 confirmed high degree of branching of the studied graft copolymers. Dilute solutions of graft copolymers in non-selective solvent (THF), examined by dynamic light scattering (DLS), small-angle X-ray scattering (SAXS) and viscometry, revealed a transition from comb-like conformation through wormlike-star to a microgel architecture under increasing number of monomeric units in side chains. These data were further supported by the structure factors R_η/R_h and R_g/R_h obtained by independent measurements and extrapolated to infinite dilution. Persistence lengths of the samples exhibiting comb-like topology were larger compared to linear polystyrene backbone and P(tBuMA) side chains in THF suggesting stiffening of the main chain with increasing size of the attached side chains. Unimolecular micelles were detected by DLS and SAXS in solvent selective for grafts, tert-amyl alcohol.     

Composite microparticle drug delivery systems based on chitosan, alginate and pectin with improved pH-sensitive drug release property

Composite microparticle drug delivery systems based on chitosan, alginate and pectin with improved pH sensitivity were developed for oral delivery of protein drugs, using bovine serum albumin (BSA) as a model drug. The composite drug-loaded microparticles with a mean particle size less than 200 μm were prepared by a convenient shredding method. Since the microparticles were formed by tripolyphosphate cross-linking, electrostatic complexation by alginate and/or pectin, as well as ionotropic gelation with calcium ions, the microparticles exhibited an improved pH-sensitive drug release property. The in vitro drug release behaviors of the microparticles were studied in simulated gastric (pH 1.2 and pH 5.0), intestinal (pH 7.4) and colonic (pH 6.0 and pH 6.8 with enzyme) media. For the composite microparticles with suitable compositions, the releases of BSA at pH 1.2 and pH 5.0 could be effectively sustained, while the releases at pH 7.4, pH 6.8 and pH 6.0 increased significantly, especially in the presence of pectinase. These results clearly suggested that the microparticles had potential for site-specific protein drug delivery through oral administration.     

Incorporation of methamphetamine and amphetamine in human hair following controlled oral methamphetamine administration

Background

Although hair testing is well established for the assessment of past drug exposure, uncertainties persist about mechanisms of drug incorporation into hair and interpretation of results. The aim of this study was to administer methamphetamine (MAMP) under controlled conditions as a model drug to investigate drug incorporation into human hair.

Material and methods

Seven volunteers with a history of stimulant use received 4 × 10 mg (low) doses of sustained release S-(+)-MAMP HCl within 1 week, with weekly head hair samples collected by shaving. 3 weeks later, 4 of them received 4 × 20 mg (high) doses. After extensive isopropanol/phosphate buffer washing of the hair, MAMP and its metabolite amphetamine (AMP) concentrations were determined in all weekly hair samples by LC–MS–MS in selected reaction monitoring mode with the undeca- and deca-deuterated drugs, respectively, as internal standards (LLOQ, 0.005 ng mg⁻¹).

Results

MAMP T_max occurred from 1 to 2 weeks after both doses, with C_max ranging from 0.6 to 3.5 ng mg⁻¹ after the low and 1.2 to 5.3 ng mg⁻¹ after the high MAMP doses. AMP C_max in hair was 0.1–0.3 ng mg⁻¹ and 0.2–0.5 ng mg⁻¹, respectively, for low and high doses. Highly dose-related concentrations within subjects, but large variability between subjects were observed. MAMP concentrations were above the 0.2 ng mg⁻¹ cut-off for at least 2 weeks following administration of both low and high doses. The overall AMP/MAMP ratio ranged from 0.07 to 0.37 with a mean value of 0.15 ± 0.07, and a median of 0.13. The percentage of MAMP and AMP removed with the washing procedure decreased with time after administration. A strong correlation was found between area under the curve of MAMP (r² = 0.90, p = 0.00) and AMP (r² = 0.94, p = 0.00) concentrations calculated for the 3-week period following administration and the total melanin concentration in hair. Significant correlations were observed also between C_max and melanin.

Conclusions

This study demonstrated that despite large inter-individual differences, the incorporation of MAMP and AMP into hair is dose-related with much of the observed scatter of MAMP and AMP concentrations explained by melanin concentration in hair.     

SiO2-PEG凝胶体系织构特性的研究

采用溶胶-凝胶法,以正硅酸乙酯(TEOS)为前驱体,以不同分子量的聚乙二醇(PEG)为改性剂,制备结构可控的多孔SiO₂干凝胶.结果表明:PEG限制了TEOS的水解反应,进而对溶胶粒子的表面进行修饰,形成“粒子团-PEG”聚集体及短程有序的环状网络结构,由此对SiO₂干凝胶的结构性质进行调控.经真空热处理后,PEG等有机残留物被脱除的同时,SiO₂-PEG干凝胶柔性骨架得到加强,孔分布更趋集中,干凝胶结构的热稳定性得到进一步提高.     

Controlled alternating copolymerization of St with MAh in the presence of DBTTC

The copolymerization of styrene (St) with maleic anhydride (MAh) performed at 22 °C in the presence of dibenzyl trithiocarbonate exhibits controlled nature evidenced by: narrow molecular weight distribution, controlled molecular weight and first-order polymerization kinetics. The composition analysis of the copolymers obtained by ¹³C NMR spectra shows the molar fraction of St in obtained copolymers is almost equal to 0.5 throughout the copolymerization. The sequence structure of the copolymer was obtained from DEPT experiments by recording the spectra at π/4 and 3π/4, and then combining them together, the results showed that the copolymers obtained possessed well-defined alternating structure. The experiment shows that charge-transfer-complex formed from St and MAh participates in both initiation and chain growth throughout the copolymerization.     

INVESTIGATION OF THE ATRP OF n-BUTYL METHACRYLATE USING THE Cu(I)/N,N,N'''',N",N"-PENTAMETHYLDIETHYLENETRIAMINE CATALYST SYSTEM

INTRODUCTIONThe atom transfer radical polymerization (ATRP) has become an important method for preparing well-definedmacromolecules. This technique offers control over the molecular weights, the chain end functionalities, and thechain architectures[1-12]. It has been used extensively for the preparation of homopolymers, block, and randomcopolymers[13-39], for the preparation of organic/inorganic hybrid materials[40-54], as well as for combining variousother living polymerization methods …